US20030105423A1 - Suspension device and method - Google Patents
Suspension device and method Download PDFInfo
- Publication number
- US20030105423A1 US20030105423A1 US10/328,483 US32848302A US2003105423A1 US 20030105423 A1 US20030105423 A1 US 20030105423A1 US 32848302 A US32848302 A US 32848302A US 2003105423 A1 US2003105423 A1 US 2003105423A1
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- Prior art keywords
- agent
- network
- container
- patient
- syringe
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61M—DEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
- A61M5/00—Devices for bringing media into the body in a subcutaneous, intra-vascular or intramuscular way; Accessories therefor, e.g. filling or cleaning devices, arm-rests
- A61M5/14—Infusion devices, e.g. infusing by gravity; Blood infusion; Accessories therefor
- A61M5/1407—Infusion of two or more substances
- A61M5/1409—Infusion of two or more substances in series, e.g. first substance passing through container holding second substance, e.g. reconstitution systems
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61M—DEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
- A61M5/00—Devices for bringing media into the body in a subcutaneous, intra-vascular or intramuscular way; Accessories therefor, e.g. filling or cleaning devices, arm-rests
- A61M5/007—Devices for bringing media into the body in a subcutaneous, intra-vascular or intramuscular way; Accessories therefor, e.g. filling or cleaning devices, arm-rests for contrast media
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61M—DEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
- A61M5/00—Devices for bringing media into the body in a subcutaneous, intra-vascular or intramuscular way; Accessories therefor, e.g. filling or cleaning devices, arm-rests
- A61M5/14—Infusion devices, e.g. infusing by gravity; Blood infusion; Accessories therefor
- A61M5/142—Pressure infusion, e.g. using pumps
- A61M5/145—Pressure infusion, e.g. using pumps using pressurised reservoirs, e.g. pressurised by means of pistons
- A61M5/1452—Pressure infusion, e.g. using pumps using pressurised reservoirs, e.g. pressurised by means of pistons pressurised by means of pistons
Definitions
- the invention relates to a device and method of using the device for providing a suspended volume of an agent without additional mixing.
- Agents that do not persist in a suspended state and sediment must be resuspended prior to use.
- a pharmaceutical colloid such as a contrast agent that is injected into a patient to enhance an imaging procedure.
- Contrast agents are used in various types of imaging including x-ray, magnetic resonance imaging (MRI), computed tomography (CT) and ultrasound (US).
- MRI magnetic resonance imaging
- CT computed tomography
- US ultrasound
- a contrast agent that comes out of suspension must be resuspended before placing the desired volume to be dosed into a delivery container such as a syringe. If there is a delay before the dose is injected into a patient, for example while preparing the patient or equipment, or if the infusion is extended, the agent must again be suspended before or during administration.
- Resuspension of contrast agent requires mechanical manipulations, for example, removing a filled syringe positioned in an injector and remixing its contents. Additional remixing steps may delay a critical infusion time or, if remixing is omitted, the entire imaging procedure may have to be repeated due to suboptimal contrast obtained. Duplicate procedures not only put patients at increased risk and inconvenience, but are also cost- and time-inefficient. Even if the need to resuspend a single bolus injection is not prohibitive for a given procedure, repeated bolus injections or long term continuous infusions can become problematic due to agent coming out of suspension during administration.
- the invention is directed to a device that provides a suspended agent without additional mechanical mixing.
- the device divides a total volume of a sedimenting agent into a network of sub-volumes and has prots for an inflow and outflow of a propellant fluid to releases the sub-volumes of agent from the device.
- the device is located within a container in which the agent is packaged, such as a vial or bottle, or in a container in which the agent is dosed, such as a syringe or bag, or in a container containing the propellant fluid.
- the device is located external to a container for the propellant fluid. In this embodiment, the device may be operably attached to an exit port of the propellant fluid container.
- the device may be positioned in-line at any point with lines that connect the propellant fluid container with a patient connector.
- the device is comprised of a network of sub-volumes that may take the form of one or more tubes, cells and/or sponges, and that may assume any configuration such as a parallel, stairstep, helical, random and/or coiled configuration.
- the network may be retained in a network holder.
- the invention is also directed to a suspension device for a volume of an agent in which a container for the propellant fluid has a network of grooves that are integral with the container and that retain a sub-volume of the agent within the grooves.
- the container has a plug that occupies an internal volume of the container and the grooves are either integral with an internal wall of the container, or are integral with an external wall of the plug.
- the plug diverts the propellant fluid flow to a variable extent from the center of the container to the periphery of the container, thus diverting fluid flow through the grooves.
- the grooves may further contain substantially perpendicular channels at regular intervals to allow uniform filling of the grooves with the agent.
- the invention is also directed to a method of providing a volume of suspended agent to a patient.
- the method includes dividing the volume of agent into contained sub-volumes, storing the sub-volumes in a network for containing sub-volumes of the agent and providing a propellant fluid under pressure to eject the sub-volumes of agent through the network and into a patient.
- the propellant fluid may be housed in a container in which the network is also located.
- the network may be external to the propellant fluid container, with the network positioned either in-line between a source of propellant fluid and a patient, or adjacent an exit port of a propellant fluid container.
- the invention is also directed to a suspension device for a folume of an imaging contrast agent.
- a network contains a plurality of sub-volumes of the agent and has inflow and outflow ports for propellant fluid.
- the device may also have a container and network holder external to the container.
- FIG. 1 is a cross-sectional view of a syringe container with an internal tubular network.
- FIG. 1A is a view similar to FIG. 1 of an alternate embodiment of the invention.
- FIG. 2 is a cross-sectional view of a syringe container with an external tubular network operably attached to a propellant fluid container exit port.
- FIG. 3 is an elevational view of an in-line device.
- FIGS. 4A, 4B and 4 C are various network embodiments and configurations.
- FIG. 5 is a cross-sectional view of a syringe container having an integral network.
- FIG. 6 is a cross-sectional view of an integral network with channels.
- the device of the invention sub-divides a desired volume of an agent to suspend the agent without mechanical mixing. Resuspension is caused by viscous fluid flow through the network of sub-volumes.
- the device is comprised of a network of structures for containing sub-volumes of the agent, with the entire volume of agent contained in the network component sub-volumes.
- the device may be located in the same container that contains propellant fluid to eject the agent from the network (container package embodiment).
- the device may be located adjacent an exit port of a propellant fluid container (add-on embodiment), or may be positioned in-line at any point in a fluid path between the propellant fluid container and the ultimate deposit site such as a patient (in-line embodiment).
- a propellant fluid is one that is used to eject the agent from the network of tubes, cells, etc.
- a network is defined as a collection of structures which contain the entire desired volume of agent in sub-volumes, and hence increase the surface area of the agent over which the propellant fluid must flow, in the device.
- the network has a common exit port, and agent sub-volumes are ejected from the network at a substantially equal rate.
- the network may encompass tubes, cells, sponges, etc. and is not limited by volume or configuration.
- the device sub-divides a volume of an agent to prevent it from settling or sedimenting into one or a few dense aggregates without the need for mechanical mixing or suspending prior to use, and thus reduces or eliminates the problem of remixing or resuspending an agent that has come out of suspension prior to use.
- Use may be either preparing an injection dose by transferring the desired volume of agent from a package to a dosing container such as syringe, or injecting the dosing volume of agent into a patient. This problem may occur with contrast agents, either while in their package or portioned in a container such as a syringe for injecting into a patient about to undergo an imaging procedure.
- the invention solves the problem by subdividing the volume of the agent to prevent separation or aggregation of the agent from the suspending liquid.
- Dividing a uniformly suspended contrast agent or other agent into a network of sub-volumes rather than a single large volume inhibits the particles from either floating or precipitating into one or more larger masses or aggregates.
- the invention thus reduces or obviates the need for mixing before or during a process, such as an infusion process. This increases the quality, safety, and cost- and time- efficiencies of the process.
- a network 8 a containing divided sub-volumes of an agent 12 is internal to a container 10 for propellant fluid 16 .
- the container 10 may be a syringe 14 or other types of containers which include but are not limited to vials, bags having flexible or semi-flexible walls, bottles of either glass or plastic, etc.
- the agent 12 contained in the network 8 a is ejected from the container 10 as propellant fluid 16 flows through the network 8 a and displaces the agent 12 .
- the propellant fluid 16 is any viscous fluid (liquid or gas) that is biocompatible.
- the propellant fluid may be a diluent for the agent 12 such as normal saline, water, buffer, etc.
- the propellant fluid 16 may also be a contrast agent that is different from the agent 12 injected for the imminent imaging procedure.
- the network 8 a may be any structure that serves to contain a sub-volume of the desired total volume of an agent 12 in a unit area.
- the network 8 a may be contained in a network holder 22 .
- the network 8 a may be tubes 18 which, as used herein, encompass tubules, microtubules, channels, or other types of hollow cylinders that convey a fluid or that function as a passageway, whereby a volume of agent 12 is divided into sub-volumes of any size.
- the tubes 18 may be in any configuration, such as one or more coils or helices, an angular or stairstep configuration, and/or even random configurations.
- a collection of tubes 18 may similarly be one or more coils or helices, an angular or stairstep configuration, and/or even random configurations, or may be arranged in a parallel configuration (FIG. 1A).
- the geometries and configurations of the network 8 may be combined in either regular or random configurations. While FIGS. 1 and 1A show tubes 18 positioned in a syringe 14 without any accompanying support, other configurations are contemplated.
- the tubes 18 may be positioned within a network holder 22 (FIGS. 2 and 3), or may be supported or held in a syringe 14 or network holder 22 by a fixture such as 24 (shown in phantom lines in FIG. 1) which may extend for part of or all of the length of the network 8 .
- a dose delivery container 10 that is a syringe 14 is shown with a network holder 22 containing the network 8 external to the syringe 14 .
- the network 8 c is packaged within a network holder 22 , which may be any container in which the network is housed or retained and may be made of any biocompatable material.
- the network holder 22 containing the network 8 c may be separable from the syringe 14 or other container 10 and attached to an exit port 24 of the syringe 14 or container 10 .
- the network holder 22 for the network 8 c may also be manufactured as part of the container 10 , which may be useful as a pre-packaged embodiment of the invention.
- the network holder 22 may be attached to an exit port 24 using, for example, connectors 26 such as luer fittings.
- the exit port 24 of the syringe 14 may be fitted with luer fittings, such as Luer-Lok® caps (Becton-Dickinson), or may have luer fittings such as metal, brass or glass luer tips attached.
- a support or fixture 30 for the tubes 28 may be used, and the support 30 and tubes 28 may be contained in a network holder 22 .
- the support 30 and tubes 28 may be contained directly in the container 10 .
- the tubes 28 in a network holder 22 may be unsupported as shown in FIG. 2.
- FIG. 2 illustrates a network holder 22 which is attached to a syringe 14
- the network (not shown) contained in a network holder 22 is shown in an in-line embodiment.
- the network holder 22 is fashioned with connectors 26 at both an inflow port 32 and an outflow port 34 .
- Tubing is connected to connectors 26 to carry propellant fluid 16 from a syringe to holder 22 and from holder 22 to a patient.
- the connectors 26 may be the same or different at the inflow 32 and outflow 34 ports and may be any type such as luer fittings, as previously described.
- Network holder 22 and the network inside may be configured symmetrically, so that the orientation of the network holder 22 in an in-flow embodiment need not be a concern; i.e., there is no back-to-front or front-to-back limitation.
- Agent 12 can be removed from the network within the network holder 22 upon pressure from a propellant fluid 16 .
- a network 8 that is internal to a container 10 such as a syringe 14 need not be housed in a network holder 22 .
- the network 8 a , 8 b of tubes 18 or other structures may be positioned directly within the barrel 36 of the syringe 14 .
- the network 8 that is internal to a syringe 14 or other container 10 may also be housed in a network holder 22 .
- the barrel 36 of the syringe 14 may contain a propellant fluid 16 that, upon initiation of flow, provides pressure to release or eject the agent 12 from the network 8 .
- the propellant fluid 16 need not be pre-filled in the barrel 36 of the syringe 14 , but instead may be added to the barrel 36 of the syringe 14 .
- the sub-dividing volume structure of tubes 18 in the network 8 may assume a variety of geometries and configurations. As shown in FIGS. 1A, 2, 4 A, 4 B and 4 C, the tubes 18 may be straight, coiled, helical, in random filaments 38 , in an angular or stairstep (not shown) configuration, or may have other configurations. All of these alternatives are appropriate for use in any of the illustrated embodiments.
- the sub-dividing network 8 need not encompass tubes 18 at all; all shown in FIGS. 4A, 4B and 4 C, the network 8 d , 8 e and 8 f respectively, may be a series of discrete cells 42 (see FIG. 4B), or may have a sponge 44 type of structure (see FIG. 4A).
- the agent 12 is retained in or on discreet cells 42 .
- the agent 12 is either absorbed in or adsorbed on the sponge 44 , rather than contained within tubes 18 or cells 42 .
- a cell 42 or sponge 44 structure may also be used effectively in a network holder 22 separate from a syringe 14 .
- the network 8 may be configured so that there is a non-uniform direction for all sub-volumes, that is, there is no single upward, downward or lateral direction for all sub-volumes.
- a network 8 g that is integral with the container 10 is shown.
- the network 8 g is fabricated as grooves or channels 48 that are etched or otherwise manufactured within the container 10 itself.
- a syringe 14 may have a cylindrical plug 46 disposed in the barrel 36 , where the plug 46 has parallel or spiral grooves 48 in its outer surface.
- the grooves 48 contain the agent 12 between the syringe 14 inner wall 50 and barrel 36 .
- the grooves 48 may contain substantially perpendicular channels 60 at one or more regularly spaced intervals. The channels 60 permit rapid and uniform filling of the network 8 with agent 12 added into one side of a container 10 when the other side of the container 10 is sealed.
- the syringe 14 has a cylindrical plug 46 disposed in the barrel 36 as previously described, where the inner wall 50 of the syringe 14 has parallel or spiral grooves in its structure.
- the grooved structures 48 may also be used in a separate network holder 22 .
- the grooved structure 48 comprises the network 8 which sub-divides the volume of agent 12 . It will thus be appreciated that the network 8 may assume a variety of forms and configurations whereby a volume of agent 12 can be sub-divided into smaller volumes with increased surface area of the agent 12 over which the propellant fluid 16 flows to reduce sedimentation.
- the network 8 may be made of any biocompatable material that can withstand sterilization and is inert with respect to the agent 12 , the propellant fluid 16 , and the container 10 .
- biocompatable tubing such as polyethylene, polypropylene, silicon, rubber, etc., for example, Tygon® tubing (halogenated vinyl plastic, Norton Plastics).
- Tubes 18 used in kidney dialysis devices, such as cellulose tubes 18 having a nominal diameter of 200 ⁇ m, may also be used in the invention.
- the cells 42 may be produced by incomplete fusion of pieces of fusable material such as thermoplastics or metals.
- the cells 42 may be made of DelrinTM, polycarbonate such as LexanTM, polyethylene, polypropylene, silicon, rubber, etc.
- the sponge 44 may be made of porous DelrinTM, porpous polycarbonate such as LexanTM, porous polyethylene, porous polypropylene, porous silicon, porous rubber, etc.
- the size and volume of the network 8 , container 10 , and network holder 22 may vary, depending upon a number of factors. These factors include the volume of agent 12 , the size of the container 10 , the duration of the imaging or other procedure to be performed, etc. There is neither a maximum nor a minimum volume for the network 8 , container 10 , or network holder 22 , and an exponential range of volumes is contemplated by the invention. For embodiments in which the network 8 is internal or integral with the container 10 , however, the volume of agent 12 contained within the network 8 is at most one-half the volume of propellant fluid 16 in the container 10 . This ensures that substantially all the agent 12 will be released from the network 8 by the flow of propellant fluid 16 .
- volumes of contrast agent 12 injected for enhanced ultrasound imaging may range from 1 ml to about 10 ml.
- a 3 ml volume of agent would require using about a 10 ml syringe 14 , with the tubular 18 or other structure of the network 8 containing 3 ml agent 12 and the remaining volume of the syringe 14 containing at least 3 ml, and more typically 4-5 ml, of propellant fluid 16 .
- a 3 ml volume of agent 12 may be sub-divided in a syringe 14 having ten threads or grooves 48 per inch, with the threads or grooves 48 one millimeter deep, each thread or groove 48 containing about 0.3 ml agent 12 .
- the container 10 and/or network holder 22 may be manufactured having the network 8 preloaded with a uniformly mixed suspension of agent 12 such as a pharmaceutical colloid.
- the container 10 and/or network holder 22 may have both an entry port 54 and an exit port 56 with appropriate fittings 26 such as luer locks for connection to standard tubing or catheters, as is known to one skilled in the art (FIG. 3).
- propellant fluid 16 may be injected into the entry port 54 or, alternatively, pressure may be applied to the propellant fluid 16 already in the container 10 .
- the container 10 may also have a single exit port 56 and a plunger 58 , with liquid 60 in the opposite end, to permit use as a prefilled syringe (FIG. 1).
- the specific location, position and configuration of the network 8 may depend upon an intended use.
- an agent containing a gas other than air should be housed in a container 10 that has been purged of air.
- a container 10 made of glass may be rendered air-tight more easily than a plastic syringe, and thus is preferable for this agent.
- a network 8 that is internal rather than external is preferred for use with an agent that contains a gas other than air. This allows the propellant fluid 16 to be purged of air and become saturated with the agent-containing gas, maintaining a substantially anaerobic environment prior to injection.
- One advantage of the invention is that it eliminates the need for resuspension of agents 12 that may come out of suspension, either in their original container 10 or in a dose delivery container such as a syringe 14 .
- Conventional containers 10 require mechanical devices or manipulations to maintain colloids such as a contrast agent 12 in suspension.
- the device and method of the present invention provides a competitive advantage for injectable agents 12 .
- a syringe 14 having a network 8 containing agent 12 can remain resuspendable for more than five months.
- Maintaining the agent 12 in a substantially fully resuspendable state assures consistent quality and reduced sensitivity to user technique.
- the agent 12 may be shipped already prepackaged in the network 8 .
- This arrangement has the potential to reduce susceptibility of agents, such as microbubble preparations, to mechanical vibration and shock which may decrease the integrity of the agent 12 .
- Dividing the volume of agent 12 into sub-volumes also allows it to be more quickly preheated to a desired temperature, facilitating the efficiency of the entire imaging procedure.
- colloid or other agent 12 may be released, ejected or expelled from the exit port 56 of the container 10 by injecting a propellant fluid 16 . This precludes the need to draw the pharmaceutical or contrast agent 12 into a syringe 14 for injection, and provides similar advantages as enjoyed by pre-filled syringes.
- Still another advantage of the invention is that, in those embodiments such as FIGS. 2 and 3 where network 8 is external to the syringe 14 , the exit port 56 of the dose delivery container 10 or network holder 22 may be connected to a short angiocatheter (not shown) that is very close to a venous or arterial puncture site in a patient.
- This arrangement prevents loss of suspension of agent 12 that would occur inside a longer catheter, and permits use of a manual or power syringe located a substantial distance away from the patient, while preventing the need for the agent 12 to maintain resuspendable in the manual or power syringe 14 and connecting tubing.
- the manual or power syringe and tubing need only contain a non-colloidal fluid that does not require mixing or resuspending during long injection times.
- a further advantage of the invention is realized with an optional built-in plunger 58 in the syringe 14 .
- a built-in plunger 58 permits use of the device as a manual syringe 14 or with a small, battery-operated power injector at the end of a very short angiocatheter.
- the filled syringe 14 could be located very close to a venous or arterial puncture site, precluding the need to maintain the agent 12 resuspended in a long catheter for infusion into a patient.
- This embodiment also precludes the need for a fluid-filled syringe 14 connected to the entry port 54 of the dose delivery container 10 in order to eject the agent 12 from the exit port 56 of the dose delivery container 10 .
- the embodiments of the present invention shown and described in the specification are exemplary embodiments contemplated by the inventor and are not limiting in any way.
- the invention is not limited to use in the clinical area and may be used in research applications, as well as in other industries where uniformly suspended agents are needed, such as the food and beverage industries.
- the propellant fluids 16 may also include oils, epoxy resins, sugars, etc., depending upon the application. Therefore, various changes, modifications or alterations to these embodiments may be made or resorted to without departing from the spirit of the invention and the scope of the following claims.
Abstract
A device and method for providing a suspended agent such as a contrast agent without mechanical resuspension. A volume of agent (12) is divided into sub-volumes in a network (8) of tubes (18), cells (42), sponges (44), grooves (48), etc. A propellant fluid (16) flows through the network (8) to release the suspended agent (12). The network (8) may be internal to a container (10) for the propellant fluid (16). Alternatively, the network (8) may be adjacent an exit port (24) of a container (10) for the propellant fluid (16), or may be in-line between a propellant fluid container (10) and a patient. The invention reduces sedimentation of agents into one or a few aggregates and eliminates a mechanical mixing step. The invention thus provides a uniformly suspended agent, improving patient health and safety and increasing cost and time savings.
Description
- This application is a divisional of U.S. application Ser. No. 09/316,315 filed May 21, 1999, now pending and expressly incorporated by reference herein in its entirety.
- The invention relates to a device and method of using the device for providing a suspended volume of an agent without additional mixing.
- Agents that do not persist in a suspended state and sediment must be resuspended prior to use. One example of an agent that must be resuspended prior to use is a pharmaceutical colloid, such as a contrast agent that is injected into a patient to enhance an imaging procedure. Contrast agents are used in various types of imaging including x-ray, magnetic resonance imaging (MRI), computed tomography (CT) and ultrasound (US). A contrast agent that comes out of suspension must be resuspended before placing the desired volume to be dosed into a delivery container such as a syringe. If there is a delay before the dose is injected into a patient, for example while preparing the patient or equipment, or if the infusion is extended, the agent must again be suspended before or during administration.
- Resuspension of contrast agent requires mechanical manipulations, for example, removing a filled syringe positioned in an injector and remixing its contents. Additional remixing steps may delay a critical infusion time or, if remixing is omitted, the entire imaging procedure may have to be repeated due to suboptimal contrast obtained. Duplicate procedures not only put patients at increased risk and inconvenience, but are also cost- and time-inefficient. Even if the need to resuspend a single bolus injection is not prohibitive for a given procedure, repeated bolus injections or long term continuous infusions can become problematic due to agent coming out of suspension during administration.
- The loss of suspension for a contrast agent at any point in a delivery system to a patient, such as in a syringe and/or in the connecting tubing, severely limits the duration of continuous infusions or the time between intermittent injections. The need to initially resuspend the colloid or other type of agent, and to further suspend if the agent is not used shortly after resuspension, requires either time-consuming effort and vigilance by the user or the use of mechanical mixing devices. In any case, the need to resuspend an agent poses an additional step and a possible source of error in an imaging procedure.
- The invention is directed to a device that provides a suspended agent without additional mechanical mixing. The device divides a total volume of a sedimenting agent into a network of sub-volumes and has prots for an inflow and outflow of a propellant fluid to releases the sub-volumes of agent from the device. In one embodiment, the device is located within a container in which the agent is packaged, such as a vial or bottle, or in a container in which the agent is dosed, such as a syringe or bag, or in a container containing the propellant fluid. In another embodiment, the device is located external to a container for the propellant fluid. In this embodiment, the device may be operably attached to an exit port of the propellant fluid container. Alternatively, in this embodiment, the device may be positioned in-line at any point with lines that connect the propellant fluid container with a patient connector. The device is comprised of a network of sub-volumes that may take the form of one or more tubes, cells and/or sponges, and that may assume any configuration such as a parallel, stairstep, helical, random and/or coiled configuration. The network may be retained in a network holder.
- The invention is also directed to a suspension device for a volume of an agent in which a container for the propellant fluid has a network of grooves that are integral with the container and that retain a sub-volume of the agent within the grooves. The container has a plug that occupies an internal volume of the container and the grooves are either integral with an internal wall of the container, or are integral with an external wall of the plug. In either embodiment, the plug diverts the propellant fluid flow to a variable extent from the center of the container to the periphery of the container, thus diverting fluid flow through the grooves. The grooves may further contain substantially perpendicular channels at regular intervals to allow uniform filling of the grooves with the agent.
- The invention is also directed to a method of providing a volume of suspended agent to a patient. The method includes dividing the volume of agent into contained sub-volumes, storing the sub-volumes in a network for containing sub-volumes of the agent and providing a propellant fluid under pressure to eject the sub-volumes of agent through the network and into a patient. The propellant fluid may be housed in a container in which the network is also located. Alternatively, the network may be external to the propellant fluid container, with the network positioned either in-line between a source of propellant fluid and a patient, or adjacent an exit port of a propellant fluid container.
- The invention is also directed to a suspension device for a folume of an imaging contrast agent. A network contains a plurality of sub-volumes of the agent and has inflow and outflow ports for propellant fluid. The device may also have a container and network holder external to the container.
- The objectives and other advantages of this invention will be further understood with reference to the following drawings and detailed description.
- FIG. 1 is a cross-sectional view of a syringe container with an internal tubular network.
- FIG. 1A is a view similar to FIG. 1 of an alternate embodiment of the invention.
- FIG. 2 is a cross-sectional view of a syringe container with an external tubular network operably attached to a propellant fluid container exit port.
- FIG. 3 is an elevational view of an in-line device.
- FIGS. 4A, 4B and4C are various network embodiments and configurations.
- FIG. 5 is a cross-sectional view of a syringe container having an integral network.
- FIG. 6 is a cross-sectional view of an integral network with channels.
- The device of the invention sub-divides a desired volume of an agent to suspend the agent without mechanical mixing. Resuspension is caused by viscous fluid flow through the network of sub-volumes. As used herein, the device is comprised of a network of structures for containing sub-volumes of the agent, with the entire volume of agent contained in the network component sub-volumes. As will be described, the device may be located in the same container that contains propellant fluid to eject the agent from the network (container package embodiment). Alternatively, the device may be located adjacent an exit port of a propellant fluid container (add-on embodiment), or may be positioned in-line at any point in a fluid path between the propellant fluid container and the ultimate deposit site such as a patient (in-line embodiment). As used herein, a propellant fluid is one that is used to eject the agent from the network of tubes, cells, etc. As used herein, a network is defined as a collection of structures which contain the entire desired volume of agent in sub-volumes, and hence increase the surface area of the agent over which the propellant fluid must flow, in the device. In one embodiment, the network has a common exit port, and agent sub-volumes are ejected from the network at a substantially equal rate. The network may encompass tubes, cells, sponges, etc. and is not limited by volume or configuration.
- The device sub-divides a volume of an agent to prevent it from settling or sedimenting into one or a few dense aggregates without the need for mechanical mixing or suspending prior to use, and thus reduces or eliminates the problem of remixing or resuspending an agent that has come out of suspension prior to use. Use may be either preparing an injection dose by transferring the desired volume of agent from a package to a dosing container such as syringe, or injecting the dosing volume of agent into a patient. This problem may occur with contrast agents, either while in their package or portioned in a container such as a syringe for injecting into a patient about to undergo an imaging procedure. The invention solves the problem by subdividing the volume of the agent to prevent separation or aggregation of the agent from the suspending liquid.
- Dividing a uniformly suspended contrast agent or other agent into a network of sub-volumes rather than a single large volume inhibits the particles from either floating or precipitating into one or more larger masses or aggregates. The invention thus reduces or obviates the need for mixing before or during a process, such as an infusion process. This increases the quality, safety, and cost- and time- efficiencies of the process.
- With reference to FIG. 1, a network8 a containing divided sub-volumes of an
agent 12 is internal to a container 10 forpropellant fluid 16. The container 10 may be asyringe 14 or other types of containers which include but are not limited to vials, bags having flexible or semi-flexible walls, bottles of either glass or plastic, etc. Theagent 12 contained in the network 8 a is ejected from the container 10 aspropellant fluid 16 flows through the network 8 a and displaces theagent 12. Thepropellant fluid 16 is any viscous fluid (liquid or gas) that is biocompatible. The propellant fluid may be a diluent for theagent 12 such as normal saline, water, buffer, etc. Thepropellant fluid 16 may also be a contrast agent that is different from theagent 12 injected for the imminent imaging procedure. - The network8 a may be any structure that serves to contain a sub-volume of the desired total volume of an
agent 12 in a unit area. The network 8 a may be contained in anetwork holder 22. The network 8 a may betubes 18 which, as used herein, encompass tubules, microtubules, channels, or other types of hollow cylinders that convey a fluid or that function as a passageway, whereby a volume ofagent 12 is divided into sub-volumes of any size. There are numerous configurations of thetubes 18 that can be used to sub-divide the volume ofagent 12. These include, but are not limited to, a singlelong tube 18 as best shown in FIG. 1 or a collection oftubes 18 a as shown in FIG. 1A. Thetubes 18 may be in any configuration, such as one or more coils or helices, an angular or stairstep configuration, and/or even random configurations. A collection oftubes 18 may similarly be one or more coils or helices, an angular or stairstep configuration, and/or even random configurations, or may be arranged in a parallel configuration (FIG. 1A). The geometries and configurations of the network 8 may be combined in either regular or random configurations. While FIGS. 1 and1A show tubes 18 positioned in asyringe 14 without any accompanying support, other configurations are contemplated. For example, thetubes 18 may be positioned within a network holder 22 (FIGS. 2 and 3), or may be supported or held in asyringe 14 ornetwork holder 22 by a fixture such as 24 (shown in phantom lines in FIG. 1) which may extend for part of or all of the length of the network 8. - With reference to FIG. 2, a dose delivery container10 that is a
syringe 14 is shown with anetwork holder 22 containing the network 8 external to thesyringe 14. The network 8 c is packaged within anetwork holder 22, which may be any container in which the network is housed or retained and may be made of any biocompatable material. Thenetwork holder 22 containing the network 8 c may be separable from thesyringe 14 or other container 10 and attached to anexit port 24 of thesyringe 14 or container 10. Thenetwork holder 22 for the network 8 c may also be manufactured as part of the container 10, which may be useful as a pre-packaged embodiment of the invention. In a non-pre-packaged embodiment, thenetwork holder 22 may be attached to anexit port 24 using, for example,connectors 26 such as luer fittings. Theexit port 24 of thesyringe 14 may be fitted with luer fittings, such as Luer-Lok® caps (Becton-Dickinson), or may have luer fittings such as metal, brass or glass luer tips attached. As previously described, a support orfixture 30 for thetubes 28 may be used, and thesupport 30 andtubes 28 may be contained in anetwork holder 22. As one alternative, thesupport 30 andtubes 28 may be contained directly in the container 10. As another alternative, thetubes 28 in anetwork holder 22 may be unsupported as shown in FIG. 2. - While FIG. 2 illustrates a
network holder 22 which is attached to asyringe 14, other embodiments are contemplated. With reference to FIG. 3, the network (not shown) contained in anetwork holder 22 is shown in an in-line embodiment. Thenetwork holder 22 is fashioned withconnectors 26 at both aninflow port 32 and anoutflow port 34. Tubing is connected toconnectors 26 to carrypropellant fluid 16 from a syringe toholder 22 and fromholder 22 to a patient. Theconnectors 26 may be the same or different at theinflow 32 andoutflow 34 ports and may be any type such as luer fittings, as previously described.Network holder 22 and the network inside may be configured symmetrically, so that the orientation of thenetwork holder 22 in an in-flow embodiment need not be a concern; i.e., there is no back-to-front or front-to-back limitation.Agent 12 can be removed from the network within thenetwork holder 22 upon pressure from apropellant fluid 16. - A network8 that is internal to a container 10 such as a
syringe 14 need not be housed in anetwork holder 22. As seen in FIGS. 1 and 1A, the network 8 a, 8 b oftubes 18 or other structures may be positioned directly within thebarrel 36 of thesyringe 14. In an alternative embodiment, the network 8 that is internal to asyringe 14 or other container 10 may also be housed in anetwork holder 22. In either embodiment, thebarrel 36 of thesyringe 14 may contain apropellant fluid 16 that, upon initiation of flow, provides pressure to release or eject theagent 12 from the network 8. Thepropellant fluid 16 need not be pre-filled in thebarrel 36 of thesyringe 14, but instead may be added to thebarrel 36 of thesyringe 14. - The sub-dividing volume structure of
tubes 18 in the network 8 may assume a variety of geometries and configurations. As shown in FIGS. 1A, 2, 4A, 4B and 4C, thetubes 18 may be straight, coiled, helical, inrandom filaments 38, in an angular or stairstep (not shown) configuration, or may have other configurations. All of these alternatives are appropriate for use in any of the illustrated embodiments. The sub-dividing network 8 need not encompasstubes 18 at all; all shown in FIGS. 4A, 4B and 4C, thenetwork 8 d, 8 e and 8 f respectively, may be a series of discrete cells 42 (see FIG. 4B), or may have a sponge 44 type of structure (see FIG. 4A). In acell 42 structure, theagent 12 is retained in or ondiscreet cells 42. In a sponge 44 structure, theagent 12 is either absorbed in or adsorbed on the sponge 44, rather than contained withintubes 18 orcells 42. Acell 42 or sponge 44 structure may also be used effectively in anetwork holder 22 separate from asyringe 14. In any embodiment, the network 8 may be configured so that there is a non-uniform direction for all sub-volumes, that is, there is no single upward, downward or lateral direction for all sub-volumes. - With reference to FIG. 5, a network8 g that is integral with the container 10 is shown. In this embodiment, the network 8 g is fabricated as grooves or
channels 48 that are etched or otherwise manufactured within the container 10 itself. For example, asyringe 14 may have acylindrical plug 46 disposed in thebarrel 36, where theplug 46 has parallel orspiral grooves 48 in its outer surface. Thegrooves 48 contain theagent 12 between thesyringe 14inner wall 50 andbarrel 36. As shown in FIG. 6, thegrooves 48 may contain substantiallyperpendicular channels 60 at one or more regularly spaced intervals. Thechannels 60 permit rapid and uniform filling of the network 8 withagent 12 added into one side of a container 10 when the other side of the container 10 is sealed. In another embodiment, thesyringe 14 has acylindrical plug 46 disposed in thebarrel 36 as previously described, where theinner wall 50 of thesyringe 14 has parallel or spiral grooves in its structure. Thegrooved structures 48 may also be used in aseparate network holder 22. In these embodiments, thegrooved structure 48 comprises the network 8 which sub-divides the volume ofagent 12. It will thus be appreciated that the network 8 may assume a variety of forms and configurations whereby a volume ofagent 12 can be sub-divided into smaller volumes with increased surface area of theagent 12 over which thepropellant fluid 16 flows to reduce sedimentation. - The network8, whether in the form of
tubes 18,cells 42 or sponges 44, may be made of any biocompatable material that can withstand sterilization and is inert with respect to theagent 12, thepropellant fluid 16, and the container 10. Examples of such materials for a tubular 18 network include biocompatable tubing such as polyethylene, polypropylene, silicon, rubber, etc., for example, Tygon® tubing (halogenated vinyl plastic, Norton Plastics).Tubes 18 used in kidney dialysis devices, such ascellulose tubes 18 having a nominal diameter of 200 μm, may also be used in the invention. In a network 8 e having cells or voids, thecells 42 may be produced by incomplete fusion of pieces of fusable material such as thermoplastics or metals. Thecells 42 may be made of Delrin™, polycarbonate such as Lexan™, polyethylene, polypropylene, silicon, rubber, etc. In a network 8 d having a sponge 44 structure, the sponge 44 may be made of porous Delrin™, porpous polycarbonate such as Lexan™, porous polyethylene, porous polypropylene, porous silicon, porous rubber, etc. - The size and volume of the network8, container 10, and
network holder 22 may vary, depending upon a number of factors. These factors include the volume ofagent 12, the size of the container 10, the duration of the imaging or other procedure to be performed, etc. There is neither a maximum nor a minimum volume for the network 8, container 10, ornetwork holder 22, and an exponential range of volumes is contemplated by the invention. For embodiments in which the network 8 is internal or integral with the container 10, however, the volume ofagent 12 contained within the network 8 is at most one-half the volume ofpropellant fluid 16 in the container 10. This ensures that substantially all theagent 12 will be released from the network 8 by the flow ofpropellant fluid 16. For example, volumes ofcontrast agent 12 injected for enhanced ultrasound imaging may range from 1 ml to about 10 ml. As an example, a 3 ml volume of agent would require using about a 10ml syringe 14, with the tubular 18 or other structure of the network 8 containing 3ml agent 12 and the remaining volume of thesyringe 14 containing at least 3 ml, and more typically 4-5 ml, ofpropellant fluid 16. A 3 ml volume ofagent 12 may be sub-divided in asyringe 14 having ten threads orgrooves 48 per inch, with the threads orgrooves 48 one millimeter deep, each thread or groove 48 containing about 0.3ml agent 12. - The container10 and/or
network holder 22 may be manufactured having the network 8 preloaded with a uniformly mixed suspension ofagent 12 such as a pharmaceutical colloid. The container 10 and/ornetwork holder 22 may have both anentry port 54 and anexit port 56 withappropriate fittings 26 such as luer locks for connection to standard tubing or catheters, as is known to one skilled in the art (FIG. 3). To eject theagent 12 in the network 8 from theexit port 56 of the container 10 ornetwork holder 22 and into the patient through a patient connector line,propellant fluid 16 may be injected into theentry port 54 or, alternatively, pressure may be applied to thepropellant fluid 16 already in the container 10. The container 10 may also have asingle exit port 56 and aplunger 58, withliquid 60 in the opposite end, to permit use as a prefilled syringe (FIG. 1). - The specific location, position and configuration of the network8 may depend upon an intended use. For example, an agent containing a gas other than air should be housed in a container 10 that has been purged of air. A container 10 made of glass may be rendered air-tight more easily than a plastic syringe, and thus is preferable for this agent. Likewise, a network 8 that is internal rather than external is preferred for use with an agent that contains a gas other than air. This allows the
propellant fluid 16 to be purged of air and become saturated with the agent-containing gas, maintaining a substantially anaerobic environment prior to injection. - One advantage of the invention is that it eliminates the need for resuspension of
agents 12 that may come out of suspension, either in their original container 10 or in a dose delivery container such as asyringe 14. Conventional containers 10 require mechanical devices or manipulations to maintain colloids such as acontrast agent 12 in suspension. By eliminating the need for prior resuspension of theagent 12 for single-bolus injection, the device and method of the present invention provides a competitive advantage forinjectable agents 12. In accordance with the principles of the present invention, asyringe 14 having a network 8 containingagent 12 can remain resuspendable for more than five months. - Maintaining the
agent 12 in a substantially fully resuspendable state assures consistent quality and reduced sensitivity to user technique. Theagent 12 may be shipped already prepackaged in the network 8. This arrangement has the potential to reduce susceptibility of agents, such as microbubble preparations, to mechanical vibration and shock which may decrease the integrity of theagent 12. Dividing the volume ofagent 12 into sub-volumes also allows it to be more quickly preheated to a desired temperature, facilitating the efficiency of the entire imaging procedure. - Another advantage of the invention is that the colloid or
other agent 12 may be released, ejected or expelled from theexit port 56 of the container 10 by injecting apropellant fluid 16. This precludes the need to draw the pharmaceutical orcontrast agent 12 into asyringe 14 for injection, and provides similar advantages as enjoyed by pre-filled syringes. - Still another advantage of the invention is that, in those embodiments such as FIGS. 2 and 3 where network8 is external to the
syringe 14, theexit port 56 of the dose delivery container 10 ornetwork holder 22 may be connected to a short angiocatheter (not shown) that is very close to a venous or arterial puncture site in a patient. This arrangement prevents loss of suspension ofagent 12 that would occur inside a longer catheter, and permits use of a manual or power syringe located a substantial distance away from the patient, while preventing the need for theagent 12 to maintain resuspendable in the manual orpower syringe 14 and connecting tubing. Instead, the manual or power syringe and tubing need only contain a non-colloidal fluid that does not require mixing or resuspending during long injection times. - A further advantage of the invention is realized with an optional built-in
plunger 58 in thesyringe 14. A built-inplunger 58 permits use of the device as amanual syringe 14 or with a small, battery-operated power injector at the end of a very short angiocatheter. In either case, the filledsyringe 14 could be located very close to a venous or arterial puncture site, precluding the need to maintain theagent 12 resuspended in a long catheter for infusion into a patient. This embodiment also precludes the need for a fluid-filledsyringe 14 connected to theentry port 54 of the dose delivery container 10 in order to eject theagent 12 from theexit port 56 of the dose delivery container 10. - It should be understood that the embodiments of the present invention shown and described in the specification are exemplary embodiments contemplated by the inventor and are not limiting in any way. For example, the invention is not limited to use in the clinical area and may be used in research applications, as well as in other industries where uniformly suspended agents are needed, such as the food and beverage industries. In such cases, for example, the
propellant fluids 16 may also include oils, epoxy resins, sugars, etc., depending upon the application. Therefore, various changes, modifications or alterations to these embodiments may be made or resorted to without departing from the spirit of the invention and the scope of the following claims.
Claims (24)
1. A method for administering an agent to a patient comprising
providing a tubular network containing subvolumes of an agent out of suspension, the network containing ports for inflow and outflow of a propellant fluid to release the agent from the network,
connecting the network to a vessel of a patient,
providing the propellant fluid to the inflow port to suspend the agent and administering the suspended agent to the patient.
2. The method of claim 1 wherein the network is within a syringe.
3. The method of claim 2 wherein the syringe contains the propellant fluid.
4. The method of claim 1 wherein the agent administered is a contrast agent.
5. The method of claim 1 wherein the tubular network is configured randomly, in parallel, coiled, or helically.
6. A method for administering a volume of an agent to a patient comprising
dividing said volume into a plurality of subvolumes of an agent out of suspension in a network,
providing a propellant fluid under pressure to said network at an inflow port to contact and suspend the subvolumes of agent, and
administering the suspended agent to a patient from an outflow port of the network to a patient connector.
7. The method of claim 6 further comprising containing said propellant fluid in a container with the network internal to the container.
8. The method of claim 6 wherein said container is a dose delivery container.
9. The method of claim 6 wherein said container is a packaging container.
10. The method of claim 8 wherein said dose delivery container is selected from the group consisting of a manual syringe, a power syringe and a bag.
11. The method of claim 6 further comprising containing said propellant fluid in a container with the network external to the container.
12. The method of claim 11 wherein said container has an exit port and said network is operably connected adjacent said exit port.
13. The method of claim 11 wherein said network is operably connected in-line between said container and said patient connector.
14. The method of claim 11 wherein said agent is released by injecting said propellant fluid into an entry port of said container.
15. A method of administering a volume of an agent to a patient comprising
containing subvolumes of an agent out of suspension in a tubular network capable of insertion within a syringe and connection to a vessel of a patient,
providing a propellant fluid to said network,
pressurizing said propellant fluid to initiate flow of said fluid to resuspend said agent, and
administering said suspended agent to said patient vessel through a patient connector.
16. The method of claim 12 wherein the agent is a contrast agent.
17. The method of claim 12 wherein pressure is provided by a mechanical source.
18. The method of claim 12 wherein pressure is provided by a manual source.
19. The method of claim 12 wherein the network is within a syringe.
20. A method for administering an agent to a patient comprising
providing the agent in a tubular network in an interior of a container having an exit port capable of coupling to a patient connector and defining an interior space containing a propellant fluid, the network having a single passageway containing subvolumes of the agent, an outflow port in fluid communication with the exit port, and an inflow port opening into the interior space, and
flowing the propellant fluid into the inflow port and through the passageway to release subvolumes of the agent from the outflow port through the exit port to the patient connector to administer the agent to the patient.
21. The method of claim 20 wherein the container is a syringe.
22. The method of claim 20 wherein the patient is administered a contrast agent.
23. The method of claim 20 wherein the patient is imaged by a method selected from the group consisting of computed tomography, magnetic resonance imaging, ultrasound, and X-ray.
24. A method for administering an agent to a patient comprising
providing subvolumes of an agent in a helical tube within a syringe having a side wall defining an interior space, an exit port connected to a patient connector, and a plunger positioned in the interior space and having a sealing engagement with the side wall, the interior space between the plunger and the exit port containing a propellant fluid for the agent and the plunger being movable in the interior space toward the exit port, the tube defining a continuously open and uninterrupted fluid passageway within the interior space of the syringe and located between the plunger and the exit port, the fluid passageway having an outflow port in fluid communication with the exit port of the syringe and an inflow port opening into the interior space,
providing pressure to the plunger to flow propellent fluid through the fluid passageway to contact the agent for flow from the outflow port and exit port and into a patient connector.
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- 2000-05-19 EP EP05077013A patent/EP1625864A3/en not_active Withdrawn
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US20070088330A1 (en) * | 2005-08-17 | 2007-04-19 | House Jamie G | Catheterization assembly |
US8177774B2 (en) * | 2005-08-17 | 2012-05-15 | Adapta Medical, Inc. | Catheterization assembly |
US20080015527A1 (en) * | 2006-07-17 | 2008-01-17 | Jamie Glen House | Catheter assemblies having protective sheaths |
US20080281271A1 (en) * | 2007-05-09 | 2008-11-13 | Griffiths Steven M | Drug delivery system with a small amount of a therapeutic agent |
US8057427B2 (en) | 2007-05-09 | 2011-11-15 | Meridian Medical Technologies, Inc. | Drug delivery system with a small amount of a therapeutic agent |
Also Published As
Publication number | Publication date |
---|---|
EP1625864A3 (en) | 2006-08-09 |
US20010018571A1 (en) | 2001-08-30 |
US6871087B1 (en) | 2005-03-22 |
US6554792B2 (en) | 2003-04-29 |
EP1625864A2 (en) | 2006-02-15 |
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Legal Events
Date | Code | Title | Description |
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STCB | Information on status: application discontinuation |
Free format text: ABANDONED -- FAILURE TO PAY ISSUE FEE |