Patent Grant
7213702
The present invention relates to a small bag-shaped drug container and, more particularly, to a small bag-shaped drug container suitable for almost insoluble or insoluble drugs. Further, the present invention relates to a small bag-shaped drug container, which enables a drug to be easily and completely dissolved or suspended in spite of a small amount of a solution.
Drugs which are easily degenerated by moisture or oxygen have conventionally been administered in the form of a liquid drug prepared just before use by mixing it with a solution. In order to prepare the liquid drug, there have widely been used a so-called syringe method comprising the steps of injecting a solution into a vial containing a dried drug with a syringe, and then drawing the resultant liquid drug into the syringe, or a method employing a double ended needle to communicate a solution container with a drug container. Recently, in order to remove troublesome dispensation, double chamber type prefilled syringes have been put into practical use. Such a prefilled syringe contains a drug in a drug chamber and a solution in a solution chamber, which are adapted to be communicated with one another by communicating means such as a bypass or a built-in connecting needle to dissolve the drug in the solution.
The syringe method is used for preparation of a liquid drug less than about 10 ml, but it is troublesome in dissolving operation. Further, in case that a drug such as a subcutaneous injection is required to be dissolved or suspended in a small amount of the solution, it is extremely difficult to perform the dissolving operation in the vial. In addition, in case of insoluble or substantially insoluble drugs, it is required to repeatedly transfer a mixture of the solid medicine and the solution from the syringe to the vial, or vice versa, in order to achieve complete dissolution or suspension. However, it is very difficult to perform such dissolving operations without producing foaming.
The above troublesome dispensation can be avoided by use of the method of employing a double ended needle or the double-chamber type prefilled syringes. However, it is very difficult with the method of employing a double-ended needle to dissolve insoluble or substantially insoluble drugs in the solution without foaming, since the mixture of the solid medicine and the solution must be repeatedly transferred from the syringe to the vial, or vice versa, in order to achieve dissolution or suspending. Similarly, it is very difficult with the double-chamber type prefilled syringe to perform dissolving operation without foaming since the mixing can be performed only by shaking of the syringe.
It is therefore an object of the present invention to provide a bag-shaped drug container, which makes it possible to easily and completely dissolve or suspend a drug in a solution even if the drug is almost insoluble or insoluble or even if the dissolution or suspension is carried out with a small amount of the solution, as well as to minimize foaming of the drug solution during dissolving or suspending operation, and to prevent the working site from being soiled with the drug solution at the time of recovery of the dissolved or suspended solution into the syringe.
The above objects of the present invention are solved by constituting a drug container with a flexible bag-shaped container to make it possible to press and rub the drug container with hands, and further providing a mouth of the container with means for fixing a tip of a syringe to the mouth of the container to prevent the syringe from falling off from the mouth of the container during pressing and rubbing.
According to the present invention, there is provided a small bag-shaped drug container comprising a container body formed into a bag with a flexible film and a mouth provided at one end of said body, and a Luer locking means provided at an open end of said mouth and being liquid-tightly connectable to a tip of a syringe.
The above film may be composed of a single layer of polyolefine, or multi-layers including an innermost layer of polyolefine. Further, the film may be a film of water permeability and oxygen permeability, or a film of water impermeability and oxygen impermeability. However, if the film is composed of a single layer film of polyolefine or a film of water permeability and oxygen permeability, it is necessary to package the container in a packaging medium with water impermeability and oxygen impermeability.
The container body may be composed of a front film having water permeability and oxygen-permeability and a rear film having water impermeability and oxygen-impermeability and partitioned into two chambers by an easily peelable tender sealing portion provided at a position close to the mouth, one of two chambers being communicated with the mouth, while other chamber being uncommunicated with the mouth. In this case, the front film of the chamber uncommunicated with said mouth may be provided with an easily peelable, water-impermeable and oxygen-impermeable cover film, and the chamber communicated with the mouth may be charged with a drug.
The terms “water-impermeability and oxygen-impermeability” used herein mean properties that can not be permeated by water and oxygen. The terms “water-permeable and oxygen-permeable” used herein mean properties that can be permeated by water and oxygen and includes the properties that are almost impermeable to water and oxygen.
The present invention will be explained below in detail, making reference to the accompanying drawings, which show, by way of example only embodiments thereof.
a)–(c) are diagrams illustrating a way to use the bag-shaped drug container of the present invention.
As illustrated in
The bag-shaped drug container of the present invention is a drug container suitable for use in syringe method widely used for preparation of a drug solution with a small amount of less than about 10 ml. Thus, the container body 1 is so designed to have a capacity of not more than 10 ml and, preferably, not more than 5 ml.
The film that forms the container body 1 may be a single layer film of polyolefine such as polypropylene, polyethylene, polyethylene terephthalate (PET), or a multi-layer film including an innermost layer of polyolefine. The film may be permeable to water and oxygen or impermeable to water and oxygen. Preferred multi-layer films include laminated films comprising a deposited silica layer which is almost impermeable to moisture or oxygen, or aluminum foil-laminated films laminated with a water-impermeable and oxygen-impermeable aluminum foil. The laminated films including a deposited silica layer comprises, for example, multilayer films including an outermost layer of a copolymer of polyethylene (PE) and polypropylene (PP) and an innermost layer of polyethylene, and having a structure of (PE+PP)/SiO2/PET/SiO2/PE. In that case, the outermost layer may be of polyethylene. Preferred aluminum foil-laminated films comprises, for example, multilayer films including an outermost layer of polyethylene terephthalate and an innermost layer of polyethylene and having a structure of PET/aluminum foil/PE. In that case, one or more other plastic layers may lie between aluminum foil and PE.
If the film is a single layer film of polyolefine or a film with water-permeability and oxygen-permeability, the whole container is required to be packaged in a water-impermeable and oxygen-impermeable packaging medium 4, as illustrated in
The container body 1 may be made of a front film 11 having water-permeability and oxygen-permeability and a rear film 12 having water-permeability and oxygen-permeability, as illustrated in
The mouth 2 is a cylindrical member generally made of the same resin at that of the innermost layer of the container body 1, and provided at an open end thereof with a Luer locking means 21. The Luer locking means 21 is connecting means, which performs Luer connection concurrently with locking connection (e.g., screw engagement). The Luer locking means used for this purpose generally comprises, for example, a female Luer portion 211 formed by decreasing taperingly a diameter of a lumen L of the mouth 2 according to a shape of a male Luer portion (designated by C1 in
The bag-shaped drug container of the present invention is used in the manner explained below with reference to
Firstly, there are prepared a bag-shaped drug container FB and a Luer locking type syringe provided at a distal end thereof with a Luer locking type needle-connecting portion C (hereinafter referred to as a “tip”). The tip C of the syringe S is fit in the mouth 2 of the drug container FB. Then, the syringe S is turned in the direction indicated by an arrow A for engagement of the tip C with the Luer locking means 21, whereby reliably connecting the syringe S to the mouth 2 of the bag-shaped drug container FB (
As will be understood from the above, the bag-shaped drug container according to the present invention makes it possible to dissolve or suspend the drug in the solution by pressing and rubbing the container body with hands. Further, the syringe is prevented from separation from the drug container during pressing and rubbing operation, thus making it possible to easily and completely dissolve or suspend the drug in the solution even if the drug is almost insoluble or insoluble or even if the dissolution or suspension is carried out with a small amount of solution. In addition, it is possible to minimize foaming of the drug solution during dissolving or suspending operation. Also, it is possible to prevent the working site from being soiled with the drug solution at the time of recovery of the dissolved or suspended solution into the syringe.
| Number | Date | Country | Kind |
|---|---|---|---|
| 2001-337531 | Nov 2001 | JP | national |
| Number | Name | Date | Kind |
|---|---|---|---|
| 4608043 | Larkin | Aug 1986 | A |
| 4842587 | Poncy | Jun 1989 | A |
| 4961495 | Yoshida et al. | Oct 1990 | A |
| 4994056 | Ikeda | Feb 1991 | A |
| 5002530 | Recker et al. | Mar 1991 | A |
| 5135489 | Jepson et al. | Aug 1992 | A |
| 5176634 | Smith et al. | Jan 1993 | A |
| 5184742 | DeCaprio et al. | Feb 1993 | A |
| 5409125 | Kimber et al. | Apr 1995 | A |
| 5423421 | Inoue et al. | Jun 1995 | A |
| 5944709 | Barney et al. | Aug 1999 | A |
| 5957898 | Jepson et al. | Sep 1999 | A |
| 5984373 | Fitoussi et al. | Nov 1999 | A |
| 6068617 | Richmond | May 2000 | A |
| 6149655 | Constantz et al. | Nov 2000 | A |
| 6261282 | Jepson et al. | Jul 2001 | B1 |
| 6267154 | Felicelli et al. | Jul 2001 | B1 |
| 6695829 | Hellstrom et al. | Feb 2004 | B2 |
| 20010047162 | Yugari | Nov 2001 | A1 |
| Number | Date | Country |
|---|---|---|
| 0 941 731 | Sep 1999 | EP |
| 1 166 742 | Jan 2002 | EP |
| H08-280775 | Oct 1996 | JP |
| H10-201820 | Aug 1998 | JP |
| 2000-197687 | Jul 2000 | JP |
| 9924086 | May 1999 | WO |
| Number | Date | Country | |
|---|---|---|---|
| 20030080129 A1 | May 2003 | US |
