CA2170486C - Synthesis of amido acids from carboxylic acids and lactams - Google Patents
Synthesis of amido acids from carboxylic acids and lactams Download PDFInfo
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07C—ACYCLIC OR CARBOCYCLIC COMPOUNDS
- C07C303/00—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides
- C07C303/02—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides of sulfonic acids or halides thereof
- C07C303/04—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides of sulfonic acids or halides thereof by substitution of hydrogen atoms by sulfo or halosulfonyl groups
- C07C303/06—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides of sulfonic acids or halides thereof by substitution of hydrogen atoms by sulfo or halosulfonyl groups by reaction with sulfuric acid or sulfur trioxide
-
- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07C—ACYCLIC OR CARBOCYCLIC COMPOUNDS
- C07C231/00—Preparation of carboxylic acid amides
- C07C231/08—Preparation of carboxylic acid amides from amides by reaction at nitrogen atoms of carboxamide groups
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07C—ACYCLIC OR CARBOCYCLIC COMPOUNDS
- C07C231/00—Preparation of carboxylic acid amides
- C07C231/12—Preparation of carboxylic acid amides by reactions not involving the formation of carboxamide groups
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07C—ACYCLIC OR CARBOCYCLIC COMPOUNDS
- C07C303/00—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides
- C07C303/02—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides of sulfonic acids or halides thereof
- C07C303/22—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides of sulfonic acids or halides thereof from sulfonic acids, by reactions not involving the formation of sulfo or halosulfonyl groups; from sulfonic halides by reactions not involving the formation of halosulfonyl groups
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07C—ACYCLIC OR CARBOCYCLIC COMPOUNDS
- C07C303/00—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides
- C07C303/32—Preparation of esters or amides of sulfuric acids; Preparation of sulfonic acids or of their esters, halides, anhydrides or amides of salts of sulfonic acids
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- Y—GENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
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- Y02P—CLIMATE CHANGE MITIGATION TECHNOLOGIES IN THE PRODUCTION OR PROCESSING OF GOODS
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- Y02P20/50—Improvements relating to the production of bulk chemicals
- Y02P20/582—Recycling of unreacted starting or intermediate materials
Abstract
Chemical synthesis of amido acids, and their conversion to amido acid phenyl ester sulfates for use as bleach activators, starting from carboxylic acids and lactams.
Description
WO 95/07883 ~ ~ PCT/US94/09965 SYNTHESIS OF AMIDO ACIDS FROM CARBOXYLIC ACIDS AND
LACTAMS
FIELD OF THE INVENTION
The present invention relates to the chemical synthesis of amido acids, and their conversion to amido acid phenyl ester sulfonates for use as bleach activators. This conversion can be direct by reaction of the amido acids with phenol sulfonic acid derivatives; or by the conversion of the amido acids to their phenyl ester form and then the conversion of said amido phenyl esters into their sulfonated form; or by the conversion of the amido acids to their anhydride and then reaction with sodium phenolsulfonate to form the amido acid phenyl ester sulfonates.
BACKGROUND OF THE INVENTION
The synthesis of ingredients for use in low unit cost consumer goods such as laundry detergents, fabric softeners, hard surface cleansers, and the like, is of considerable interest to manufacturers. Indeed, while formularies and patents are filled with listings of prospective ingredients for use in such products, the reality is that many such ingredients are simply too expensive for day-to-day use.
This expense is often due either to the cost of the raw materials used to make such ingredients, or to the complex reaction and processing chemistry which is required in their manufacture. Accordingly, manufacturers have conducted a continuing search for both inexpensive raw materials and simple reaction sequences which can produce high performance, high value ingredients at the lowest possible cost.
The amido acids comprise one class of chemicals whose amido and carboxylate functional groups suggest their use as surfactants (i.e., sarcosinates), fabric softeners, antistatic agents and the like. Moreover, the amido acids constitute a basic raw material for the amido phenyl ester sulfonate class of chemicals which can serve as bleach activators in laundry detergents and other types of bleach-containing cleaning compositions. Such activators have several desirable attributes such as excellent bleaching performance with minimal color damage on fabric dyes, good washing machine compatibility and a good odor profile in the wash. On the positive side, the amido acids and their aforementioned derivatives are potentially obtainable from inexpensive raw materials. Unfortunately, the synthesis of certain amido acids is somewhat complicated and can involve the use of solvents, with additional problems associated with recycle streams and the like. Problems can also arise with the formation of undesirable colored by-products. Moreover, the conversion of the amido acids to their phenyl ester form is not straightforward and can be surprisingly problematic.
The present invention provides a simple, one-step method for the synthesis of amido acids. It also provides four methods for converting amido acids into amido acid phenyl ester sulfonates which are suitable for use as bleach activators in laundry detergents, and the like. The first method is a simple, one-step esterification of amido acid with phenol to provide an amido acid phenyl ester which can subsequently be reacted with S03 and neutralized in conventional fashion to give amido acid phenyl ester sulfonates. The second prepares the amido acid phenyl ester by transesterification of ester derivatives of phenol followed by the conversion to the amido acid phenyl ester sulfonates as described for the first method. The third method involves transesterification of ester derivatives of phenol sulfonic acid or salt, preferably acetoxybenzenesulfonic acid or salt (typically sodium or potassium), with amido acid to provide amido acid phenyl ester sulfonates directly. The fourth method involves making the anhydride of the amido acid and reacting this anhydride with sodium phenolsulfonate to also produce amido acid phenyl ester sulfonate directly.
The individual reaction sequences herein proceed in acceptable yields (typically 60%, and higher) and, importantly, result in products with minimal discoloration. The reactions may be conducted without added solvents, i.e..
the reactants act as solvents. Hence, for many purposes the reaction products need not be extensively purified which further improve the overall economics of the processes.
BACKGROUND ART
The boric acid-catalyzed esterification of certain phenols is described by W. Lowrance, Jr., in Tetrahedron Letters No. 37 pp. 3453-3454 ( 1971 ) See U.S. Patent 2,956,068, Dohr et al, October 1 1, 1960, for one type of reaction of lactams with carboxylic acids. A process for preparing certain benzenesulfonate salts appears in U.S. 5,153,541, Amini and Dumas, October 6, 1992.
SUMMARY OF THE INVENTION
The present invention encompasses a method for preparing amido acids of the formulas O
II
R°- C w N w RtwCw-OH
I II
H O
(I) and O H O
R-C-N-RrC-N-RrC-OH
H O
(II) wherein R is a C 1 or higher hydrocarbyl substituent and R 1 is C~-C 10 hydrocarbylene substituent, and R1 is preferably -(CH2)x- wherein x is from 2 to 10, by reacting a carboxylic acid of the formula O
a R-C-OH
with a lactam of the structure O H
.C.-.~
l ~..Rli wherein R 1 is as described before, in the presence of an acid catalyst, preferably a member selected from the group consisting of boric acid, sulfuric acid, methanesulfonic acid, trifluoromethanesulfonic acid, phosphoric acid and aryl sulfonic acids such as toluenesulfonic acid and phenolsulfonic acid, and mixtures thereof A preferred acid catalyst is boric acid, methanesulfonic acid or toluenesulfonic acid. if sulfuric acid is used, it is preferred that it be about a 50%-70% concentrated aqueous sulfuric acid, most preferably 70% aqueous H2S04.
The preferred method for preparing said amido acids is conducted at a temperature from about 150°C to about 250°C, especially from about 200°C to about 235°C.
In one preferred embodiment, the method herein employs a lactam selected from caprolactam and valerolactam. In a preferred aspect, the carboxylic acid has substituent R as C6-C 17.
In order to minimize polymerization of the lactam, it is preferred to conduct the reaction herein at a molar ratio of the fatty acid reactant to the lactam reactant of at least about 1.5:1. In a highly preferred mode, the molar ratio of the fatty acid:lactam is in the range of about 2:1 to about 10:1, preferably 3:1 to 4:1, and .the reaction is conducted without added solvent.
t~
LACTAMS
FIELD OF THE INVENTION
The present invention relates to the chemical synthesis of amido acids, and their conversion to amido acid phenyl ester sulfonates for use as bleach activators. This conversion can be direct by reaction of the amido acids with phenol sulfonic acid derivatives; or by the conversion of the amido acids to their phenyl ester form and then the conversion of said amido phenyl esters into their sulfonated form; or by the conversion of the amido acids to their anhydride and then reaction with sodium phenolsulfonate to form the amido acid phenyl ester sulfonates.
BACKGROUND OF THE INVENTION
The synthesis of ingredients for use in low unit cost consumer goods such as laundry detergents, fabric softeners, hard surface cleansers, and the like, is of considerable interest to manufacturers. Indeed, while formularies and patents are filled with listings of prospective ingredients for use in such products, the reality is that many such ingredients are simply too expensive for day-to-day use.
This expense is often due either to the cost of the raw materials used to make such ingredients, or to the complex reaction and processing chemistry which is required in their manufacture. Accordingly, manufacturers have conducted a continuing search for both inexpensive raw materials and simple reaction sequences which can produce high performance, high value ingredients at the lowest possible cost.
The amido acids comprise one class of chemicals whose amido and carboxylate functional groups suggest their use as surfactants (i.e., sarcosinates), fabric softeners, antistatic agents and the like. Moreover, the amido acids constitute a basic raw material for the amido phenyl ester sulfonate class of chemicals which can serve as bleach activators in laundry detergents and other types of bleach-containing cleaning compositions. Such activators have several desirable attributes such as excellent bleaching performance with minimal color damage on fabric dyes, good washing machine compatibility and a good odor profile in the wash. On the positive side, the amido acids and their aforementioned derivatives are potentially obtainable from inexpensive raw materials. Unfortunately, the synthesis of certain amido acids is somewhat complicated and can involve the use of solvents, with additional problems associated with recycle streams and the like. Problems can also arise with the formation of undesirable colored by-products. Moreover, the conversion of the amido acids to their phenyl ester form is not straightforward and can be surprisingly problematic.
The present invention provides a simple, one-step method for the synthesis of amido acids. It also provides four methods for converting amido acids into amido acid phenyl ester sulfonates which are suitable for use as bleach activators in laundry detergents, and the like. The first method is a simple, one-step esterification of amido acid with phenol to provide an amido acid phenyl ester which can subsequently be reacted with S03 and neutralized in conventional fashion to give amido acid phenyl ester sulfonates. The second prepares the amido acid phenyl ester by transesterification of ester derivatives of phenol followed by the conversion to the amido acid phenyl ester sulfonates as described for the first method. The third method involves transesterification of ester derivatives of phenol sulfonic acid or salt, preferably acetoxybenzenesulfonic acid or salt (typically sodium or potassium), with amido acid to provide amido acid phenyl ester sulfonates directly. The fourth method involves making the anhydride of the amido acid and reacting this anhydride with sodium phenolsulfonate to also produce amido acid phenyl ester sulfonate directly.
The individual reaction sequences herein proceed in acceptable yields (typically 60%, and higher) and, importantly, result in products with minimal discoloration. The reactions may be conducted without added solvents, i.e..
the reactants act as solvents. Hence, for many purposes the reaction products need not be extensively purified which further improve the overall economics of the processes.
BACKGROUND ART
The boric acid-catalyzed esterification of certain phenols is described by W. Lowrance, Jr., in Tetrahedron Letters No. 37 pp. 3453-3454 ( 1971 ) See U.S. Patent 2,956,068, Dohr et al, October 1 1, 1960, for one type of reaction of lactams with carboxylic acids. A process for preparing certain benzenesulfonate salts appears in U.S. 5,153,541, Amini and Dumas, October 6, 1992.
SUMMARY OF THE INVENTION
The present invention encompasses a method for preparing amido acids of the formulas O
II
R°- C w N w RtwCw-OH
I II
H O
(I) and O H O
R-C-N-RrC-N-RrC-OH
H O
(II) wherein R is a C 1 or higher hydrocarbyl substituent and R 1 is C~-C 10 hydrocarbylene substituent, and R1 is preferably -(CH2)x- wherein x is from 2 to 10, by reacting a carboxylic acid of the formula O
a R-C-OH
with a lactam of the structure O H
.C.-.~
l ~..Rli wherein R 1 is as described before, in the presence of an acid catalyst, preferably a member selected from the group consisting of boric acid, sulfuric acid, methanesulfonic acid, trifluoromethanesulfonic acid, phosphoric acid and aryl sulfonic acids such as toluenesulfonic acid and phenolsulfonic acid, and mixtures thereof A preferred acid catalyst is boric acid, methanesulfonic acid or toluenesulfonic acid. if sulfuric acid is used, it is preferred that it be about a 50%-70% concentrated aqueous sulfuric acid, most preferably 70% aqueous H2S04.
The preferred method for preparing said amido acids is conducted at a temperature from about 150°C to about 250°C, especially from about 200°C to about 235°C.
In one preferred embodiment, the method herein employs a lactam selected from caprolactam and valerolactam. In a preferred aspect, the carboxylic acid has substituent R as C6-C 17.
In order to minimize polymerization of the lactam, it is preferred to conduct the reaction herein at a molar ratio of the fatty acid reactant to the lactam reactant of at least about 1.5:1. In a highly preferred mode, the molar ratio of the fatty acid:lactam is in the range of about 2:1 to about 10:1, preferably 3:1 to 4:1, and .the reaction is conducted without added solvent.
t~
2~~ c~~~
The invention also encompasses a method for preparing amido acid phenyl esters of the formulas and O
R---C ---N----Rr--C----OPh ~i H O
(III) O H O
ti R~-wC--wNw-wR~--Cw-N----R~-wC ---OPh H O
(IV) wherein R and R 1 are as described herein before, comprising reacting an amido acid having Formulas (I) and/or (II) above with phenol in the presence of a strong catalyst and boric acid to produce the amido acid phenyl esters of Formulas (III) and (IV), respectively.
In this method the strong acid (non-boric acid) catalyst is a member selected from the group consisting of sulfuric acid, methanesulfonic acid, trifluoromethanesulfonic acid, toluenesulfonic acid, phosphonic acid and mixtures thereof. Preferably, the mole ratio of boric acid to the strong acid catalyst is at least about 1:1, more preferably at least about 1 3.6.
Preferably, the mole ratio of amido acid to strong acid catalyst is at least about 1:0.05 and more preferably about 1:0.25. This esterification reaction is preferably conducted at a temperature in the range from about 180°C to about 210°C, and is most preferably conducted without added solvent.
The esterification herein is preferably conducted at a temperature of about 180-190°C in the absence of solvent, with 98% sulfuric acid as the acidic catalyst, and at a mole ratio of boric acid to sulfuric acid of at least about 1:3.6.
Preferably, an excess of phenol is used, typically a phenol:amido acid mole ratio of about 5:1 to about 20:1.
The invention also encompasses a method for preparing amido acid phenyl esters of the formula (II) comprising reacting an amido acid having Formula (I) above with a phenyl ester of a lower molecular weight carboxylic acid moiety, preferably phenyl acetate, in the presence of a basic catalyst. The basic catalyst can be selected from the group consisting of carboxylate salts, carbonates, imidazole and mixtures thereof Preferably, the mole ratio of basic catalyst to amido acid is at least about 0.001:1, more preferably at least about 0 0 I I
Preferably, the mole ratio of amido acid to phenyl ester is at least about I I
and more preferably about 3:1. This transesterification reaction is preferably conducted at a temperature in the range from about 160°C to about ?
10°C. and is most preferably conducted without added solvent.
As an overall proposition, the invention herein also provides a method for preparing bleach activators comprising sulfonating and neutralizing an amido acid phenyl ester of Formulas (III) and/or (IV) prepared according to the foregoing processes to produce, respectively, amido acid phenyl ester sulfonates of the formulas:
p ...
n R-C-N-RrC-O-t~ ~ ~ ~>-----S03M
H p ......::.;, (V) and O H O _ II i~rw\
R-C-N-RrC-N-RrC-O-~~i '~;-S03M
i:
O H .._._..., ( wherein R and Rl are as described hereinbefore, the amido acid phenyl ester sulfonate is predominantly para-substituted (as pictured) although ortho-substitution is acceptable, and M is a cationic moiety, preferably a mono- or divalent metal salt (e.g., potassium, sodium) or hydrogen, which for use of these compounds as bleach activators should be substantially free of transition metal ions (known to cause instability of peroxy compounds).
The invention also encompasses a method for preparing amido acid phenyl ester sulfonates of the Formulas (V) and (VI) above by reacting an amido acid of Formulas (I) and/or (II) above with an ester derivative of phenol sulfonic acid or salt of the formula:
..
~' ORz wherein M is a cationic moiety as described herein before and R2 is an acid moiety, preferably a lower (C2-CS) molecular weight carboxylic acid moiety such as the most preferred acetic acid moiety. When M is hydrogen, the addition of catalyst is not required; when M is a metal salt, this transesterification reaction can utilize an acid or base catalyst.
Reaction temperatures for this transesterification reaction are at least about 1 SO°C, preferably from about 180°C to about 220°C, for reactions with acetoxv .~ 1._1;~4~b benzene sulfonic acid sodium salt. Lower reaction temperatures. from about 140°C to about 180°C, are preferred for reactions with acetoxv benzene sulfonic acid.
The invention also provides a method for preparin; amido acid phenyl ester sulfonates of the Formulas (V) and (VI) above by reacting an amido acid of Formulas (I) and/or (II) above with a lower (C4-C 10) molecular weight carboxylic acid anhydride (e.g., (R3C0)20, wherein each R' is the same or different C 1-C4 hydrocarbyl substituents), preferably acetic anhydride, to form the amido acid anhydride. The amido acid anhydride is then reacted with phenolsulfonate salt (preferably the sodium salt) to form the desired amido acid phenyl ester sulfonates.
The amido acid anhydride is prepared by reacting amido acid with the lower molecular weight carboxylic acid anhydride in a molar ratio ran~in~ from about 1:3 to about 5:1. Reaction temperatures are from about 70-110°C
with reaction times of about 1-18 hr. Catalysts such as sodium acetate, sodium carbonate, sodium bicarbonate, imidazole, or methanesulfonic acid can be used.
At the end of the reaction, carboxylic acid and/or excess carboxylic acid anhydride, such as acetic acid and/or excess acetic anhydride, are removed by distillation.
The crude amido acid anhydride mixture is then reacted with anhydrous phenolsulfonate salt in a molar ratio of about I : I. Reaction temperatures are from about 100-200°C with reaction times of about 1-6 hr. Basic catalysts such as sodium acetate or imidazole can be used. If the crude amido acid anhydride contains excess amido acid, then solvent is not needed. If excess amido acid is not present in the amido acid anhydride, solvents such as dimethylformamide, toluene, or xylenes can be used.
All percentages, ratios and proportions herein are on a mole basis, unless otherwise specified. All documents cited are incorporated herein by reference.
DETAILED DESCRIPTION OF THE INVENTION
Shown herein after are the reaction Sequence ( 1 ) illustrating the synthesis of the amido acids, and reaction Sequence (2a) and (2b) illustratin; their conversion to the phenyl ester form. Sequence (3) illustrates the conventional sulfonation step, which typically includes base neutralization to prepare the salt form of the amido phenyl ester sulfonate class of bleach activators Sequences (4a), (4b), and (5) illustrate alternative methods for preparing the amido phenyl ester sulfonate directly from the amido acid prepared by Sequence ( I ) The 21 7y~+~e reaction sequences as illustrated employ octanoic acid and caprolactam, but this is only by way of illustration and not limitation, as will be seen hereinafter Sequence 1 OOH O Acid Catalyst H O
Carboxylic Acid Lactam Amido acid H O
+ ~ ' OH
O hi O
Diamido acid O O
Acyllactam Sequence 2a H O OH H O
Jla"i + ~ Acid Catalyst OPh O
Amido Acid Phenol Amido Acid Phenyl Ester ~OPh O
Carboxylic Acid Phenyl Ester Sequence 2b ~ H-OOH ~c NaOAc catalyst ,~~~~N-,v~Vl~Ov~.
-..
o + :L~: H o Sequence 3 H
° y ' ,, spa H O '=~%' 2, Neutralization H /' O ~~ ~S03Na Amido Acid Phenyl Ester Amido Acid Phenylestersulfonate Sequence 4a O S03Na O
+ ,;.-'i ~ ':_.N.., Ø ,., .. ... _.%~.N~''. ..-~,~OH ~w . .. .. .~ .. _ H O ~:~% H O
'S03Na OAc Sodium Acetoxybenzenesulfonate Amido Acid Phenylestersulfonate S03Na ...............
+ AcyO
OH
Sequence 4b OH + ~ ~ OOPhS03H
OAc Amido Acid Acetoxybenzenesulfonate Amido Acid Phenylestersulfonate a"i OAc OH
S03 Acid or Base + Ac20 ~ ~ Ac20 +
S43H Catalysis Phenolsulfonic Acid Phenylacetate Phenol Sequence 5 ° 0 0 s.~w~.N._.'~~'y~..~.OH + ACZO ..-H~......". ,.. .. ._~-'.~~N~~. .~-~~Ø ~ ..
~
H O H O O ~ /\
Amido Acid Anhydride off '~ _,NaOAc catalyst v SO~Na O
O
. ~ N -..
i~
H O :-~~ SO~Na 2~~o~8s The following is by way of illustration, and not limitation, of conditions.
equipment and the like, useful in Sequences 1, 2, ;, 4, and > of the instant process.
Sequence I. The carboxylic acid reactant can be selected from straight chain aliphatic, branched chain aliphatic, saturated or unsaturated. aromatic.
heteroaromatic. ethercarboxylic and cycloaliphatic carboxylic acids.
Nonlimitin<, examples include the following carboxylic acids: acetic, propionic, butyric.
caprylic, caproic, nonanoic, 3,5,5-trimethylhexanoic, decanoic, lauric.
myristic.
palmitic, stearic, oleic, linoleic, behenic, 2-methyl-undecanoic, 2-butyl-octanoic, 2-ethyl-hexanoic, alkyl- and alkenylsucciruc, adipic, cyclohexyl, Cg(EO)2C02H, benzoic, chloro-benzoic, nitrobenzoic, naphthertic, abietic, nicotinic, 2-pyridine-carboxylic, terephthalic, phthalic, and mixtures thereof.
The lactam reactant in Sequence 1 can be, for example: butanolactam, valerolactam, caprolactam, heptanolactam, decanolactam, dodecanolactam, and mixtures thereof.
. The acid catalyst in Sequence 1 can be, for example: boric. sulfuric, phosphoric, perchloric, alkylsulfonic acids such as methanesulfonic and trifluoromethanesulfonic, arylsulfonic acids such as benzenesulfonic, toluenesulfonic, naphthalenesulfonic, phenolsulfonic, and strong acid ion-exchange resins such as AMBERLYST"''t and NAFION'~'~''. If a strong acid is used which has oxidizing properties (e.g., sulfuric) it is preferred to add water in order to maintain acceptable color of the final product. As noted, 70% H~S04 is preferred over concentrated H2S04 for this reason. However, nonoxidizing acids such as toluenesulfonic, methanesulfonic, and phosphoric acid do not cause as much color formation and water is not needed.
The acid catalyst in Sequence 1 is employed typically in the range of at least about 0.001 mole, preferably from about 0.01 mole to about 0.1 mole, based on the moles of lactam reactant being used. (The carboxylic acid reactant is present in excess, and is thus not used to calculate the amount of catalyst. ) Water (from about 0.1 to about 1, preferably from about 0.2 to about 0.4, molar equivalents based on the lactam) may be added in Sequence I to increase the conversion of caprolactam to amido acid. The addition can occur at the beginning of the reaction or preferably after 2-4 hours when a maximum amount of amido acid and acyl caprolactam has been formed. The increase in conversion is believed to result from hydrolysis of acyl caprolactam byproduct to amido acid. The conversion is optimum at room temperature in the presence of a strong acid such as methanesulfonic acid. It is believed that selective hydrolysis ~ n~~a6 of the ring amide bond in acyl caprolactam occurs. Although room temperature is preferred for highest conversion, reaction times are long ( 1-2 days) Higher temperatures can be used for quicker reaction times, but the conversion is not as high.
The reaction conditions in Sequence 1 include the following. .Any air in the system causes a drastic darkening of the reaction mixture. Consequently, an inert gas (nitrogen is convenient) is sparged through the reaction mixture during Sequence 1. Inert gases such as argon, or the like, can also be used. The objective is to provide a nonoxidizing reaction system in order to minimize the formation of colored contaminants.
The highly acidic nature of the catalyst used in Sequence I requires inert reaction vessels, such as those made from, or lined with, glass, quartz, high quality stainless steel, and the like. It is highly preferred that all mixers, inlet ports, and the like, also be constructed from inert materials.
Reaction times can vary, of course, depending on the reactant volumes being employed. However, as a general rule for reactions in the 100 mls size range, a reaction time in the range from about 2 hours to about 4 hours is sufficient.
Reaction temperatures in Sequence 1 will typically be above about 150°C
and below about 250°C, and are preferably in the range from about 185°C to about 240°C. For low boiling carboxylic acids such acetic acids, it may be appropriate to use a pressure vessel in order to achieve the desired reaction temperature.
Reaction stoichiometry in Sequence 1 employs an excess of carboxylic acid, which is necessary to prevent oligomerization of the lactam, especially caprolactam. To illustrate this point further, for 1 mole of caprolactam reactant, from about a 1.5 to a 10 mole excess of the carboxylic acid is used. Similar considerations hold with the other lactam reactants and typically at least a 0. I
mole excess of the carboxylic acid is employed. Excess carboxylic acid and any unreacted lactam can be removed from the reaction mixture by vacuum distillation and recycled. (It may be desirable to neutralize the acid catalyst before distillation to prevent oligomers from forming. ) Sequence 2a. The preparation of the phenyl esters of carboxylic acids, especially the amido acids, is as follows. Useful carboxylic acid reactants in Sequence 2 include all of the amido acids prepared per Sequence 1 The phenol reactant includes phenol. itself, as well as alkyl substituted phenols such as cresols and phenol derivatives such as phenolsulfonates.
21704 ~6 The strong acid catalyst used in Sequence ? can be any of the stron;
protonic acid catalysts used in Sequence 1 Sulfuric acid (98%) is convenient.
inexpensive and preferred. Under the process conditions the sulfuric acid sulfates the phenol in situ, so that the strong acid catalyst is at least partially the phenolsulfonic acid.
While not intended to be limiting by theory, it is believed that the mechanism of ester formation involves the formation of a triphenol borate ester by a reaction of a borate material with the phenolic material; followed by exchange of phenol for carboxylic acid to form a carboxylic/boric anhydride species; followed by some manner of phenol displacement of the borate ester from the carboxylic-boric anhydride species; followed by exchange of water to form the borate species and reform the triphenol borate active catalyst agent Accordingly, any borate or boric acid material, or precursor thereof, which results in the formation of a triphenol borate ester with phenol or substituted phenols can be used herein. Typical examples of such materials include boric acid, boric acid precursors, boric acid esters, for example, materials such as borax, tributylborate, triphenylborate, and the like. A wide variety of borate materials are available from standard, commercial sources. Boric acid is a convenient and inexpensive catalyst for use in Sequence 2 It is further hypothesized that the presence of the strong protic acids probably plays at least three different roles in the esterification mechanism:
catalysis of the initial borate ester fotntation; catalysis of phenol displacement of the borate species; and as a desiccant for water which is produced in the reaction.
With regard to reaction conditions. in Sequence 2 any air in the system causes a drastic darkening of the reaction mixture, just as in Sequence 1 Consequently, nitrogen sparging or sparging with another inert has in order to provide a nonoxidizing condition is preferably used. Again, as in Sequence 1, it is preferred in Sequence 2 to use an inert reaction vessel such as those made from glass, quartz, stainless steel, or the like.
Reaction temperatures of at least 150°C, preferably from about 180°C to about 200°C, are preferred, and reaction times are similar to those disclosed for Sequence 1, typically 2 to 4 hours. Water (which may be present in the startin';
materials) is removed during the first 30 minutes of the reaction by azeotropic distillation of phenol/water. The presence of water is detrimental to the overall yield because it can result in the hydrolysis of the amide linkage of the amido acids and/or amido acid phenol esters.
,1~,J~~6 It has been determined that excess phenol or substituted phenol is necessary to drive the reaction to completion. Less excess phenol is viable if azeotropic distillation is carried out for the entire reaction time.
Typically. about a 5 mole excess of said phenol or substituted phenol is employed, preferably from about 8 to about 12 mole excess. Based on the amido acid portion of one mole, the strong acid catalyst proportion is at least about 0.01 mole, preferably from about 0.25 mole to about 0.5 mole. The boric acid is used at levels from about 0.01 mole to about 0.07 moles, based on the amido acid reactant.
Following the esterification reaction, excess phenol is removed from the reaction mixture by vacuum distillation or other suitable means, and can be recycled. The remaining reaction product consists of the desired amido acid phenyl ester, carboxylic acid phenyl ester and unreacted amido acid. This reaction product can be purified prior to sulfonation, or can be sulfonated without further purification since the contaminants are compatable with many detergent compositions.
Sequence 2b Transesterification of a phenyl ester of a lower (C~-CS) molecular weight carboxylic acid moiety, preferably phenyl acetate, with amido acid in the presence of a basic catalyst provides amido acid phenyl ester in food yield. The basic catalyst can be selected from the group consisting of carboxylate salts, carbonates, imidazole and mixtures thereof Preferably, the mole ratio of basic catalyst to amido acid is at least about 0.00 I : I , more preferably at least about 0.01:1. Preferably, the mole ratio of amido acid to phenyl ester is at least about 1:1 and more preferably about 3:1. This transesterification reaction is preferably conducted at a temperature in the range from about 160°C to about 210°C, and is most preferably conducted without added solvent.
Sequence 3. Sulfonation of the amido acid phenol ester can be conducted using sulfiar trioxide, sulfur trioxide vapor, chlorosulfonic acid, sulfur trioxide complexes, oleum, sulfamic acid, and the like, plus other typical sulfonatin~
agents. Reaction can be carried out without solvent, or, if desired, can be conducted in solvents such as sulfiar dioxide, methylene chloride. ethylene dichloride, carbon tetrachloride, fluorotrichloromethane, and the like. It is preferred to run the sulfonation reaction of Sequence 3 without solvent. Of course, unsaturated materials should be avoided in the reaction mixture, primarily due to color formation.
As in the case of Sequences 1 and 2. the sulfonation reaction of Sequence 3 is highly acidic and inert reaction vessels are again used. Reactors can be ~t -....
a the continuous film or continuous cascade types, for example. When sulfur trioxide is used as the sulfonating reactant, it is preferably introduced in an inert gas stream (nitrogen or dry air) containing 1-20% by weight sulfur trioxide Reaction temperatures are typically 20°C to 200°C with reaction times of from to 180 minutes (based on 1 mole of amido acid phenyl ester being sulfonated) For a typical run, the amido acid phenyl ester is present at a 1 mole level and thi, sulfonating agent used at a 0.9-1.5 mole level. Product work-up involves neutralizing the crude reaction mixture to pH 4-6 with base such as sodium bicarbonate, sodium acetate, sodium formate, or the like.
Sequence 4. Amido acid phenyl ester sulfonate can also be made by transesterification of acetoxybenzenesulfonic acid or its salt (typically sodium or potassium) with amido acid. If acetoxybenzenesulfonic acid sodium salt is used, then a 3-4 mol equivalent excess of amido acid is necessary to act as solvent.
If acetoxybenzenesulfonic acid is used, then a 1.2 mol equivalent excess of amido acid is sufficient. Either base or acid catalysis promotes the transesterification of acetoxybenzenesulfonic acid sodium salt; sodium acetate or sulfuric acid are typically used. Transesterification with acetoxybenzenesulfonic acid does not require a catalyst.
A stream of inert gas is passed over the reaction so as remove acetic acid as it is formed and provide a nonoxidizing environment. As in Sequence 3, inert reaction vessels are preferred.
Reaction temperatures of at least about 150° C, preferably from about I 80 ° C to about 220° C, are necessary for transesterification with acetoxybenzenesulfonic acid sodium salt. Lower reaction temperatures (from about 140° C to about 180° C) are preferred when using acetoxybenzenesulfonic acid because less side products are formed. Reaction times are 1-4 hours for either transesterification.
Acetoxybenzenesulfonic acid sodium salt can be prepared from reaction of excess acetic anhydride with dry phenolsulfonic acid sodium salt Acetic anhydride or acetic acid can serve as a solvent. Acetoxybenzenesulfonic acid can be made from reaction of acetic anhydride with dry phenolsulfonic acid.
Alternatively, it can be made from sulfonation of phenyl acetate with sulfur trioxide or chlorosulfonic acid.
Following transesterification with acetoxybenzenesulfonic acid sodium salt, the excess amido acid must be removed from product and recycled. This can be achieved by grinding the reaction product into small particles and dissolvin'_ the amido acid with a solvent. The solid amido acid phenyl ester sulfonate is then collected by filtration. Several solvents are suitable: cold methanol, butanol at 60° C, toluene and xylenes at 100°C, octanoic acid. Product workup after transesterification with acetoxybenzenesulfonic acid involves neutralizing the crude reaction mixture as in Sequence 3.
Sequence 5. Formation of the amido acid anhydride is accomplished by reacting amido acid with acetic anhydride. Reaction temperatures between about 70 and about I 10°C are favored to avoid acylation of the amide nitrogen.
The molar ratio of amido acid to acetic anhydride is from about 1:3 to about 5:1 If the molar ratio is about 3.0: I or higher, it is not necessary to add a solvent for the reaction with sodium phenolsulfonate. After a reaction time of about l - I
hr, acetic acid and/or acetic anhydride are distilled from the reaction mixture to give the crude amido acid anhydride. Sodium phenolsulfonate is then added in about a I :1 molar ratio to the amido acid anhydride and the reaction is heated at from about 100 - 200°C for about 1-18 hr. Toluene or xylenes can be used as solvents for this reaction. At the end of the reaction, unreacted amido acid can be removed from the amido acid phenyl ester sulfonate by washing with a hot solvent (eg, toluene) which melts or dissolves the amido acid, but does not dissolve the amido acid phenyl ester sulfonate.
It is to be understood that the overall process herein provide several advantages over other processes. For example, with respect to the amido acids, the usual synthesis of amido acids employs the reaction of fatty acid chlorides with an amino acid in an aqueous alkaline medium. There are substantial cost advantages over the present development, inasmuch as fatty acids and caprolactams are less expensive starting materials than fatty acid chlorides and aminocaproic acid. In the usual synthesis, sodium chloride waste is generated, which is not a factor in the present invention. Moreover, the process herein has fewer synthetic steps and does not involve large amounts of water, which would have to be removed prior to Sequence 2. Sequence 1 of the present process produces nearly exclusively amido and diamido acids and not lactam-derived higher oligomers. The present invention also has shorter reaction times, lower temperatures and does not require pressures as the reactions of U.S. 2,9S6,U68 With regard to the amido acid phenyl ester synthesis of Sequence ~, esterification of the amido acid can be achieved by forming the acid chloride of the amido acid and subsequently reacting it with phenol or phenolsulfonate This reaction has the same problems as those mentioned above for the amido acid synthesis. While esterification of conventional carboxylic acids with phenols using boric/sulfuric acid has been described in the Lowrance article, cited 21704 ~ti a hereinabove, the reaction conditions described by Lowrance fail to esteritv amido acids in any reasonable yields. For example, the present process employs much higher reaction temperatures than those disclosed by Lowrance, said temperatures being achieved by using phenol as the azeotroping agent Moreover, much higher amounts of sulfuric acid catalyst are used herein, which promotes the desired reaction while reducing side reactions.
In earlier described methods of forming phenyl ester sulfonates (e.g., European Patent Application No. 105,673, published April l8, 1984), a fatty acid anhydride is formed (from reaction with acetic anhydride) and then reacted with phenolsulfonic acid sodium salt. It should be noted that reaction of amido acid with acetic anhydride under the described conditions results not only in formation of amido acid anhydride, but also in formation of imides which is unacceptable. Transesterification with acetoxybenzenesulfonic acid or its salt avoids imide formation.
The overall processes herein comprising either Sequences I-3. Sequences 1 and 4, or Sequences 1 and 5 have several advantages, including one or more of low cost starting materials; minimum number of reaction steps; good yields for each step; reasonable reaction times; no waste by-products; ability to recycle starting materials; and no solids handling until the last step.
The following Examples further illustrate the invention but are not intended to be limiting thereof.
Analytical GC Analysis Method. This method is applicable to the determination of the relative content of octanoic acid, decanoic acid, octanoic acid phenyl ester, octanoyl caprolactam, 2-pyrrolidinone, octanoyl diamido acid, phenylesters of Cg-Clp amidocaproic acid, Cg amidobutyric acid, caprolactam, 6-aminocaproic acid, Cg-C 1 p amidocaproic acid, and phenol, in reaction samples.
The components listed above are separated, after silylation, by temperature programmed GC on a 15m DB 1 column. A hot (300°C) split injector is used and detection is by Fm. GC area % is used to estimate content of components in a sample. The materials containing active hydrogens are derivatized with BSTFA containing 1% TMCS.
Chemicals:
Reagents Pyridine N.O-bis (trimethylsilyl)trifluoroacetamide with 1 % trimethvlchlorosilane Equipment:
2~ ~ ~ c~~6 Equipment Description Source Hewlett Packard 5890 GC Hewlett Packard HP7673 split injection flame ionization detector Column: lSm, DB-1, J&W Scientific 0.25mm ID, .25u Procedure:
1. Standard Preparation:
(See sample preparation to make retention time below standard solutions ) 2. Sample Preparation:
Weigh 5-10 mg sample GC vial, add 1.0 mL derivatization grade into a pyridine and 0.6 mL BSTFATMCS), seal vial, and (w/1% heat at 70C for 30 minutes.
3. Instrument Settines 4. Approximate Retention Times:
a) Split injection On Phenol 6.3 2-Pyrrolidinone 7. 6 b) Split ratio About Caprolactam 10.0 ( 30:1 185)*
c) Column flow I mL/min.Octanoic acid 10.3 d) Purge flow O.SmL/min.Decanoic acid 13.6 e) Injection volume luL 6-aminocaproic acid 14.3, 17.9 (347)*
f) Injector temperature Octanoic acid phenyl 16.4 300C ester Octanoyl amidobutyric 17 ;
acid g) Inlet oven tracking Octanoyl caprolactam 19.5 (239)*
Off h) FID detector 330C Octanoyl amido caproic 23 2, acid 24 0 temperature ( 3 29 ) i) Oven initial 50C Decanoyl amido caproic 25.3, 26.2 temperature acid j) Oven ramp rate 8.0C/min.Hexanoyl amido acid phenyl25.7 ester k) Oven final 325°C Octanoyl amido acid phenyl 27.6 (333)*
temperature ester 1) Oven final hold time 4.63 min. Decanoyl amido acid phenyl 29 6. 30 5 ester Octanoyl diamido acid 31 4. 32 4 (442)*
*Molecular weight of GC component.
2 7 ~p4 g~
The invention also encompasses a method for preparing amido acid phenyl esters of the formulas and O
R---C ---N----Rr--C----OPh ~i H O
(III) O H O
ti R~-wC--wNw-wR~--Cw-N----R~-wC ---OPh H O
(IV) wherein R and R 1 are as described herein before, comprising reacting an amido acid having Formulas (I) and/or (II) above with phenol in the presence of a strong catalyst and boric acid to produce the amido acid phenyl esters of Formulas (III) and (IV), respectively.
In this method the strong acid (non-boric acid) catalyst is a member selected from the group consisting of sulfuric acid, methanesulfonic acid, trifluoromethanesulfonic acid, toluenesulfonic acid, phosphonic acid and mixtures thereof. Preferably, the mole ratio of boric acid to the strong acid catalyst is at least about 1:1, more preferably at least about 1 3.6.
Preferably, the mole ratio of amido acid to strong acid catalyst is at least about 1:0.05 and more preferably about 1:0.25. This esterification reaction is preferably conducted at a temperature in the range from about 180°C to about 210°C, and is most preferably conducted without added solvent.
The esterification herein is preferably conducted at a temperature of about 180-190°C in the absence of solvent, with 98% sulfuric acid as the acidic catalyst, and at a mole ratio of boric acid to sulfuric acid of at least about 1:3.6.
Preferably, an excess of phenol is used, typically a phenol:amido acid mole ratio of about 5:1 to about 20:1.
The invention also encompasses a method for preparing amido acid phenyl esters of the formula (II) comprising reacting an amido acid having Formula (I) above with a phenyl ester of a lower molecular weight carboxylic acid moiety, preferably phenyl acetate, in the presence of a basic catalyst. The basic catalyst can be selected from the group consisting of carboxylate salts, carbonates, imidazole and mixtures thereof Preferably, the mole ratio of basic catalyst to amido acid is at least about 0.001:1, more preferably at least about 0 0 I I
Preferably, the mole ratio of amido acid to phenyl ester is at least about I I
and more preferably about 3:1. This transesterification reaction is preferably conducted at a temperature in the range from about 160°C to about ?
10°C. and is most preferably conducted without added solvent.
As an overall proposition, the invention herein also provides a method for preparing bleach activators comprising sulfonating and neutralizing an amido acid phenyl ester of Formulas (III) and/or (IV) prepared according to the foregoing processes to produce, respectively, amido acid phenyl ester sulfonates of the formulas:
p ...
n R-C-N-RrC-O-t~ ~ ~ ~>-----S03M
H p ......::.;, (V) and O H O _ II i~rw\
R-C-N-RrC-N-RrC-O-~~i '~;-S03M
i:
O H .._._..., ( wherein R and Rl are as described hereinbefore, the amido acid phenyl ester sulfonate is predominantly para-substituted (as pictured) although ortho-substitution is acceptable, and M is a cationic moiety, preferably a mono- or divalent metal salt (e.g., potassium, sodium) or hydrogen, which for use of these compounds as bleach activators should be substantially free of transition metal ions (known to cause instability of peroxy compounds).
The invention also encompasses a method for preparing amido acid phenyl ester sulfonates of the Formulas (V) and (VI) above by reacting an amido acid of Formulas (I) and/or (II) above with an ester derivative of phenol sulfonic acid or salt of the formula:
..
~' ORz wherein M is a cationic moiety as described herein before and R2 is an acid moiety, preferably a lower (C2-CS) molecular weight carboxylic acid moiety such as the most preferred acetic acid moiety. When M is hydrogen, the addition of catalyst is not required; when M is a metal salt, this transesterification reaction can utilize an acid or base catalyst.
Reaction temperatures for this transesterification reaction are at least about 1 SO°C, preferably from about 180°C to about 220°C, for reactions with acetoxv .~ 1._1;~4~b benzene sulfonic acid sodium salt. Lower reaction temperatures. from about 140°C to about 180°C, are preferred for reactions with acetoxv benzene sulfonic acid.
The invention also provides a method for preparin; amido acid phenyl ester sulfonates of the Formulas (V) and (VI) above by reacting an amido acid of Formulas (I) and/or (II) above with a lower (C4-C 10) molecular weight carboxylic acid anhydride (e.g., (R3C0)20, wherein each R' is the same or different C 1-C4 hydrocarbyl substituents), preferably acetic anhydride, to form the amido acid anhydride. The amido acid anhydride is then reacted with phenolsulfonate salt (preferably the sodium salt) to form the desired amido acid phenyl ester sulfonates.
The amido acid anhydride is prepared by reacting amido acid with the lower molecular weight carboxylic acid anhydride in a molar ratio ran~in~ from about 1:3 to about 5:1. Reaction temperatures are from about 70-110°C
with reaction times of about 1-18 hr. Catalysts such as sodium acetate, sodium carbonate, sodium bicarbonate, imidazole, or methanesulfonic acid can be used.
At the end of the reaction, carboxylic acid and/or excess carboxylic acid anhydride, such as acetic acid and/or excess acetic anhydride, are removed by distillation.
The crude amido acid anhydride mixture is then reacted with anhydrous phenolsulfonate salt in a molar ratio of about I : I. Reaction temperatures are from about 100-200°C with reaction times of about 1-6 hr. Basic catalysts such as sodium acetate or imidazole can be used. If the crude amido acid anhydride contains excess amido acid, then solvent is not needed. If excess amido acid is not present in the amido acid anhydride, solvents such as dimethylformamide, toluene, or xylenes can be used.
All percentages, ratios and proportions herein are on a mole basis, unless otherwise specified. All documents cited are incorporated herein by reference.
DETAILED DESCRIPTION OF THE INVENTION
Shown herein after are the reaction Sequence ( 1 ) illustrating the synthesis of the amido acids, and reaction Sequence (2a) and (2b) illustratin; their conversion to the phenyl ester form. Sequence (3) illustrates the conventional sulfonation step, which typically includes base neutralization to prepare the salt form of the amido phenyl ester sulfonate class of bleach activators Sequences (4a), (4b), and (5) illustrate alternative methods for preparing the amido phenyl ester sulfonate directly from the amido acid prepared by Sequence ( I ) The 21 7y~+~e reaction sequences as illustrated employ octanoic acid and caprolactam, but this is only by way of illustration and not limitation, as will be seen hereinafter Sequence 1 OOH O Acid Catalyst H O
Carboxylic Acid Lactam Amido acid H O
+ ~ ' OH
O hi O
Diamido acid O O
Acyllactam Sequence 2a H O OH H O
Jla"i + ~ Acid Catalyst OPh O
Amido Acid Phenol Amido Acid Phenyl Ester ~OPh O
Carboxylic Acid Phenyl Ester Sequence 2b ~ H-OOH ~c NaOAc catalyst ,~~~~N-,v~Vl~Ov~.
-..
o + :L~: H o Sequence 3 H
° y ' ,, spa H O '=~%' 2, Neutralization H /' O ~~ ~S03Na Amido Acid Phenyl Ester Amido Acid Phenylestersulfonate Sequence 4a O S03Na O
+ ,;.-'i ~ ':_.N.., Ø ,., .. ... _.%~.N~''. ..-~,~OH ~w . .. .. .~ .. _ H O ~:~% H O
'S03Na OAc Sodium Acetoxybenzenesulfonate Amido Acid Phenylestersulfonate S03Na ...............
+ AcyO
OH
Sequence 4b OH + ~ ~ OOPhS03H
OAc Amido Acid Acetoxybenzenesulfonate Amido Acid Phenylestersulfonate a"i OAc OH
S03 Acid or Base + Ac20 ~ ~ Ac20 +
S43H Catalysis Phenolsulfonic Acid Phenylacetate Phenol Sequence 5 ° 0 0 s.~w~.N._.'~~'y~..~.OH + ACZO ..-H~......". ,.. .. ._~-'.~~N~~. .~-~~Ø ~ ..
~
H O H O O ~ /\
Amido Acid Anhydride off '~ _,NaOAc catalyst v SO~Na O
O
. ~ N -..
i~
H O :-~~ SO~Na 2~~o~8s The following is by way of illustration, and not limitation, of conditions.
equipment and the like, useful in Sequences 1, 2, ;, 4, and > of the instant process.
Sequence I. The carboxylic acid reactant can be selected from straight chain aliphatic, branched chain aliphatic, saturated or unsaturated. aromatic.
heteroaromatic. ethercarboxylic and cycloaliphatic carboxylic acids.
Nonlimitin<, examples include the following carboxylic acids: acetic, propionic, butyric.
caprylic, caproic, nonanoic, 3,5,5-trimethylhexanoic, decanoic, lauric.
myristic.
palmitic, stearic, oleic, linoleic, behenic, 2-methyl-undecanoic, 2-butyl-octanoic, 2-ethyl-hexanoic, alkyl- and alkenylsucciruc, adipic, cyclohexyl, Cg(EO)2C02H, benzoic, chloro-benzoic, nitrobenzoic, naphthertic, abietic, nicotinic, 2-pyridine-carboxylic, terephthalic, phthalic, and mixtures thereof.
The lactam reactant in Sequence 1 can be, for example: butanolactam, valerolactam, caprolactam, heptanolactam, decanolactam, dodecanolactam, and mixtures thereof.
. The acid catalyst in Sequence 1 can be, for example: boric. sulfuric, phosphoric, perchloric, alkylsulfonic acids such as methanesulfonic and trifluoromethanesulfonic, arylsulfonic acids such as benzenesulfonic, toluenesulfonic, naphthalenesulfonic, phenolsulfonic, and strong acid ion-exchange resins such as AMBERLYST"''t and NAFION'~'~''. If a strong acid is used which has oxidizing properties (e.g., sulfuric) it is preferred to add water in order to maintain acceptable color of the final product. As noted, 70% H~S04 is preferred over concentrated H2S04 for this reason. However, nonoxidizing acids such as toluenesulfonic, methanesulfonic, and phosphoric acid do not cause as much color formation and water is not needed.
The acid catalyst in Sequence 1 is employed typically in the range of at least about 0.001 mole, preferably from about 0.01 mole to about 0.1 mole, based on the moles of lactam reactant being used. (The carboxylic acid reactant is present in excess, and is thus not used to calculate the amount of catalyst. ) Water (from about 0.1 to about 1, preferably from about 0.2 to about 0.4, molar equivalents based on the lactam) may be added in Sequence I to increase the conversion of caprolactam to amido acid. The addition can occur at the beginning of the reaction or preferably after 2-4 hours when a maximum amount of amido acid and acyl caprolactam has been formed. The increase in conversion is believed to result from hydrolysis of acyl caprolactam byproduct to amido acid. The conversion is optimum at room temperature in the presence of a strong acid such as methanesulfonic acid. It is believed that selective hydrolysis ~ n~~a6 of the ring amide bond in acyl caprolactam occurs. Although room temperature is preferred for highest conversion, reaction times are long ( 1-2 days) Higher temperatures can be used for quicker reaction times, but the conversion is not as high.
The reaction conditions in Sequence 1 include the following. .Any air in the system causes a drastic darkening of the reaction mixture. Consequently, an inert gas (nitrogen is convenient) is sparged through the reaction mixture during Sequence 1. Inert gases such as argon, or the like, can also be used. The objective is to provide a nonoxidizing reaction system in order to minimize the formation of colored contaminants.
The highly acidic nature of the catalyst used in Sequence I requires inert reaction vessels, such as those made from, or lined with, glass, quartz, high quality stainless steel, and the like. It is highly preferred that all mixers, inlet ports, and the like, also be constructed from inert materials.
Reaction times can vary, of course, depending on the reactant volumes being employed. However, as a general rule for reactions in the 100 mls size range, a reaction time in the range from about 2 hours to about 4 hours is sufficient.
Reaction temperatures in Sequence 1 will typically be above about 150°C
and below about 250°C, and are preferably in the range from about 185°C to about 240°C. For low boiling carboxylic acids such acetic acids, it may be appropriate to use a pressure vessel in order to achieve the desired reaction temperature.
Reaction stoichiometry in Sequence 1 employs an excess of carboxylic acid, which is necessary to prevent oligomerization of the lactam, especially caprolactam. To illustrate this point further, for 1 mole of caprolactam reactant, from about a 1.5 to a 10 mole excess of the carboxylic acid is used. Similar considerations hold with the other lactam reactants and typically at least a 0. I
mole excess of the carboxylic acid is employed. Excess carboxylic acid and any unreacted lactam can be removed from the reaction mixture by vacuum distillation and recycled. (It may be desirable to neutralize the acid catalyst before distillation to prevent oligomers from forming. ) Sequence 2a. The preparation of the phenyl esters of carboxylic acids, especially the amido acids, is as follows. Useful carboxylic acid reactants in Sequence 2 include all of the amido acids prepared per Sequence 1 The phenol reactant includes phenol. itself, as well as alkyl substituted phenols such as cresols and phenol derivatives such as phenolsulfonates.
21704 ~6 The strong acid catalyst used in Sequence ? can be any of the stron;
protonic acid catalysts used in Sequence 1 Sulfuric acid (98%) is convenient.
inexpensive and preferred. Under the process conditions the sulfuric acid sulfates the phenol in situ, so that the strong acid catalyst is at least partially the phenolsulfonic acid.
While not intended to be limiting by theory, it is believed that the mechanism of ester formation involves the formation of a triphenol borate ester by a reaction of a borate material with the phenolic material; followed by exchange of phenol for carboxylic acid to form a carboxylic/boric anhydride species; followed by some manner of phenol displacement of the borate ester from the carboxylic-boric anhydride species; followed by exchange of water to form the borate species and reform the triphenol borate active catalyst agent Accordingly, any borate or boric acid material, or precursor thereof, which results in the formation of a triphenol borate ester with phenol or substituted phenols can be used herein. Typical examples of such materials include boric acid, boric acid precursors, boric acid esters, for example, materials such as borax, tributylborate, triphenylborate, and the like. A wide variety of borate materials are available from standard, commercial sources. Boric acid is a convenient and inexpensive catalyst for use in Sequence 2 It is further hypothesized that the presence of the strong protic acids probably plays at least three different roles in the esterification mechanism:
catalysis of the initial borate ester fotntation; catalysis of phenol displacement of the borate species; and as a desiccant for water which is produced in the reaction.
With regard to reaction conditions. in Sequence 2 any air in the system causes a drastic darkening of the reaction mixture, just as in Sequence 1 Consequently, nitrogen sparging or sparging with another inert has in order to provide a nonoxidizing condition is preferably used. Again, as in Sequence 1, it is preferred in Sequence 2 to use an inert reaction vessel such as those made from glass, quartz, stainless steel, or the like.
Reaction temperatures of at least 150°C, preferably from about 180°C to about 200°C, are preferred, and reaction times are similar to those disclosed for Sequence 1, typically 2 to 4 hours. Water (which may be present in the startin';
materials) is removed during the first 30 minutes of the reaction by azeotropic distillation of phenol/water. The presence of water is detrimental to the overall yield because it can result in the hydrolysis of the amide linkage of the amido acids and/or amido acid phenol esters.
,1~,J~~6 It has been determined that excess phenol or substituted phenol is necessary to drive the reaction to completion. Less excess phenol is viable if azeotropic distillation is carried out for the entire reaction time.
Typically. about a 5 mole excess of said phenol or substituted phenol is employed, preferably from about 8 to about 12 mole excess. Based on the amido acid portion of one mole, the strong acid catalyst proportion is at least about 0.01 mole, preferably from about 0.25 mole to about 0.5 mole. The boric acid is used at levels from about 0.01 mole to about 0.07 moles, based on the amido acid reactant.
Following the esterification reaction, excess phenol is removed from the reaction mixture by vacuum distillation or other suitable means, and can be recycled. The remaining reaction product consists of the desired amido acid phenyl ester, carboxylic acid phenyl ester and unreacted amido acid. This reaction product can be purified prior to sulfonation, or can be sulfonated without further purification since the contaminants are compatable with many detergent compositions.
Sequence 2b Transesterification of a phenyl ester of a lower (C~-CS) molecular weight carboxylic acid moiety, preferably phenyl acetate, with amido acid in the presence of a basic catalyst provides amido acid phenyl ester in food yield. The basic catalyst can be selected from the group consisting of carboxylate salts, carbonates, imidazole and mixtures thereof Preferably, the mole ratio of basic catalyst to amido acid is at least about 0.00 I : I , more preferably at least about 0.01:1. Preferably, the mole ratio of amido acid to phenyl ester is at least about 1:1 and more preferably about 3:1. This transesterification reaction is preferably conducted at a temperature in the range from about 160°C to about 210°C, and is most preferably conducted without added solvent.
Sequence 3. Sulfonation of the amido acid phenol ester can be conducted using sulfiar trioxide, sulfur trioxide vapor, chlorosulfonic acid, sulfur trioxide complexes, oleum, sulfamic acid, and the like, plus other typical sulfonatin~
agents. Reaction can be carried out without solvent, or, if desired, can be conducted in solvents such as sulfiar dioxide, methylene chloride. ethylene dichloride, carbon tetrachloride, fluorotrichloromethane, and the like. It is preferred to run the sulfonation reaction of Sequence 3 without solvent. Of course, unsaturated materials should be avoided in the reaction mixture, primarily due to color formation.
As in the case of Sequences 1 and 2. the sulfonation reaction of Sequence 3 is highly acidic and inert reaction vessels are again used. Reactors can be ~t -....
a the continuous film or continuous cascade types, for example. When sulfur trioxide is used as the sulfonating reactant, it is preferably introduced in an inert gas stream (nitrogen or dry air) containing 1-20% by weight sulfur trioxide Reaction temperatures are typically 20°C to 200°C with reaction times of from to 180 minutes (based on 1 mole of amido acid phenyl ester being sulfonated) For a typical run, the amido acid phenyl ester is present at a 1 mole level and thi, sulfonating agent used at a 0.9-1.5 mole level. Product work-up involves neutralizing the crude reaction mixture to pH 4-6 with base such as sodium bicarbonate, sodium acetate, sodium formate, or the like.
Sequence 4. Amido acid phenyl ester sulfonate can also be made by transesterification of acetoxybenzenesulfonic acid or its salt (typically sodium or potassium) with amido acid. If acetoxybenzenesulfonic acid sodium salt is used, then a 3-4 mol equivalent excess of amido acid is necessary to act as solvent.
If acetoxybenzenesulfonic acid is used, then a 1.2 mol equivalent excess of amido acid is sufficient. Either base or acid catalysis promotes the transesterification of acetoxybenzenesulfonic acid sodium salt; sodium acetate or sulfuric acid are typically used. Transesterification with acetoxybenzenesulfonic acid does not require a catalyst.
A stream of inert gas is passed over the reaction so as remove acetic acid as it is formed and provide a nonoxidizing environment. As in Sequence 3, inert reaction vessels are preferred.
Reaction temperatures of at least about 150° C, preferably from about I 80 ° C to about 220° C, are necessary for transesterification with acetoxybenzenesulfonic acid sodium salt. Lower reaction temperatures (from about 140° C to about 180° C) are preferred when using acetoxybenzenesulfonic acid because less side products are formed. Reaction times are 1-4 hours for either transesterification.
Acetoxybenzenesulfonic acid sodium salt can be prepared from reaction of excess acetic anhydride with dry phenolsulfonic acid sodium salt Acetic anhydride or acetic acid can serve as a solvent. Acetoxybenzenesulfonic acid can be made from reaction of acetic anhydride with dry phenolsulfonic acid.
Alternatively, it can be made from sulfonation of phenyl acetate with sulfur trioxide or chlorosulfonic acid.
Following transesterification with acetoxybenzenesulfonic acid sodium salt, the excess amido acid must be removed from product and recycled. This can be achieved by grinding the reaction product into small particles and dissolvin'_ the amido acid with a solvent. The solid amido acid phenyl ester sulfonate is then collected by filtration. Several solvents are suitable: cold methanol, butanol at 60° C, toluene and xylenes at 100°C, octanoic acid. Product workup after transesterification with acetoxybenzenesulfonic acid involves neutralizing the crude reaction mixture as in Sequence 3.
Sequence 5. Formation of the amido acid anhydride is accomplished by reacting amido acid with acetic anhydride. Reaction temperatures between about 70 and about I 10°C are favored to avoid acylation of the amide nitrogen.
The molar ratio of amido acid to acetic anhydride is from about 1:3 to about 5:1 If the molar ratio is about 3.0: I or higher, it is not necessary to add a solvent for the reaction with sodium phenolsulfonate. After a reaction time of about l - I
hr, acetic acid and/or acetic anhydride are distilled from the reaction mixture to give the crude amido acid anhydride. Sodium phenolsulfonate is then added in about a I :1 molar ratio to the amido acid anhydride and the reaction is heated at from about 100 - 200°C for about 1-18 hr. Toluene or xylenes can be used as solvents for this reaction. At the end of the reaction, unreacted amido acid can be removed from the amido acid phenyl ester sulfonate by washing with a hot solvent (eg, toluene) which melts or dissolves the amido acid, but does not dissolve the amido acid phenyl ester sulfonate.
It is to be understood that the overall process herein provide several advantages over other processes. For example, with respect to the amido acids, the usual synthesis of amido acids employs the reaction of fatty acid chlorides with an amino acid in an aqueous alkaline medium. There are substantial cost advantages over the present development, inasmuch as fatty acids and caprolactams are less expensive starting materials than fatty acid chlorides and aminocaproic acid. In the usual synthesis, sodium chloride waste is generated, which is not a factor in the present invention. Moreover, the process herein has fewer synthetic steps and does not involve large amounts of water, which would have to be removed prior to Sequence 2. Sequence 1 of the present process produces nearly exclusively amido and diamido acids and not lactam-derived higher oligomers. The present invention also has shorter reaction times, lower temperatures and does not require pressures as the reactions of U.S. 2,9S6,U68 With regard to the amido acid phenyl ester synthesis of Sequence ~, esterification of the amido acid can be achieved by forming the acid chloride of the amido acid and subsequently reacting it with phenol or phenolsulfonate This reaction has the same problems as those mentioned above for the amido acid synthesis. While esterification of conventional carboxylic acids with phenols using boric/sulfuric acid has been described in the Lowrance article, cited 21704 ~ti a hereinabove, the reaction conditions described by Lowrance fail to esteritv amido acids in any reasonable yields. For example, the present process employs much higher reaction temperatures than those disclosed by Lowrance, said temperatures being achieved by using phenol as the azeotroping agent Moreover, much higher amounts of sulfuric acid catalyst are used herein, which promotes the desired reaction while reducing side reactions.
In earlier described methods of forming phenyl ester sulfonates (e.g., European Patent Application No. 105,673, published April l8, 1984), a fatty acid anhydride is formed (from reaction with acetic anhydride) and then reacted with phenolsulfonic acid sodium salt. It should be noted that reaction of amido acid with acetic anhydride under the described conditions results not only in formation of amido acid anhydride, but also in formation of imides which is unacceptable. Transesterification with acetoxybenzenesulfonic acid or its salt avoids imide formation.
The overall processes herein comprising either Sequences I-3. Sequences 1 and 4, or Sequences 1 and 5 have several advantages, including one or more of low cost starting materials; minimum number of reaction steps; good yields for each step; reasonable reaction times; no waste by-products; ability to recycle starting materials; and no solids handling until the last step.
The following Examples further illustrate the invention but are not intended to be limiting thereof.
Analytical GC Analysis Method. This method is applicable to the determination of the relative content of octanoic acid, decanoic acid, octanoic acid phenyl ester, octanoyl caprolactam, 2-pyrrolidinone, octanoyl diamido acid, phenylesters of Cg-Clp amidocaproic acid, Cg amidobutyric acid, caprolactam, 6-aminocaproic acid, Cg-C 1 p amidocaproic acid, and phenol, in reaction samples.
The components listed above are separated, after silylation, by temperature programmed GC on a 15m DB 1 column. A hot (300°C) split injector is used and detection is by Fm. GC area % is used to estimate content of components in a sample. The materials containing active hydrogens are derivatized with BSTFA containing 1% TMCS.
Chemicals:
Reagents Pyridine N.O-bis (trimethylsilyl)trifluoroacetamide with 1 % trimethvlchlorosilane Equipment:
2~ ~ ~ c~~6 Equipment Description Source Hewlett Packard 5890 GC Hewlett Packard HP7673 split injection flame ionization detector Column: lSm, DB-1, J&W Scientific 0.25mm ID, .25u Procedure:
1. Standard Preparation:
(See sample preparation to make retention time below standard solutions ) 2. Sample Preparation:
Weigh 5-10 mg sample GC vial, add 1.0 mL derivatization grade into a pyridine and 0.6 mL BSTFATMCS), seal vial, and (w/1% heat at 70C for 30 minutes.
3. Instrument Settines 4. Approximate Retention Times:
a) Split injection On Phenol 6.3 2-Pyrrolidinone 7. 6 b) Split ratio About Caprolactam 10.0 ( 30:1 185)*
c) Column flow I mL/min.Octanoic acid 10.3 d) Purge flow O.SmL/min.Decanoic acid 13.6 e) Injection volume luL 6-aminocaproic acid 14.3, 17.9 (347)*
f) Injector temperature Octanoic acid phenyl 16.4 300C ester Octanoyl amidobutyric 17 ;
acid g) Inlet oven tracking Octanoyl caprolactam 19.5 (239)*
Off h) FID detector 330C Octanoyl amido caproic 23 2, acid 24 0 temperature ( 3 29 ) i) Oven initial 50C Decanoyl amido caproic 25.3, 26.2 temperature acid j) Oven ramp rate 8.0C/min.Hexanoyl amido acid phenyl25.7 ester k) Oven final 325°C Octanoyl amido acid phenyl 27.6 (333)*
temperature ester 1) Oven final hold time 4.63 min. Decanoyl amido acid phenyl 29 6. 30 5 ester Octanoyl diamido acid 31 4. 32 4 (442)*
*Molecular weight of GC component.
2 7 ~p4 g~
4. Calculation of Mole% Conversion: The GC relative area ° o for each component derived from caprolactam is divided by its molecular weight or the molecular weight of its trimethylsilyl derivative to give a relative mol°,'o The relative mol% for all components derived from caprolactam are summed to give a total relative mol%. Finally, each relative mol% is divided by the total relative mol% to give mol% conversion. An analogous procedure is used to calculate mol% conversion of amido acid to amido acid phenyl ester.
AMIDATION EXAMPLES I-XV
Synthesis of C8-Amidocaproic Acid - A 100 mL, 3-neck, round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a purge tube through which nitrogen is passed through the reaction mixture. The reaction vessel is charged with caprolactam (4.00 g, 0.036 mol, 1 mol equivalent), octanoic acid, the indicated strong acid catalyst (TSA, MSA, PSA, PPA, SA, as described in the tables), and optionally boric acid. The reaction is kept at the designated temperature for 4 hours using a high temperature oil bath, continuously purging with nitrogen. After 4 hour reaction time, the reaction mixture is analyzed by GC (see GC Analysis Method) to determine conversion of caprolactam to amido acid (see Table 1 ). Reaction mixture color after 4 hours is also noted.
Table 1. Amidation Results Example # I II III IV V
Octanoic acid (mol equivalent) 4 4 4 4 2 Strong acid catalyst* (mol equivalent) 0.1 0.05 0.1 0.05 0. I
TSA TSA TSA TSA TSA
Boric acid (mol equivalent) ----- 0.05 ----- ----- _--__ Water (mol equivalent) ----- ----- ----- 0 2 _-___ Temperature (°C) 200 200 175 220 200 Reaction color after 4 hr brown brown yellow brown brown GC Relative Area % for Components Caprolactam 3.59 3.82 I 0.33 3 56 9 09 Octanoic acid 74.97 73.23 79.21 74 79 62.96 6-aminocaproic acid 0.12 0 1.12 0.26 0 Octanoylcaprolactam 2.37 3.0? 0 94 3.67 1 48 Octanoyl amido acid 15 95 17.24 6 49 I 5 6 19 1 Octanoyl diamido acid 1.63 1.21 0.62 0 89 5 07 Mole % Conversion of Caprolactam to Components Caprolactam 23.7 23.3 66 ?2.9 39 6-aminocaproic acid 0.4 0 3 0 0 Octanoylcaprolactam 12.1 14.3 4 18.3 5 0 Octanoyl amido acid 59.2 59.3 23.4 56 4 46 Octanoyl diamido acid 4.5 3.1 I 2.4 9 2 .7 *Key to abbreviations: 99%), SA
TSA (toluenesulfonic acid M
monohydrate (methanesulfonic acid 99%), lsulfoniccid SA (sulfuric acid 98%), a PSA (pheno 65%), PA (polyphosphoric acid) Table 1. continued Example # VI VII VIII IX X
Octanoic acid (mol equivalent)4 4 4 4 4 Strong acid catalyst* (mol0.05 0.05 0.05 0.05 U US
equivalent) MSA MSA MSA PSA PPA
Boric acid (mol equivalent)----- ----- 0.05 0.05 -----Water (mol equivalent) ----- 0.2 ---------- -----Temperature (C) 200 200 200 200 200 Reaction color after 4 brown brown yellowblack yellow hr GC Relative Area % for Components Caprolactam 5.08 3.86 3.68 8 99 6.64 Octanoic acid 73.5 74.06 72.3678.29 71 6-aminocaproic acid 0 0 0 0.60 0 Octanoylcaprolactam 3.41 2.40 3.08 1.26 4.02 Octanoyl amido acid 15.75 17.07 17.358.91 15.03 Octanoyl diamido acid 0.90 1.23 2.02 0.62 0 98 Mole % Conversion of Caprolactam to Components Caprolactam 30.0 24.4 22.1 57 8 35 6-aminocaproic acid 0 0 0 2. I 0 Octanoylcaprolactam 15.6 1 1.7 14.3 6.3 16 Octanoyl amido acid 52.2 60.6 58.5 32.2 45 Octanoyl diamido acid 2.2 3.3 5.1 1.7 ?.?
Table 1. continued Example # XI XII XIII XIV ?CV
Octanoic acid (mol equivalent)4 4 4 4 I
Strong acid catalyst* (mol0.01 0.05 0 0 ?4 0 O
equivalent) 05 i SA SA SA SA SA
Boric acid (mol equivalent)0.05 0.05 0 0 05 0 05 ,~17p4g6 Water (mol equivalent) ----- 1 0.2 0.4 - ----Temperature (C) 210 200 200 200 200 Reaction color after 4 hr black yellow black black black GC Relative Area % for Components Caprolactam 3.22 7.54 3 88 2.6 21 Octanoic acid 72.41 78.54 73.68 78.24 40 6-aminocaproic acid 0.14 1.47 0.44 2.41 0.22 Octanoylcaprolactam 2.33 0.17 0 51 0 33 0 Octanoyl amido acid 17.46 9.53 18.21 13.58 23.34 Octanoyl diamido acid 2.61 1.28 2.46 1.38 9.85 Mole % Conversion of Caprolactam To Components Caprolactam 20.2 52.6 24.6 21.0 >3.5 6-aminocaproic acid 0 5.5 1.5 I 0 4 0.3 Octanoylcaprolactam 11.3 0.9 2.5 2.0 0.9 Octanoyl amido acid 61.6 3 7.4 64.9 61. 8 3 .
Octanoyl diamido acid 6.9 3 .7 6.5 4. 7 t U.4 *Key to abbreviations: TSA (toluenesulfonic acid monohydrate 99%), MSA
(methanesulfonic acid 99%), SA (sulfuric acid 98%), PSA (phenolsulfonic acid 65%), PA (polyphosphoric acid) EXAMPLES XVI-XVIII
Synthesis of C8-Amidocaproic Acid - A 100 ml, 3-neck round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a spare tube through which nitrogen is passed through the reaction mixture. The reaction vessel is charged with caprolactam (4.00 g, 0.036 mol, 1 mol equivalent), octanoic acid, boric acid, and water. The reaction is kept at the designated temperature for 3.5 hr using a high temperature oil bath, continuously sparing with nitrogen. After 3.5 hr reaction time, the reaction mixture is analvz.ed by GC
(see GC Analysis Method) to determine % conversion of the caprolactam to amido acid (see Table 2). Other products formed are 6-aminocaproic acid, octanoyl caprolactam, and octanoyl diamido acid. Reaction mixture color after 3.5 hr is also noted.
Table 2. Amidation Results Example # XVI XVII
XVIII
Octanoic acid (mol equivalent) 4 8 ~_ boric acid (mol equivalent) 0.025 0.05 0 025 water (mol equivalent) 0.1 0. I 0 I
temperature (C) 235 220 23s reaction color after 4 hours yellow yellow oran<~e GC Relative Area % for Components caprolactam 3.46 1.39 6 42 octanoic acid 71.57 85.06 55.01 6-aminocaproic acid 0 0 0 octanoylcaprolactam 4.71 1.18 3.49 octanoyl amido acid 15.44 10.33 26.09 octanoyl diamido acid 1.74 0.39 5.37 Mole % Conversion of Caprolactam to Components caprolactam 20.9 16.8 24 7 6-aminocaproic acid 0 0 0 octanoylcaprolactam 22.1 I 1.1 10.4 octanoyl amido acid 52.6 70.2 56.3 octanoyl diamido acid 4.4 2.0 8.6 EXAMPLES XIX-XX
Synthesis of C8-Amidoc~roic Acid - A 100 ml, 3-neck round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a sparge tube through which nitrogen is passed through the reaction mixture. The reaction vessel is charged with caprolactam (4.00 g, 0.036 mol, 1 mol equivalent), octanoic acid, methanesulfonic acid, and boric acid. The reaction is kept at the designated temperature for 6.5 hr using a high temperature oil bath, continuously sparging with nitrogen. The reaction is then allowed to cool to room temperature and water is added. The reaction is allowed to stir at room temperature for 18 hr. Before water addition (Example XIX) and 18 hr after water addition (Example XX), the reaction mixture is analyzed by GC (see GC
Analysis Method) to determine % conversion of caprolactam to amido acid (see Table 3). Other products formed are 6-aminocaproic acid, octanoyl caprolactam, and octanoyl diamido acid. Reaction mixture color is also noted.
Table 3. Amidation Results Example # XIX XX
Octanoic acid (mol equivalent) 9.28 9.28 boric acid (mol equivalent) O OS 0 05 water (mol equivalent) ---- 0 I
methanesulfonic acid (mol 0.1 0.01 equivalent) temperature (C) 235 250 reaction color orange orange GC Relative Area % for Components caprolactam 0.60 I 39 octanoic acid 84.89 8 5 06 6-aminocaproic acid 0 0 octanoylcaprolactam 2.75 1.18 octanoyl amido acid 6.36 10 3 octanoyl diamido acid 0 0 39 Mole % Conversion of Caprolactam to Components caprolactam 9.5 I6 8 6-aminocaproic acid 0 0 octanoylcaprolactam 33 . 8 1 1.1 octanoyl amido acid 56.8 70.2 octanoyl diamido acid 0 2 0 EXAMPLE XXI
Synthesis of C8 Amidobutyric Acid - A 100 mL, 3-neck, round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a purge tube through which nitrogen is passed through the reaction mixture The reaction vessel is charged with 2-pyrrolidinone (2.00 g, 0.024 mol), octanoic acid ( I
3.56 g, 0.094 mol), and sulfuric acid 98% (0.12 g, 0.0012 mol). The reaction is kept at 200°C for 4 hours using a high temperature oil bath, continuously purging with nitrogen. After 4 hour reaction time, the reaction mixture is analyzed by GC (see Table 2). A 31% conversion of pyrrolidinone to amido acid is obtained The reaction mixture is brown after 4 hours.
Table 4. Amidation Results with 2-Pyrrolidinone GC Relative Area % for Components 2-pyrrolidinone 8.6;
Octanoic acid 82.;9 Octanoyl amido acid 7 54 Mole % Conversion of 2-~rrolidinone to Components 2-pyrrolidinone 68 g Octanoyl amido acid 31.2 EXAMPLE XXII
,, Scale-u~ Synthesis of C_g Amidocaproic Acid - A 250 mL, 3-neck, round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a purge tube through which nitrogen is passed through the reaction mixture The reaction vessel is charged with caprolactam ( 15.00 g, 0.131 mol), octanoic acid (76.10 g, 0.525 mol), and p-toluenesulfonic acid ( 1.26 g. 0.0065 mol) The reaction is kept at 200°C for 4 hours using a high temperature oil bath, continuously purging with nitrogen. After 4 hours reaction time. the reaction mixture is analyzed by GC to determine % conversion of caprolactam to amido acid (see Table 5). Reaction mixture is brown after 4 hours. Caprolactam and octanoic acid are removed by vacuum distillation (90-100°C, 4.3 mm) to give the desired C8 amido acid as a brown solution (20.8 g) with the analysis as shown in Table 5.
Table 5. Amidation Results of Scale-up Reaction Reaction Product (after GC Relative Area % for Components Mixture distillation) Caprolactam 6.36 3.61 Octanoic acid 76.18 1.22 6-aminocaproic acid 0.28 0.56 Octanoylcaprolactam 1.12 I . 26 Octanoyl amido acid 14.43 76.04 Octanoyl diamido acid ---- 12.62 Mole % Conversion of C~rolactam to Components (before distillation Caprolactam 4 I . I
6-aminocaproic acid 1.0 Octanoylcaprolactam 5.6 Octanoyl amido acid 52.4 In addition to the above, the amidation reaction can be conducted usin~, benzoic acid and caprolactam with methanesulfonic acid plus boric acid to provide benzoylamide caproic acid ESTERIFICATION EXAMPLES XXIII-XXVI
Synthesis of C8 Amidocaproic Acid Phenyl Ester - .A 100 mL, 3-neck.
round bottom flask is fitted with thermometer, Dean-Stark trap with condenser, magnetic stir bar, and a purge tube through which nitrogen is passed through the reaction mixture. The reaction vessel is charged with C8 amido acid - made from C8 acid chloride and aminocaproic acid - ( 10 g, 0.037 mol, I mol equivalent), phenol, sulfuric acid 98°~0, and boric acid. The reaction is kept at 180-195°C for 4 hours using a high temperature oil bath held at ?OS-210°C.
ll ~U4~36 o;
continuously sparging Some of with nitrogen. the phenol is optionally removed with a Dean-Stark trap.
After 4 hours reaction time, the reaction mixture is analyzed by GC (see GC n of Analysis Method) to determine C8 % conversio amidocaproic acid to C8 Other amidocaproic acid phenyl ester (see Table 61 products formed are caprolactam. anoic acid octanoic acid, oct phenyl ester, aminocaproic acid. Reaction mixture color after 4 hours is noted.
Table 6. Esterification Results with C8 Amidocaproic Acid Example # XXTII XXIV XXV
Phenol (mol equivalent) 20 5.7 15 Sulfuric acid (mol equivalent)0.25 0.25 0.05 Boric acid (mol equivalent)0.07 0.07 0.05 phenol removed 50% removed50% removed no phenol during firstduring first removed min 30 min Reaction color after 4 orange orange yellow hr GC Relative Area % for Components Caprolactam 1.28 10.16 7.41 Octanoic acid 0.12 4.22 l .87 6-aminocaproic acid 0.1 0.39 I .61 Octanoic acid phenyl ester4.71 28.89 16.33 Octanoylcaprolactam 0.91 1.18 2.62 Octanoyl amido acid 0.58 8.9 46.39 Octanoyl amido acid phenyl82.04 37.07 23.76 ester Octanoyl diamido acid 3.95 0 0 Octanoyl diamido acid 0 2.71 0 phenyl ester Mole % Conversion of Amido Acid to Components Caprolactam 3 . 7 15 .4 I 1.4 6-aminocaproic acid 0.3 0.3 l .3 Octanoic acid phenyl ester13.2 36.8 ~ I
.2 Octanoylcaprolactam 1.1 I .4 3 I
Octanoyl amido acid 1.2 7.6 40.2 Octanoyl amido acid phenyl76.2 31.3 20.3 ester Octanoyl diamido acid 3.8 0 0 Octanoic acid 0 4 5 5 2 5 Octanoyl diamido acid 0 1 7 0 phenyl ester ~ ~~~n 2-~
Table 6. continued Example # XXVI
Phenol (mol equivalent) 20 Sulfuric acid (mol equivalent)0.25 Boric acid (mol equivalent)0.07 phenol removed 50% removed during first 40 min Reaction color after yellow 4 hr GC Relative Area % for Components Caprolactam 3 .60 Octanoic acid 0.37 6-aminocaproic acid 0 Octanoic acid phenyl 12.54 ester Octanoylcaprolactam 1.36 Octanoyl amido acid 5.95 Octanoyl amido acid phenyl67.46 ester Octanoyl diamido acid 2.14 Mole % Conversion of Octanovl Amido Acid to Components Caprolactam 6.3 6-aminocaproic acid 0 Octanoic acid phenyl 18.4 ester Octanoylcaprolactam 1.8 Octanoyl amido acid 5.8 Octanoyl amido acid phenyl65.5 ester Octanoyl diamido acid 1.6 Octanoic acid 0.6 EXAMPLE XXVII
Scale-~ Synthesis of C8 Amidocaproic Acid Phenyl Ester - A 250 mL, 3-neck, round bottom with thermometer, condenser.
flask is fitted magnetic stir bar, and a sparge tube h nitrogen is passed through through whic the reaction mixture. The reaction vessel is charged with C8 amidocaproic acid - product of Example 17 -(20.8 g, 0.081 mol), phenol ( 152.3 g, 1.62 mol), sulfuric acid 98%
(2.03 g, 0.02 mol), and boric acid (0.35 ~, 0.0057 mol). The reaction is kept at 200 C for 4 hours using perature oil bath. continuously a high tem pur'iny= with 2170488 .:
nitrogen. During the first hour. of reaction time. 50 mL of phenol is removed via the Dean-Stark trap. After 4 hours reaction time. the reaction mixture is analyzed by GC to determine % conversion of C8 amidocaproic acid to C8 amidocaproic acid phenyl ester (see Table 5). Reaction mixture is brown after hours. Phenol is removed by vacuum distillation (90-100°C. 4.3 mm) to give the desired C8 amido acid phenyl ester as a brown solution (31.6 g) with the analysis shown in Table 7.
Table 7. Esterification Results of Scale-up Reaction GC Relative Area % for Components Reaction Product (after Mixture distillation?
Caprolactam 3.47 3.97 Octanoic acid 0 0 6-aminocaproic acid 0 0.29 Octanoic acid phenyl ester 8.33 5.~9 Octanoylcaprolactam 1.17 0 Octanoyl amido acid 3.68 0 Octanoyl amido acid phenyl ester 48.77 63.07 Octanoyl diamido acid 10.08 1 1.10 Octanoyl diamido acid phenyl ester 2.07 8.22 Mole % Conversion of Caprolactam to Components Caprolactam 7, 5 7. 7 6-aminocaproic acid 0 0 Octanoic acid phenyl ester l5.1 8.6 Octanoylcaprolactam 2.0 0 Octanoyl amido acid 4.5 0 Octanoyl amido acid phenyl ester ~ 60.1 67.8 Octanoyl diamido acid 9.1 9.0 Octanoyl diamido acid phenyl ester 1.8 6.6 SULFONATION EXAMPLE XXVIII
Synthesis of C8 Amidocaproic Acid Phenyl Ester Sulfonate - C8 Amidocaproic acid phenyl ester (22.00 g, 0.0634 mol) is placed in 100 mL ?-neck round-bottom fitted with a glass tube reaching the bottom of the flask and a condenser connected to a bubbler. The flask is heated to SO°C in an oil bath to melt the phenyl ester. Sulfur trioxide (5.0 g, 2.6 mL, 0.0634 mol) vapor diluted with nitrogen is added to the reaction over 1 hour through the glass tube.
[The glass tube is connected via TeflonTM tubing to another flask heated at 65°C in n r which liquid sulfur trioxide is placed. Nitrogen is bubbled through the liquid sulfur trioxide to obtain the gas mixture.] The reaction is then heated at 50°C
for an additional 30 minutes after the sulfur trioxide addition. The reaction is allowed to cool to room temperature and then poured into saturated aqueous sodium bicarbonate. The product precipitates as a white solid and is collected by vacuum filtration. After drying, the product ( 17.7 g) is obtained in 65%
yield.
TRANSESTERIFICATION EXAMPLE XXIX
Synthesis of C 10 Amidocaproic Acid Phenyl Ester - Amido acid ( I 00 ~, 0.0039 mol), phenyl acetate ( 1.59 g, 0.012 mol), and sodium acetate (0.032 ~, 0.00039 mol) are placed in a 100 mL round-bottom flask fitted with condenser The solution is heated at 210 C for 0.5 hr under nitrogen. Then acetic acid and excess phenyl acetate are removed by vacuum distillation with a Kugelrohr apparatus. The product ( 1.10 g) is obtained as a white solid which contains unreacted amido acid and excess phenyl acetate. HN1MR of crude reaction mixture indicates -75% yield (by integration ratio of the 2.58 ppm resonance -CH2C(=O)OPh - to the 3.16 resonance - C(=O)NHCH2,~.
TRANSESTERIFICATION EXAMPLE XXX
Synthesis of CIO Amidocaproic Acid Phenyl Ester Sulfonate - lnto a 100 mL, 3 neck round bottom flask fitted with a nitrogen sparge tube, magnetic stirrer, Dean-Stark trap with condenser, and thermometer, is added C 10 amido acid (48.5 g, 0.17 mol), sodium acetoxybenzenesulfonate ( 15 g, 0.057 mol), and sodium acetate (0.94 g, 0.114 mol). The reaction is kept at 200°C for 3 hr using a high temperature oil bath held at 205-210° C, continuously spargin~
with nitrogen. Distillate (7 mL) is collected in the Dean-Stark trap. The reaction is poured hot into a mortar and after cooling is ground into a powder H1VMR of crude reaction mixture indicates -90% yield (by integration ratio of the 2.58 ppm resonance - CH~C(=O)OPhS03Na - to the 3.16 resonance -C(=O)NHCH2~ . The reaction mixture is recrystallized from methanol (370- mL.) to obtain a first crop ( 15.1 g) and a second crop (4.7 g) of desired product (75%
recrystallized yield based on sodium acetoxybenzenesulfonate) ESTERIFICATION EXAMPLE XXXI
Synthesis of C 10 Amidocaproic Acid Phenyl Ester Sulfonate - Into a 100 mL, 3 neck round bottom flask fitted with a nitro~7en spar~_e tube.
ma~__=netic stirrer, Dean-Stark trap with condenser, and thermometer, is added C I 0 amido acid (3.5 g, 0.0123 mol), acetic anhydride (0.46 ~, 0.0045 mol), and methanesulfonic acid (0.002 g, 0.00002 mol). The reaction mixture is heated at ~1~U4~6 100°C for 2 hr. to form the amido acid anhydride. Then anhydrous sodium phenolsulfonate (0.80 g, 0.0041 mol) and sodium acetate (0.017 ~. 0 0002 mol) is added and the reaction heated at 180°C for 1 5 hr. At the be~,innin~, the reaction is fluid, but at the end it is a thick paste. HNMR of crude reaction mixture indicates -70% yield (by integration ratio of the 2.58 ppm resonance -CH2C(=O)OPh - to the 3.16 resonance - C(=O)NHCH2~ .
ESTERIFICATION EXAMPLE XXXII
Synthesis of C8 Amidoca~roic Acid Phenyl Ester Sulfonate - Into a 250 mL. 3 neck round bottom flask fitted with a nitrogen sparge tube, magnetic stirrer.
Dean-Stark trap with condenser, and thermometer, is added C8 amidocaproic acid ( 10.0 g, 0.039 mol), acetic anhydride ( 17.9 g, 0.175 mol), sodium acetate (0.16 g, 0.002 mol), and imidazole (0.13 g, 0.002 mol). The reaction mixture is heated at 110°C for 3 hr with a nitrogen sparge; 10 mL of distillate is collected in the Dean-Stark trap. Then acetic acid and excess acetic anhydride is removed by vacuum distillation to obtain amido acid anhydride. The crude amido acid anhydride is dispersed in ether (60 mL), filtered, and dried to obtain nearly pure amido acid anhydride (indicated by HIVMR) as a white solid (8.6 g).
Into a 100 mL, 3 neck round bottom flask fitted with a nitrogen sparge tube, magnetic stirrer, condenser, and thermometer, is added a portion of the pure amido acid anhydride (3.5 g, 0.0071 mol), anhydrous sodium phenolsulfonate ( 1.11 g, 0.0056 mol), sodium acetate (0.029 g, 0.0004 mol), and toluene ( l2 rnL). The reaction is refluxed 3 hr 180°C. A small, homogeneous aliquot of the reaction mixture is taken and evaporated for HNMR analysis. HNMR indicates 75% yield based on sodium phenolsulfonate (by integration ratio of the 2 58 ppm resonance - CH2C(=O)OPh - to the 3.16 resonance - C(=O)NHCH2~. Then additional toluene (50 mL) is added, the reaction mixture filtered hot, and the precipitate dried to obtain the desired product as a white solid (2.6 ~) which is 54% pure by HNMR (by integration ratio of the 2.58 ppm resonance -CH2C(=O)OPh - to the 3.16 resonance - C(=O)NHCH2,~ . The remainder of the material is amido acid, sodium phenol sulfonate, and acetoxybenzenesulfonate.
The following illustrates the use of the amido acids and bleach activators of this invention in otherwise conventional consumer goods. but is not intended to be limiting thereof.
EXAMPLE XXXIII
A mild lubricious soap bar composition is prepared in conventional extrusion apparatus, as follows. The bar resists dry crackin~~ and wet smear Ingredient Percent 1 wt.
2~ ~ ~,4~~
C 16_ 1 g fatty acid soap* 7g.0 Amido acid** 6 0 NaCI/KC1 ( 1:1 wt. ) 0. 5 C 12H33C(O)N-methylglucamide g.0 Water and minors Balance * 1:1 (wt.) mixture of Na and K soaps **Per Example I, above.
EXAMPLE XXXIII
A laundry bleaching system suitable for use alone or in admixture with a conventional granular laundry detergent is as follows.
Ingredient Percent (wt.) Sodium percarbonate 90.0 Bleach activator* 10.0 *Per Example XXVIII, above.
The foregoing composition can be added at levels of to water l00 ppm, and above, to provide a fabric bleaching action.
AMIDATION EXAMPLES I-XV
Synthesis of C8-Amidocaproic Acid - A 100 mL, 3-neck, round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a purge tube through which nitrogen is passed through the reaction mixture. The reaction vessel is charged with caprolactam (4.00 g, 0.036 mol, 1 mol equivalent), octanoic acid, the indicated strong acid catalyst (TSA, MSA, PSA, PPA, SA, as described in the tables), and optionally boric acid. The reaction is kept at the designated temperature for 4 hours using a high temperature oil bath, continuously purging with nitrogen. After 4 hour reaction time, the reaction mixture is analyzed by GC (see GC Analysis Method) to determine conversion of caprolactam to amido acid (see Table 1 ). Reaction mixture color after 4 hours is also noted.
Table 1. Amidation Results Example # I II III IV V
Octanoic acid (mol equivalent) 4 4 4 4 2 Strong acid catalyst* (mol equivalent) 0.1 0.05 0.1 0.05 0. I
TSA TSA TSA TSA TSA
Boric acid (mol equivalent) ----- 0.05 ----- ----- _--__ Water (mol equivalent) ----- ----- ----- 0 2 _-___ Temperature (°C) 200 200 175 220 200 Reaction color after 4 hr brown brown yellow brown brown GC Relative Area % for Components Caprolactam 3.59 3.82 I 0.33 3 56 9 09 Octanoic acid 74.97 73.23 79.21 74 79 62.96 6-aminocaproic acid 0.12 0 1.12 0.26 0 Octanoylcaprolactam 2.37 3.0? 0 94 3.67 1 48 Octanoyl amido acid 15 95 17.24 6 49 I 5 6 19 1 Octanoyl diamido acid 1.63 1.21 0.62 0 89 5 07 Mole % Conversion of Caprolactam to Components Caprolactam 23.7 23.3 66 ?2.9 39 6-aminocaproic acid 0.4 0 3 0 0 Octanoylcaprolactam 12.1 14.3 4 18.3 5 0 Octanoyl amido acid 59.2 59.3 23.4 56 4 46 Octanoyl diamido acid 4.5 3.1 I 2.4 9 2 .7 *Key to abbreviations: 99%), SA
TSA (toluenesulfonic acid M
monohydrate (methanesulfonic acid 99%), lsulfoniccid SA (sulfuric acid 98%), a PSA (pheno 65%), PA (polyphosphoric acid) Table 1. continued Example # VI VII VIII IX X
Octanoic acid (mol equivalent)4 4 4 4 4 Strong acid catalyst* (mol0.05 0.05 0.05 0.05 U US
equivalent) MSA MSA MSA PSA PPA
Boric acid (mol equivalent)----- ----- 0.05 0.05 -----Water (mol equivalent) ----- 0.2 ---------- -----Temperature (C) 200 200 200 200 200 Reaction color after 4 brown brown yellowblack yellow hr GC Relative Area % for Components Caprolactam 5.08 3.86 3.68 8 99 6.64 Octanoic acid 73.5 74.06 72.3678.29 71 6-aminocaproic acid 0 0 0 0.60 0 Octanoylcaprolactam 3.41 2.40 3.08 1.26 4.02 Octanoyl amido acid 15.75 17.07 17.358.91 15.03 Octanoyl diamido acid 0.90 1.23 2.02 0.62 0 98 Mole % Conversion of Caprolactam to Components Caprolactam 30.0 24.4 22.1 57 8 35 6-aminocaproic acid 0 0 0 2. I 0 Octanoylcaprolactam 15.6 1 1.7 14.3 6.3 16 Octanoyl amido acid 52.2 60.6 58.5 32.2 45 Octanoyl diamido acid 2.2 3.3 5.1 1.7 ?.?
Table 1. continued Example # XI XII XIII XIV ?CV
Octanoic acid (mol equivalent)4 4 4 4 I
Strong acid catalyst* (mol0.01 0.05 0 0 ?4 0 O
equivalent) 05 i SA SA SA SA SA
Boric acid (mol equivalent)0.05 0.05 0 0 05 0 05 ,~17p4g6 Water (mol equivalent) ----- 1 0.2 0.4 - ----Temperature (C) 210 200 200 200 200 Reaction color after 4 hr black yellow black black black GC Relative Area % for Components Caprolactam 3.22 7.54 3 88 2.6 21 Octanoic acid 72.41 78.54 73.68 78.24 40 6-aminocaproic acid 0.14 1.47 0.44 2.41 0.22 Octanoylcaprolactam 2.33 0.17 0 51 0 33 0 Octanoyl amido acid 17.46 9.53 18.21 13.58 23.34 Octanoyl diamido acid 2.61 1.28 2.46 1.38 9.85 Mole % Conversion of Caprolactam To Components Caprolactam 20.2 52.6 24.6 21.0 >3.5 6-aminocaproic acid 0 5.5 1.5 I 0 4 0.3 Octanoylcaprolactam 11.3 0.9 2.5 2.0 0.9 Octanoyl amido acid 61.6 3 7.4 64.9 61. 8 3 .
Octanoyl diamido acid 6.9 3 .7 6.5 4. 7 t U.4 *Key to abbreviations: TSA (toluenesulfonic acid monohydrate 99%), MSA
(methanesulfonic acid 99%), SA (sulfuric acid 98%), PSA (phenolsulfonic acid 65%), PA (polyphosphoric acid) EXAMPLES XVI-XVIII
Synthesis of C8-Amidocaproic Acid - A 100 ml, 3-neck round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a spare tube through which nitrogen is passed through the reaction mixture. The reaction vessel is charged with caprolactam (4.00 g, 0.036 mol, 1 mol equivalent), octanoic acid, boric acid, and water. The reaction is kept at the designated temperature for 3.5 hr using a high temperature oil bath, continuously sparing with nitrogen. After 3.5 hr reaction time, the reaction mixture is analvz.ed by GC
(see GC Analysis Method) to determine % conversion of the caprolactam to amido acid (see Table 2). Other products formed are 6-aminocaproic acid, octanoyl caprolactam, and octanoyl diamido acid. Reaction mixture color after 3.5 hr is also noted.
Table 2. Amidation Results Example # XVI XVII
XVIII
Octanoic acid (mol equivalent) 4 8 ~_ boric acid (mol equivalent) 0.025 0.05 0 025 water (mol equivalent) 0.1 0. I 0 I
temperature (C) 235 220 23s reaction color after 4 hours yellow yellow oran<~e GC Relative Area % for Components caprolactam 3.46 1.39 6 42 octanoic acid 71.57 85.06 55.01 6-aminocaproic acid 0 0 0 octanoylcaprolactam 4.71 1.18 3.49 octanoyl amido acid 15.44 10.33 26.09 octanoyl diamido acid 1.74 0.39 5.37 Mole % Conversion of Caprolactam to Components caprolactam 20.9 16.8 24 7 6-aminocaproic acid 0 0 0 octanoylcaprolactam 22.1 I 1.1 10.4 octanoyl amido acid 52.6 70.2 56.3 octanoyl diamido acid 4.4 2.0 8.6 EXAMPLES XIX-XX
Synthesis of C8-Amidoc~roic Acid - A 100 ml, 3-neck round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a sparge tube through which nitrogen is passed through the reaction mixture. The reaction vessel is charged with caprolactam (4.00 g, 0.036 mol, 1 mol equivalent), octanoic acid, methanesulfonic acid, and boric acid. The reaction is kept at the designated temperature for 6.5 hr using a high temperature oil bath, continuously sparging with nitrogen. The reaction is then allowed to cool to room temperature and water is added. The reaction is allowed to stir at room temperature for 18 hr. Before water addition (Example XIX) and 18 hr after water addition (Example XX), the reaction mixture is analyzed by GC (see GC
Analysis Method) to determine % conversion of caprolactam to amido acid (see Table 3). Other products formed are 6-aminocaproic acid, octanoyl caprolactam, and octanoyl diamido acid. Reaction mixture color is also noted.
Table 3. Amidation Results Example # XIX XX
Octanoic acid (mol equivalent) 9.28 9.28 boric acid (mol equivalent) O OS 0 05 water (mol equivalent) ---- 0 I
methanesulfonic acid (mol 0.1 0.01 equivalent) temperature (C) 235 250 reaction color orange orange GC Relative Area % for Components caprolactam 0.60 I 39 octanoic acid 84.89 8 5 06 6-aminocaproic acid 0 0 octanoylcaprolactam 2.75 1.18 octanoyl amido acid 6.36 10 3 octanoyl diamido acid 0 0 39 Mole % Conversion of Caprolactam to Components caprolactam 9.5 I6 8 6-aminocaproic acid 0 0 octanoylcaprolactam 33 . 8 1 1.1 octanoyl amido acid 56.8 70.2 octanoyl diamido acid 0 2 0 EXAMPLE XXI
Synthesis of C8 Amidobutyric Acid - A 100 mL, 3-neck, round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a purge tube through which nitrogen is passed through the reaction mixture The reaction vessel is charged with 2-pyrrolidinone (2.00 g, 0.024 mol), octanoic acid ( I
3.56 g, 0.094 mol), and sulfuric acid 98% (0.12 g, 0.0012 mol). The reaction is kept at 200°C for 4 hours using a high temperature oil bath, continuously purging with nitrogen. After 4 hour reaction time, the reaction mixture is analyzed by GC (see Table 2). A 31% conversion of pyrrolidinone to amido acid is obtained The reaction mixture is brown after 4 hours.
Table 4. Amidation Results with 2-Pyrrolidinone GC Relative Area % for Components 2-pyrrolidinone 8.6;
Octanoic acid 82.;9 Octanoyl amido acid 7 54 Mole % Conversion of 2-~rrolidinone to Components 2-pyrrolidinone 68 g Octanoyl amido acid 31.2 EXAMPLE XXII
,, Scale-u~ Synthesis of C_g Amidocaproic Acid - A 250 mL, 3-neck, round bottom flask is fitted with thermometer, condenser, magnetic stir bar, and a purge tube through which nitrogen is passed through the reaction mixture The reaction vessel is charged with caprolactam ( 15.00 g, 0.131 mol), octanoic acid (76.10 g, 0.525 mol), and p-toluenesulfonic acid ( 1.26 g. 0.0065 mol) The reaction is kept at 200°C for 4 hours using a high temperature oil bath, continuously purging with nitrogen. After 4 hours reaction time. the reaction mixture is analyzed by GC to determine % conversion of caprolactam to amido acid (see Table 5). Reaction mixture is brown after 4 hours. Caprolactam and octanoic acid are removed by vacuum distillation (90-100°C, 4.3 mm) to give the desired C8 amido acid as a brown solution (20.8 g) with the analysis as shown in Table 5.
Table 5. Amidation Results of Scale-up Reaction Reaction Product (after GC Relative Area % for Components Mixture distillation) Caprolactam 6.36 3.61 Octanoic acid 76.18 1.22 6-aminocaproic acid 0.28 0.56 Octanoylcaprolactam 1.12 I . 26 Octanoyl amido acid 14.43 76.04 Octanoyl diamido acid ---- 12.62 Mole % Conversion of C~rolactam to Components (before distillation Caprolactam 4 I . I
6-aminocaproic acid 1.0 Octanoylcaprolactam 5.6 Octanoyl amido acid 52.4 In addition to the above, the amidation reaction can be conducted usin~, benzoic acid and caprolactam with methanesulfonic acid plus boric acid to provide benzoylamide caproic acid ESTERIFICATION EXAMPLES XXIII-XXVI
Synthesis of C8 Amidocaproic Acid Phenyl Ester - .A 100 mL, 3-neck.
round bottom flask is fitted with thermometer, Dean-Stark trap with condenser, magnetic stir bar, and a purge tube through which nitrogen is passed through the reaction mixture. The reaction vessel is charged with C8 amido acid - made from C8 acid chloride and aminocaproic acid - ( 10 g, 0.037 mol, I mol equivalent), phenol, sulfuric acid 98°~0, and boric acid. The reaction is kept at 180-195°C for 4 hours using a high temperature oil bath held at ?OS-210°C.
ll ~U4~36 o;
continuously sparging Some of with nitrogen. the phenol is optionally removed with a Dean-Stark trap.
After 4 hours reaction time, the reaction mixture is analyzed by GC (see GC n of Analysis Method) to determine C8 % conversio amidocaproic acid to C8 Other amidocaproic acid phenyl ester (see Table 61 products formed are caprolactam. anoic acid octanoic acid, oct phenyl ester, aminocaproic acid. Reaction mixture color after 4 hours is noted.
Table 6. Esterification Results with C8 Amidocaproic Acid Example # XXTII XXIV XXV
Phenol (mol equivalent) 20 5.7 15 Sulfuric acid (mol equivalent)0.25 0.25 0.05 Boric acid (mol equivalent)0.07 0.07 0.05 phenol removed 50% removed50% removed no phenol during firstduring first removed min 30 min Reaction color after 4 orange orange yellow hr GC Relative Area % for Components Caprolactam 1.28 10.16 7.41 Octanoic acid 0.12 4.22 l .87 6-aminocaproic acid 0.1 0.39 I .61 Octanoic acid phenyl ester4.71 28.89 16.33 Octanoylcaprolactam 0.91 1.18 2.62 Octanoyl amido acid 0.58 8.9 46.39 Octanoyl amido acid phenyl82.04 37.07 23.76 ester Octanoyl diamido acid 3.95 0 0 Octanoyl diamido acid 0 2.71 0 phenyl ester Mole % Conversion of Amido Acid to Components Caprolactam 3 . 7 15 .4 I 1.4 6-aminocaproic acid 0.3 0.3 l .3 Octanoic acid phenyl ester13.2 36.8 ~ I
.2 Octanoylcaprolactam 1.1 I .4 3 I
Octanoyl amido acid 1.2 7.6 40.2 Octanoyl amido acid phenyl76.2 31.3 20.3 ester Octanoyl diamido acid 3.8 0 0 Octanoic acid 0 4 5 5 2 5 Octanoyl diamido acid 0 1 7 0 phenyl ester ~ ~~~n 2-~
Table 6. continued Example # XXVI
Phenol (mol equivalent) 20 Sulfuric acid (mol equivalent)0.25 Boric acid (mol equivalent)0.07 phenol removed 50% removed during first 40 min Reaction color after yellow 4 hr GC Relative Area % for Components Caprolactam 3 .60 Octanoic acid 0.37 6-aminocaproic acid 0 Octanoic acid phenyl 12.54 ester Octanoylcaprolactam 1.36 Octanoyl amido acid 5.95 Octanoyl amido acid phenyl67.46 ester Octanoyl diamido acid 2.14 Mole % Conversion of Octanovl Amido Acid to Components Caprolactam 6.3 6-aminocaproic acid 0 Octanoic acid phenyl 18.4 ester Octanoylcaprolactam 1.8 Octanoyl amido acid 5.8 Octanoyl amido acid phenyl65.5 ester Octanoyl diamido acid 1.6 Octanoic acid 0.6 EXAMPLE XXVII
Scale-~ Synthesis of C8 Amidocaproic Acid Phenyl Ester - A 250 mL, 3-neck, round bottom with thermometer, condenser.
flask is fitted magnetic stir bar, and a sparge tube h nitrogen is passed through through whic the reaction mixture. The reaction vessel is charged with C8 amidocaproic acid - product of Example 17 -(20.8 g, 0.081 mol), phenol ( 152.3 g, 1.62 mol), sulfuric acid 98%
(2.03 g, 0.02 mol), and boric acid (0.35 ~, 0.0057 mol). The reaction is kept at 200 C for 4 hours using perature oil bath. continuously a high tem pur'iny= with 2170488 .:
nitrogen. During the first hour. of reaction time. 50 mL of phenol is removed via the Dean-Stark trap. After 4 hours reaction time. the reaction mixture is analyzed by GC to determine % conversion of C8 amidocaproic acid to C8 amidocaproic acid phenyl ester (see Table 5). Reaction mixture is brown after hours. Phenol is removed by vacuum distillation (90-100°C. 4.3 mm) to give the desired C8 amido acid phenyl ester as a brown solution (31.6 g) with the analysis shown in Table 7.
Table 7. Esterification Results of Scale-up Reaction GC Relative Area % for Components Reaction Product (after Mixture distillation?
Caprolactam 3.47 3.97 Octanoic acid 0 0 6-aminocaproic acid 0 0.29 Octanoic acid phenyl ester 8.33 5.~9 Octanoylcaprolactam 1.17 0 Octanoyl amido acid 3.68 0 Octanoyl amido acid phenyl ester 48.77 63.07 Octanoyl diamido acid 10.08 1 1.10 Octanoyl diamido acid phenyl ester 2.07 8.22 Mole % Conversion of Caprolactam to Components Caprolactam 7, 5 7. 7 6-aminocaproic acid 0 0 Octanoic acid phenyl ester l5.1 8.6 Octanoylcaprolactam 2.0 0 Octanoyl amido acid 4.5 0 Octanoyl amido acid phenyl ester ~ 60.1 67.8 Octanoyl diamido acid 9.1 9.0 Octanoyl diamido acid phenyl ester 1.8 6.6 SULFONATION EXAMPLE XXVIII
Synthesis of C8 Amidocaproic Acid Phenyl Ester Sulfonate - C8 Amidocaproic acid phenyl ester (22.00 g, 0.0634 mol) is placed in 100 mL ?-neck round-bottom fitted with a glass tube reaching the bottom of the flask and a condenser connected to a bubbler. The flask is heated to SO°C in an oil bath to melt the phenyl ester. Sulfur trioxide (5.0 g, 2.6 mL, 0.0634 mol) vapor diluted with nitrogen is added to the reaction over 1 hour through the glass tube.
[The glass tube is connected via TeflonTM tubing to another flask heated at 65°C in n r which liquid sulfur trioxide is placed. Nitrogen is bubbled through the liquid sulfur trioxide to obtain the gas mixture.] The reaction is then heated at 50°C
for an additional 30 minutes after the sulfur trioxide addition. The reaction is allowed to cool to room temperature and then poured into saturated aqueous sodium bicarbonate. The product precipitates as a white solid and is collected by vacuum filtration. After drying, the product ( 17.7 g) is obtained in 65%
yield.
TRANSESTERIFICATION EXAMPLE XXIX
Synthesis of C 10 Amidocaproic Acid Phenyl Ester - Amido acid ( I 00 ~, 0.0039 mol), phenyl acetate ( 1.59 g, 0.012 mol), and sodium acetate (0.032 ~, 0.00039 mol) are placed in a 100 mL round-bottom flask fitted with condenser The solution is heated at 210 C for 0.5 hr under nitrogen. Then acetic acid and excess phenyl acetate are removed by vacuum distillation with a Kugelrohr apparatus. The product ( 1.10 g) is obtained as a white solid which contains unreacted amido acid and excess phenyl acetate. HN1MR of crude reaction mixture indicates -75% yield (by integration ratio of the 2.58 ppm resonance -CH2C(=O)OPh - to the 3.16 resonance - C(=O)NHCH2,~.
TRANSESTERIFICATION EXAMPLE XXX
Synthesis of CIO Amidocaproic Acid Phenyl Ester Sulfonate - lnto a 100 mL, 3 neck round bottom flask fitted with a nitrogen sparge tube, magnetic stirrer, Dean-Stark trap with condenser, and thermometer, is added C 10 amido acid (48.5 g, 0.17 mol), sodium acetoxybenzenesulfonate ( 15 g, 0.057 mol), and sodium acetate (0.94 g, 0.114 mol). The reaction is kept at 200°C for 3 hr using a high temperature oil bath held at 205-210° C, continuously spargin~
with nitrogen. Distillate (7 mL) is collected in the Dean-Stark trap. The reaction is poured hot into a mortar and after cooling is ground into a powder H1VMR of crude reaction mixture indicates -90% yield (by integration ratio of the 2.58 ppm resonance - CH~C(=O)OPhS03Na - to the 3.16 resonance -C(=O)NHCH2~ . The reaction mixture is recrystallized from methanol (370- mL.) to obtain a first crop ( 15.1 g) and a second crop (4.7 g) of desired product (75%
recrystallized yield based on sodium acetoxybenzenesulfonate) ESTERIFICATION EXAMPLE XXXI
Synthesis of C 10 Amidocaproic Acid Phenyl Ester Sulfonate - Into a 100 mL, 3 neck round bottom flask fitted with a nitro~7en spar~_e tube.
ma~__=netic stirrer, Dean-Stark trap with condenser, and thermometer, is added C I 0 amido acid (3.5 g, 0.0123 mol), acetic anhydride (0.46 ~, 0.0045 mol), and methanesulfonic acid (0.002 g, 0.00002 mol). The reaction mixture is heated at ~1~U4~6 100°C for 2 hr. to form the amido acid anhydride. Then anhydrous sodium phenolsulfonate (0.80 g, 0.0041 mol) and sodium acetate (0.017 ~. 0 0002 mol) is added and the reaction heated at 180°C for 1 5 hr. At the be~,innin~, the reaction is fluid, but at the end it is a thick paste. HNMR of crude reaction mixture indicates -70% yield (by integration ratio of the 2.58 ppm resonance -CH2C(=O)OPh - to the 3.16 resonance - C(=O)NHCH2~ .
ESTERIFICATION EXAMPLE XXXII
Synthesis of C8 Amidoca~roic Acid Phenyl Ester Sulfonate - Into a 250 mL. 3 neck round bottom flask fitted with a nitrogen sparge tube, magnetic stirrer.
Dean-Stark trap with condenser, and thermometer, is added C8 amidocaproic acid ( 10.0 g, 0.039 mol), acetic anhydride ( 17.9 g, 0.175 mol), sodium acetate (0.16 g, 0.002 mol), and imidazole (0.13 g, 0.002 mol). The reaction mixture is heated at 110°C for 3 hr with a nitrogen sparge; 10 mL of distillate is collected in the Dean-Stark trap. Then acetic acid and excess acetic anhydride is removed by vacuum distillation to obtain amido acid anhydride. The crude amido acid anhydride is dispersed in ether (60 mL), filtered, and dried to obtain nearly pure amido acid anhydride (indicated by HIVMR) as a white solid (8.6 g).
Into a 100 mL, 3 neck round bottom flask fitted with a nitrogen sparge tube, magnetic stirrer, condenser, and thermometer, is added a portion of the pure amido acid anhydride (3.5 g, 0.0071 mol), anhydrous sodium phenolsulfonate ( 1.11 g, 0.0056 mol), sodium acetate (0.029 g, 0.0004 mol), and toluene ( l2 rnL). The reaction is refluxed 3 hr 180°C. A small, homogeneous aliquot of the reaction mixture is taken and evaporated for HNMR analysis. HNMR indicates 75% yield based on sodium phenolsulfonate (by integration ratio of the 2 58 ppm resonance - CH2C(=O)OPh - to the 3.16 resonance - C(=O)NHCH2~. Then additional toluene (50 mL) is added, the reaction mixture filtered hot, and the precipitate dried to obtain the desired product as a white solid (2.6 ~) which is 54% pure by HNMR (by integration ratio of the 2.58 ppm resonance -CH2C(=O)OPh - to the 3.16 resonance - C(=O)NHCH2,~ . The remainder of the material is amido acid, sodium phenol sulfonate, and acetoxybenzenesulfonate.
The following illustrates the use of the amido acids and bleach activators of this invention in otherwise conventional consumer goods. but is not intended to be limiting thereof.
EXAMPLE XXXIII
A mild lubricious soap bar composition is prepared in conventional extrusion apparatus, as follows. The bar resists dry crackin~~ and wet smear Ingredient Percent 1 wt.
2~ ~ ~,4~~
C 16_ 1 g fatty acid soap* 7g.0 Amido acid** 6 0 NaCI/KC1 ( 1:1 wt. ) 0. 5 C 12H33C(O)N-methylglucamide g.0 Water and minors Balance * 1:1 (wt.) mixture of Na and K soaps **Per Example I, above.
EXAMPLE XXXIII
A laundry bleaching system suitable for use alone or in admixture with a conventional granular laundry detergent is as follows.
Ingredient Percent (wt.) Sodium percarbonate 90.0 Bleach activator* 10.0 *Per Example XXVIII, above.
The foregoing composition can be added at levels of to water l00 ppm, and above, to provide a fabric bleaching action.
Claims (39)
1. A method for preparing amido acids of the formula wherein R is a C1 or higher hydrocarbyl substituent and R1 is C2-C10 hydrocarbylene substituent by reacting in the presence of an acid catalyst a carboxylic acid of the formula with a lactam of the structure wherein R and R1 are as described before.
2. A method according to Claim 1 wherein the acid catalyst is a member selected from the group consisting of sulfuric acid, methanesulfonic acid, trifluoromethanesulfonic acid, phosphoric acid, boric acid and mixtures thereof
3. A method according to Claim 2 wherein the acid catalyst is a mixture comprising boric acid.
4. A method according to Claim 2 wherein water is added in an amount of from about 0.1 to about 1 molar equivalent, based on the lactam.
5. A method according to Claim 1 which is conducted at a temperature from about 150°C to about 250°C.
6. A method according to Claim 1 wherein R is C6-C17 and R1 is -(CH2)x-, wherein x is from 2 to 10.
7. A method according to Claim 6 wherein the lactam is selected from caprolactam and valerolactam.
8. A method according to Claim 7 wherein the carboxylic acid has substituent R as C6-C17.
9. A method according to Claim 1 wherein the molar ratio of the carboxylic acid reactant to the lactam reactant is at least about 2:1.
10. A reaction according to Claim 9 wherein the molar ratio of the carboxylic acid:lactam is in the range of 3:1 to 4:1 and wherein the reaction is conducted without added solvent.
11. A method for preparing amido acid phenyl esters of the formulas comprising (a) preparing, according to the method of Claim 1, an amido acid, or mixture thereof, of the formulas (b) reacting the amido acid, or mixture thereof, of step (a) with phenol in the presence of a strong acid catalyst and boric acid;
wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent.
wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent.
12. A method according to Claim 11 wherein the acidic catalyst is a member selected from the group consisting of sulfuric acid, methanesultonic acid, toluenesulfonic acid, trifluoromethanesulfonic acid, phosphonic acid and mixtures thereof.
13. A method according to Claim 12 wherein the mole ratio of boric acid to the acidic catalysis is at least about 1:1.
14. A method according to Claim 11 which is conducted at a temperature in the range from about 180°C to about 210°C without added solvent.
15. A method according to Claim 11 which is conducted at a temperature of about 180-190°C in the absence of solvent, with 98% sulfuric acid as the acidic catalyst, and at a mole ratio of boric acid to sulfuric acid of at least about 1:3.6.
16. A method according to Claim 11 wherein R is C6-C17 and R1 is (CH2)x wherein x is from 2 to 5.
17. A method for preparing bleach activators which are amido acid phenyl ester sulfonates, or mixtures thereof, of the formulas:
wherein R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent, the sulfonate group is ortho or para substituted, and M is a canon moiety, said method comprising sulfonating and neutralizing an amido acid phenyl ester of Formulas III or IV, or mixtures thereof, prepared according to Claim 11.
wherein R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent, the sulfonate group is ortho or para substituted, and M is a canon moiety, said method comprising sulfonating and neutralizing an amido acid phenyl ester of Formulas III or IV, or mixtures thereof, prepared according to Claim 11.
18. A method according to Claim 17 wherein R is C6-C17 and R1 is (CH2)x wherein x is from 2 to 5.
19. A method for preparing amido acid phenyl esters of the formulas comprising (a) preparing, according to the method of Claim 1, an amido acid, or mixture thereof, of the formulas (b) reacting the amido acid, or mixture thereof, of step (a) with a phenyl ester of a lower molecular weight carboxylic acid moiety in the presence of a basic catalyst;
wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent.
wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent.
20. A method according to Claim 19 wherein the basic catalyst is a member selected from the group consisting of carboxylate salts, carbonates, imidazole, and mixtures thereof.
21. A method according to Claim 19 wherein the molar ratio of amido acid to phenyl ester is at least about 1:1.
22. A method according to Claim 19 wherein R is C6-C17 and R1 is (CH2)x wherein x is from 2 to 5.
23. A method for preparing bleach activators which are amido acid phenyl ester sulfonates, or mixtures thereof, of the formulas:
wherein R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent, the sulfonate group is ortho or para substituted, and M is a cation moiety, said method comprising sulfonating and neutralizing an amido acid phenyl ester of Formulas III or IV, or mixtures thereof; prepared according to Claim 19
wherein R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent, the sulfonate group is ortho or para substituted, and M is a cation moiety, said method comprising sulfonating and neutralizing an amido acid phenyl ester of Formulas III or IV, or mixtures thereof; prepared according to Claim 19
24. A method according to Claim 23 wherein R is C6-C17 and R1 is (CH2)x wherein x is from 2 to 5.
25. A method for preparing bleach activators which are amido acid phenyl ester sulfonates, or mixtures thereof, of the formulas:
said method comprising (a) preparing, according to the method of Claim 1, an amido acid. or mixtures thereof, of the formulas:
(b) reacting the amido acid, or mixtures thereof, of step (a) with an ester derivative of phenol sulfonic acid or salt of the formula:
wherein in each of the above formulas R is a C 1 or higher hydrocarbyl substituent, R1 is a C2-C10 hydrocarbylene substituent, R2 is an acid moiety, and M is a cationic moiety.
said method comprising (a) preparing, according to the method of Claim 1, an amido acid. or mixtures thereof, of the formulas:
(b) reacting the amido acid, or mixtures thereof, of step (a) with an ester derivative of phenol sulfonic acid or salt of the formula:
wherein in each of the above formulas R is a C 1 or higher hydrocarbyl substituent, R1 is a C2-C10 hydrocarbylene substituent, R2 is an acid moiety, and M is a cationic moiety.
26. A method according to Claim 25 wherein M is hydrogen and R2 is a lower molecular weight carboxylic acid moiety.
27. A method according to Claim 26 wherein R is C6-C17 and R1 is (CH2)x wherein x is from 2 to 5.
28. A method according to Claim 25 wherein M is a member selected from monovalent metal salts and divalent metal salts, and R2 is a lower molecular weight carboxylic acid moiety.
29. A method according to Claim 28 wherein R is C6-C17 and R1 is (CH2)x wherein x is from 2 to 5.
30. A method for preparing bleach activators which are amido acid phenyl ester sulfonates, or mixtures thereof, of the formulas:
and said method comprising the steps of (a) preparing, according to the method of Claim 1, an amido acid, or mixture thereof, having the formulas:
(b) reacting the amido acid, or mixtures thereof, of step (a) with a lower C4-molecular weight carboxylic acid anhydride to form the amido acid anhydride;
and (c) reacting the amido acid anhydride, or mixture thereof, of step (b) with phenolsulfonate salt to form the amido acid phenyl ester sulfonate, wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent, R1 is a C2-C10 hydrocarbylene substituent, and M is a cationic moiety.
and said method comprising the steps of (a) preparing, according to the method of Claim 1, an amido acid, or mixture thereof, having the formulas:
(b) reacting the amido acid, or mixtures thereof, of step (a) with a lower C4-molecular weight carboxylic acid anhydride to form the amido acid anhydride;
and (c) reacting the amido acid anhydride, or mixture thereof, of step (b) with phenolsulfonate salt to form the amido acid phenyl ester sulfonate, wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent, R1 is a C2-C10 hydrocarbylene substituent, and M is a cationic moiety.
31. A method according to Claim 30 wherein in step (a) the lower molecular weight carboxylic acid anhydride is selected from anhydrides having the formula (R3CO)2O, wherein each R3 is the same or different C1-C4 hydrocarbyl substituents.
32. A method according to Claim 31 wherein the lower molecular weight carboxylic acid anhydride is acetic anhydride.
33. A method according to Claim 30 wherein the molar ratio of amido acid to carboxylic acid anhydride is in the range from about 1:3 to 5:1.
34. A method according to Claim 30 wherein in step (b) the amido acid anhydride is reacted with sodium phenolsulfonate salt.
35. A method according to Claim 30 wherein R is C6-C17 and R1 is (CH2)x wherein x is from 2 to 5.
36. A method for preparing amido acid phenyl esters of the formulas comprising reacting, with phenol in the presence of a non-boric acid acidic catalyst and boric acid, an amido acid, or mixture thereof, of the formulas wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent
37. A method for preparing amido acid phenyl esters of the formulas comprising reacting, with phenyl ester of a lower molecular weight carboxylic acid moiety in the presence of a basic catalyst, an amido acid. or mixture thereof.
of the formulas wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent.
of the formulas wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent and R1 is a C2-C10 hydrocarbylene substituent.
38. A method for preparing bleach activators which are amido acid phenyl ester sulfonates, or mixtures thereof, of the formulas:
said method comprising reacting an amido acid, or mixtures thereof, of the formulas:
with an ester derivative of phenol sulfonic acid or salt of the formula.
wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent, R1 is a C2-C10 hydrocarbylene substituent, R2 is an acid moiety, and M is a cationic moiety.
said method comprising reacting an amido acid, or mixtures thereof, of the formulas:
with an ester derivative of phenol sulfonic acid or salt of the formula.
wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent, R1 is a C2-C10 hydrocarbylene substituent, R2 is an acid moiety, and M is a cationic moiety.
39. A method for preparing bleach activators which are amido acid phenyl ester sulfonates, or mixtures thereof, of the formulas:
said method comprising the steps of (a) reacting an amido acid, or mixture thereof, having the formulas:
with a lower C4-C10 molecular weight carboxylic acid anhydride to form the amido acid anhydride; and (b) reacting the amido acid anhydride of step (a) with phenolsulfate salt to form the amido acid phenyl ester sulfonate, wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent, R1 is a C2-C10 hydrocarbylene substituent, and M is a cationic moiety.
said method comprising the steps of (a) reacting an amido acid, or mixture thereof, having the formulas:
with a lower C4-C10 molecular weight carboxylic acid anhydride to form the amido acid anhydride; and (b) reacting the amido acid anhydride of step (a) with phenolsulfate salt to form the amido acid phenyl ester sulfonate, wherein in each of the above formulas R is a C1 or higher hydrocarbyl substituent, R1 is a C2-C10 hydrocarbylene substituent, and M is a cationic moiety.
Applications Claiming Priority (3)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| US121,013 | 1993-09-14 | ||
| US08/121,013 US5414099A (en) | 1993-09-14 | 1993-09-14 | Synthesis of amido acids from carboxylic acids and lactams |
| PCT/US1994/009965 WO1995007883A1 (en) | 1993-09-14 | 1994-09-01 | Synthesis of amido acids from carboxylic acids and lactams |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| CA2170486A1 CA2170486A1 (en) | 1995-03-23 |
| CA2170486C true CA2170486C (en) | 2000-03-28 |
Family
ID=22393922
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA002170486A Expired - Fee Related CA2170486C (en) | 1993-09-14 | 1994-09-01 | Synthesis of amido acids from carboxylic acids and lactams |
Country Status (10)
| Country | Link |
|---|---|
| US (2) | US5414099A (en) |
| EP (2) | EP0884306A3 (en) |
| JP (1) | JPH09502717A (en) |
| AT (1) | ATE178885T1 (en) |
| CA (1) | CA2170486C (en) |
| DE (1) | DE69417904T2 (en) |
| DK (1) | DK0719250T3 (en) |
| ES (1) | ES2129671T3 (en) |
| GR (1) | GR3029956T3 (en) |
| WO (1) | WO1995007883A1 (en) |
Families Citing this family (17)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US5414099A (en) * | 1993-09-14 | 1995-05-09 | The Procter & Gamble Company | Synthesis of amido acids from carboxylic acids and lactams |
| WO1996028413A1 (en) * | 1995-03-16 | 1996-09-19 | Hoechst Celanese Corporation | Synthesis of amidocarboxylic acid derivatives |
| US5837670A (en) * | 1995-04-18 | 1998-11-17 | Hartshorn; Richard Timothy | Detergent compositions having suds suppressing properties |
| US5945392A (en) * | 1995-06-20 | 1999-08-31 | Procter & Gamble Company | Nonaqueous, particulate-containing detergent compositions |
| DE19609953A1 (en) * | 1996-03-14 | 1997-09-18 | Basf Ag | Solid composition of heterocyclic compounds and / or oxime esters and inert porous support materials and their use as a stable bleach activator component in detergents, bleaches and cleaners |
| DE69716761T2 (en) | 1996-12-17 | 2003-07-03 | Procter & Gamble | METHOD FOR PRODUCING N- (ALKANOYL) AMINOALKANOYLOXYBENZENE SULFONATES |
| EP1005451A2 (en) | 1997-08-20 | 2000-06-07 | The Procter & Gamble Company | Process for preparing and/or purifying amido acid phenyl ester sulfonates |
| EP1131285A2 (en) | 1998-11-20 | 2001-09-12 | The Procter & Gamble Company | Improved synthesis of bleach activators |
| US6448430B1 (en) | 1999-09-10 | 2002-09-10 | Eastman Chemical Company | Process for the preparation of aryl carboxylate esters |
| US6448431B1 (en) | 1999-09-13 | 2002-09-10 | Eastman Chemical Company | Production of aryl carboxylate esters |
| US6500973B2 (en) | 2000-06-02 | 2002-12-31 | Eastman Chemical Company | Extractive solution crystallization of chemical compounds |
| US6660712B2 (en) | 2000-06-02 | 2003-12-09 | Dale Elbert Van Sickle | Stabilization of amido acids with antioxidants |
| EP1292566A2 (en) | 2000-06-02 | 2003-03-19 | Eastman Chemical Company | Process for hydrolyzing amido-carboxylic acid esters into amido-carboxylic acids |
| US6498124B2 (en) | 2000-06-02 | 2002-12-24 | Eastman Chemical Company | Isolation of phenyl ester salts from mixtures comprising sulfolane |
| ATE286876T1 (en) | 2000-06-02 | 2005-01-15 | Eastman Chem Co | PHENYL ESTER SALTS PURIFICATION |
| US7425527B2 (en) | 2004-06-04 | 2008-09-16 | The Procter & Gamble Company | Organic activator |
| FR3007759B1 (en) * | 2013-06-28 | 2015-07-24 | Arkema France | CAPROLACTAM BASED FATTY AMIDE AS A HYDROGELING ADDITIVE. |
Family Cites Families (13)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US2956068A (en) * | 1956-08-28 | 1960-10-11 | Henkel & Compagnie G M B H | Preparation of acylamino carboxylic acids |
| GB1177099A (en) * | 1967-12-20 | 1970-01-07 | Hydrierwerk Rodleben Veb | Process for the production of omega-Acyl Amino Caproic Acid |
| NL7100453A (en) * | 1970-01-30 | 1971-08-03 | ||
| DE3377490D1 (en) * | 1982-09-28 | 1988-09-01 | Procter & Gamble | Synthesis of hydrophilic phenol ester derivatives |
| US4634551A (en) * | 1985-06-03 | 1987-01-06 | Procter & Gamble Company | Bleaching compounds and compositions comprising fatty peroxyacids salts thereof and precursors therefor having amide moieties in the fatty chain |
| GB8415909D0 (en) * | 1984-06-21 | 1984-07-25 | Procter & Gamble Ltd | Peracid compounds |
| US4852989A (en) * | 1987-05-08 | 1989-08-01 | The Procter & Gamble Company | Bleaching compounds and compositions comprising fatty peroxyacids salts thereof and precursors therefor having amide moieties in the fatty chain |
| CA2063071C (en) * | 1991-03-25 | 2004-11-23 | Thomas B. Ottoboni | Method for sulfonating acyloxybenzenes and neutralization of resulting product |
| US5153341A (en) * | 1991-03-25 | 1992-10-06 | E. I. Du Pont De Nemours And Company | Process for preparing benzenesulfonate salts |
| JP3107426B2 (en) * | 1991-10-21 | 2000-11-06 | 三井化学株式会社 | Method for producing N-methyl-β-alanine |
| JP2923101B2 (en) * | 1991-10-22 | 1999-07-26 | 三井化学株式会社 | Method for producing N-long-chain acylamino acid type surfactant |
| EP0719249A1 (en) * | 1993-09-14 | 1996-07-03 | The Procter & Gamble Company | Synthesis of amido acids from carboxylic acid esters and amino acid salts |
| US5414099A (en) * | 1993-09-14 | 1995-05-09 | The Procter & Gamble Company | Synthesis of amido acids from carboxylic acids and lactams |
-
1993
- 1993-09-14 US US08/121,013 patent/US5414099A/en not_active Expired - Fee Related
-
1994
- 1994-09-01 AT AT94928005T patent/ATE178885T1/en not_active IP Right Cessation
- 1994-09-01 DE DE69417904T patent/DE69417904T2/en not_active Expired - Fee Related
- 1994-09-01 CA CA002170486A patent/CA2170486C/en not_active Expired - Fee Related
- 1994-09-01 JP JP7509231A patent/JPH09502717A/en active Pending
- 1994-09-01 ES ES94928005T patent/ES2129671T3/en not_active Expired - Lifetime
- 1994-09-01 EP EP98114127A patent/EP0884306A3/en not_active Withdrawn
- 1994-09-01 DK DK94928005T patent/DK0719250T3/en active
- 1994-09-01 WO PCT/US1994/009965 patent/WO1995007883A1/en active IP Right Grant
- 1994-09-01 EP EP94928005A patent/EP0719250B1/en not_active Expired - Lifetime
-
1995
- 1995-02-23 US US08/392,599 patent/US5534642A/en not_active Expired - Fee Related
-
1999
- 1999-04-15 GR GR990400889T patent/GR3029956T3/en unknown
Also Published As
| Publication number | Publication date |
|---|---|
| GR3029956T3 (en) | 1999-07-30 |
| DK0719250T3 (en) | 1999-10-25 |
| EP0884306A3 (en) | 1999-12-22 |
| ATE178885T1 (en) | 1999-04-15 |
| EP0719250A1 (en) | 1996-07-03 |
| JPH09502717A (en) | 1997-03-18 |
| WO1995007883A1 (en) | 1995-03-23 |
| EP0884306A2 (en) | 1998-12-16 |
| DE69417904T2 (en) | 1999-11-25 |
| EP0719250B1 (en) | 1999-04-14 |
| US5414099A (en) | 1995-05-09 |
| US5534642A (en) | 1996-07-09 |
| ES2129671T3 (en) | 1999-06-16 |
| DE69417904D1 (en) | 1999-05-20 |
| CA2170486A1 (en) | 1995-03-23 |
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