The present invention relates to a patch containing diclofenac sodium as an active ingredient, the patch exhibiting excellent releasability and percutaneous absorbability of diclofenac sodium and exerting a stable analgesic anti-inflammatory effect for a long period of time upon topical application.
Diclofenac sodium exerts excellent antipyretic, analgesic, and anti-inflammatory effects. Drug preparations containing diclofenac sodium are generally divided into peroral drugs exhibiting a systemic action and drugs for external use exhibiting a topical action. When a peroral drug is administered, grave, systemic adverse effects such as gastrointestinal disorders occur, thereby calling for further development of percutaneous-absorption-type patches for topical application for mitigating such adverse effects. In connection with a patch containing a non-steroidal analgesic anti-inflammatory drug such as diclofenac sodium, the most important issues are effective, sustained percutaneous absorption of the active ingredient into the disturbed portion directly under the patch and delivery of the active ingredient to the disturbed portion directly under the patch.
Since diclofenac sodium has considerably low solubility in water and an oily component, a wide range of studies have been carried out in order to stabilize it in a dissolved state in a drug for external use for promoting percutaneous absorption from a patch. For example, Japanese Patent Application Laid-Open (kokai) No. 61-280426 discloses incorporation of an organic acid (citric acid) as an additive for enhancing the solubility and percutaneous absorbability of diclofenac sodium. Japanese Patent Application Laid-Open (kokai) No. 4-193826 discloses incorporation of an essential oil component such as menthol or mentha oil as a percutaneous absorption promoter for diclofenac sodium. Japanese Patent Application Laid-Open (kokai) No. 5-178763 discloses incorporation of a polyhydric alcohol medium-chain fatty acid ester as a solubilizer for slightly soluble drugs. Japanese Patent Application Laid-Open (kokai) No. 11-222443 discloses incorporation of 1-menthol and a pyrrolidone (pyrrolidone or at least one derivative thereof) as a percutaneous absorption promoter for diclofenac sodium.
However, percutaneous absorbability of a drug containing diclofenac sodium for external use is still unsatisfactory, and thus, there still remains a need for a drug for external use which promises more effective percutaneous absorption.
Thus, an object of the present invention is to provide a patch which exhibits excellent releasability and percutaneous absorbability of diclofenac sodium.
The present inventors have carried out extensive studies in order to solve the aforementioned problems, and have found that, by incorporating pyrrolidone or a derivative thereof, a polyhydric alcohol fatty acid ester, and an organic acid in combination into a Pressure Sensitive Adhesive (PSA) containing diclofenac sodium, there can be produced a patch of a hydrophobic type which attains a consistently dissolved state of diclofenac sodium in the PSA; exhibits excellent releasability of diclofenac sodium from the PSA and excellent percutaneous absorbability of diclofenac sodium; and exerts a stable analgesic anti-inflammatory effect for a long period of time.
Accordingly, the present invention provides an analgesic anti-inflammatory patch of a hydrophobic type for topical application containing, in a PSA, diclofenac sodium, pyrrolidone or a derivative thereof, a polyhydric alcohol fatty acid ester, and an organic acid.
The patch of the present invention contains, in a PSA, diclofenac sodium, pyrrolidone or a derivative thereof, a polyhydric alcohol fatty acid ester, and an organic acid. As mentioned above, diclofenac sodium is an active ingredient of the patch of the present invention. Preferably, diclofenac sodium is incorporated, as an active ingredient, into a PSA layer in an amount of 0.1-5.0 wt. %, more preferably 0.5-4.0 wt. %. From another viewpoint, diclofenac sodium is preferably incorporated into a PSA layer in an amount, per skin-contact area, of 5-2,000 μg/cm2, more preferably 50-400 μg/cm2. In the context of the present invention, the “PSA layer” does not include the support; i.e., the “PSA layer” refers to a layer containing the aforementioned ingredients and other ingredients in the PSA.
Examples of the above pyrrolidone or derivative thereof include 2-pyrrolidone and N-alkyl-2-pyrrolidones, with 2-pyrrolidone and N-methyl-2-pyrrolidone being particularly preferred. These pyrrolidone and derivetives thereof function as a solubilizer for diclofenac sodium, and each pyrrolidone species is preferably incorporated into a PSA layer in an amount of 0.5-8.0 wt. %, more preferably 1.0-5.0 wt. %.
Examples of the polyhydric alcohol fatty acid ester include alcohol (dihydric to tetrahydric) fatty acid esters; e.g., glycerin fatty acid esters, ethylene glycol fatty acid esters, propylene glycol fatty acid esters, sorbitan fatty acid esters, and pentaerythritol fatty acid esters. Specific examples include glycerin mono-(C6-C18) fatty acid esters, ethylene glycol mono-(C6-C18) fatty acid esters, propylene glycol mono-(C6-C18) fatty acid esters, sorbitan mono-(C6-C18) fatty acid esters, propylene glycol di-(C6-C18) fatty acid esters, and pentaerythritol tetra-(C6-C18) fatty acid esters. Of these, glycerin fatty acid esters (e.g., glyceryl tri(caprylate.caprate)), ethylene glycol fatty acid esters, pentaerythritol fatty acid ester (e.g., pentaerythrityl tetra-2-ethylhexanoate), and propylene glycol fatty acid esters (e.g., propylene glycol monocaprylate and propylene glycol dicaprylate) are more preferred. Of these, propylene glycol fatty acid esters are still more preferred. Examples of commercial products of these esters include Sefsol (product of Nikko Chemicals Co., Ltd.). These polyhydric alcohol fatty acid esters function as a percutaneous absorption promoter for diclofenac sodium and may be used in combination of two or more species. The ester is preferably incorporated into a PSA layer in an amount of 0.2-10.0 wt. %, more preferably 0.5-5.0 wt. %.
Examples of the organic acid include C3-C6 dicarboxylic acids and C3-C6 tricarboxylic acids. Of these, citric acid, tartaric acid, and succinic acid are preferred. These organic acids function as percutaneous absorption promoters for diclofenac sodium and may be used in combination of two or more species. The organic acid is preferably incorporated into a PSA layer in an amount of 0.05-4.0 wt. %, more preferably 0.1-2.0 wt. %.
As mentioned above, both the polyhydric alcohol fatty acid ester and the organic acid function as percutaneous absorption promoters for diclofenac sodium. The ratio by weight of the polyhydric alcohol fatty acid ester to the organic acid preferably falls within a range of 1:20 to 200:1, more preferably 1:4 to 50:1. The total amount of the polyhydric alcohol fatty acid ester and the organic acid incorporated into a PSA layer preferably falls within a range of 0.25-14 wt. %, more preferably 0.6-7 wt. %.
The PSA into which the above components are to be incorporated is formed from a PSA base and a tackifier in combination. A preferable PSA base is a styrene-isoprene-styrene block copolymer (SIS). The SIS is commercially available, and examples of commercial products include Cariflex TR-1107 and Cariflex TR-1117 (trade names; product of Shell Kagaku K.K.). The amount of the PSA base incorporated into a PSA layer preferably falls within a range of 10-50 wt. %, more preferably 10-40 wt. %.
Examples of the tackifier include rosin ester resin, polyterpene resin, terpene phenol resin, and petroleum resin. Of these, rosin ester resin is preferred, with a rosin ester resin which has been subjected to removal of low-boiling fractions and subsequent hydrogenation (e.g., Ester Gum HG, product of Arakawa Chemical Industries, Ltd.) being particularly preferred. YS Resin (polyterpene resin, product of Yasuhara Yushi Kogyo Co., Ltd.), YS Polyster (terpene phenol resin, product of Yasuhara Yushi Kogyo Co., Ltd.), Quintone (petroleum resin, product of Nippon Zeon Co., Ltd.),
Arkon (petroleum resin, product of Arakawa Chemical Industries, Ltd.), Escorez (petroleum resin, product of Exxon Corp.), and other similar products may be used. The amount of the tackifier incorporated into a PSA layer preferably falls within a range of 5-50 wt. %, more preferably 5-30 wt. %.
The patch of the present invention may further contain arbitrary components such as an essential oil component (e.g., l-menthol or mentha oil); a softening agent (e.g., liquid paraffin); an antiageing agent; or a filler (inorganic compound). In addition to diclofenac sodium, the patch of the present invention may further contain another drug component such as ketoprofen, indomethacin, flurbiprofen, glycolyl salicylate, methyl salicylate, capsaicine, nonyl vanillylamide, tocopheryl acetate, a phellodendron bark extract, or an Aesculus Hippocastanum Seed extract. The softening agent is preferably incorporated into a PSA layer in an amount of 30-70 wt. %, more preferably 40-60 wt. %. The essential oil component is preferably incorporated into a PSA layer in an amount of 0.2-5.0 wt. %, more preferably 0.5-3.0 wt. %.
As mentioned above, the PSA layer included in the patch of the present invention is of hydrophobic type and contains substantially no water. This feature renders the present invention fundamentally different from that of conventional cataplasms.
The patch of the present invention can be produced by spreading the aforementioned PSA base on a soft support. Any type of support can be employed so long as the support is formed of a soft sheet which does not permit permeation of the PSA base through the back of the support. Examples of the sheet employable as the support of the present invention include woven and non-woven fabrics; plastic films such as polyolefin film, polyvinyl alcohol film, vinyl chloride film, urethane alloy film, urethane-vinyl chloride copolymer film, and ethylene-vinyl acetate film; film of a foamed blend of acrylic polymer or polystyrene-polybutadiene and polyisoprene; these films on which metal is coated through vapor deposition; and laminated sheets obtained from two or more species of these films. Appropriately, the support typically has a thickness of about 1,000 μm or less, preferably 30-700 μm.
The thus-produced patch of the present invention is applied to skin sites where an analgesic anti-inflammatory effect is needed; e.g., inflammation sites of the joints, muscles, neck, etc.
The present invention will next be described in more detail by way of examples, which should not be construed as limiting the invention thereto.
In each example, a PSA base and a softening agent shown in Table 1 were kneaded by use of a heating-kneader. A tackifier was added to the kneaded product, and the resultant mixture was further kneaded. Subsequently, diclofenac sodium was dissolved in a liquid mixture containing pyrrolidone, a polyhydric alcohol fatty acid ester, and citric acid, and the resultant solution was added to the above kneaded product. The resultant mixture was further kneaded, to thereby yield a uniform mixture. The mixture was applied to and spread on a support, to thereby form a PSA layer. After an appropriate period of time, the PSA layer was covered with a liner, and the resultant laminated product was cut into pieces of desired dimensions, to thereby obtain patches.
The time-elapsed dissolution amount of diclofenac sodium released from each patch was determined through a paddle over disk method by use of a dissolution tester according to Japanese Pharmacopoeia. Specifically, each test patch was cut into pieces (5 cm×5 cm), and each piece was bonded to Teflon mesh. The piece was clamped by two pieces of watch glass and placed in a phosphate buffer (900 mL, pH: 7.2) at 32° C. A paddle was rotated 25 mm above the patch, and a liquid (1 mL) was sampled at an intermediate level between the bottom of the paddle and the liquid surface. The sampling was performed 0.5, 1, 2, 3, 4, 6, and 8 hours after paddle rotation. Diclofenac sodium contained in each sampled liquid was quantitated through high performance liquid chromatography.
The patches prepared in the above Examples 1 to 4 and those prepared in Comparative Examples were employed as test patches. Test patches of Comparative Examples were prepared in accordance with the formulations shown in Table 2 in a manner similar to those employed in Examples 1 to 4.
Each of the thus-determined diclofenac sodium levels was converted to the corresponding percent dissolution from the patch (%). The results are shown in
The results indicate that the patches according to the present invention exhibit percent dissolution as high as four times or more that of all patches of Comparative Examples 1 to 6.
Hairless rats (body weight: 170 g) were anesthetized by pentobarbital. After removal of hair from the abdomen, abdominal skin samples were extirpated. Each of the thus-extirpated skin samples was set in a vertical cell (effective permeation area: 2.83 cm2, cell capacity: 16 mL), and a test patch (diameter: 1.9 cm) was attached to the skin sample. Subsequently, the receiver liquid in the cell was stirred by means of an electromagnetic stirrer while the cell was heated at 37° C. A portion (0.5 mL) of the receiver liquid was sampled a plurality of times at constant time intervals, and the diclofenac sodium content of the liquid portion was determined.
The results of Test Examples 1 and 2 indicate that the patch of the present invention can exhibit remarkably promoted releasability and percutaneous absorbability of diclofenac sodium which conventional techniques have not satisfactorily attained. Thus, the patch of the present invention has proven to be a clinically useful patch which mitigates systemic adverse effect and provides other advantages.
The patch of the present invention exerts the following effects:
(1) diclofenac sodium is effectively and continuously released from a PSA and percutaneously absorbed, thereby attaining sustained, excellent pharmaceutical and pharmacological effects;
(2) the patch per se has high tackiness and safety; and
(3) diclofenac sodium remains stable in the PSA.
Number | Date | Country | Kind |
---|---|---|---|
2001-154008 | May 2001 | JP | national |
This application is a Continuation of U.S. application Ser. No. 10/332,978, filed on Jan. 23, 2003, pending, which is a 371 of international application No. PCT/JP02/04942.
Number | Name | Date | Kind |
---|---|---|---|
4455146 | Noda et al. | Jun 1984 | A |
4738848 | Yoshida et al. | Apr 1988 | A |
4880742 | Hayaishi et al. | Nov 1989 | A |
5132115 | Wolter et al. | Jul 1992 | A |
5192753 | McGeer et al. | Mar 1993 | A |
5332577 | Gertner et al. | Jul 1994 | A |
5474985 | Polansky et al. | Dec 1995 | A |
5554650 | Holl et al. | Sep 1996 | A |
5599535 | Polansky et al. | Feb 1997 | A |
5656286 | Miranda et al. | Aug 1997 | A |
5674888 | Polansky et al. | Oct 1997 | A |
5725874 | Oda et al. | Mar 1998 | A |
5994401 | Cohen et al. | Nov 1999 | A |
6001875 | Cohen et al. | Dec 1999 | A |
6262121 | Kawaji et al. | Jul 2001 | B1 |
6365180 | Meyer et al. | Apr 2002 | B1 |
6399093 | Petrus | Jun 2002 | B1 |
6569463 | Patel et al. | May 2003 | B2 |
6923988 | Patel et al. | Aug 2005 | B2 |
6991095 | Yamasoto et al. | Jan 2006 | B1 |
7615237 | Takada et al. | Nov 2009 | B1 |
20020004065 | Kanios | Jan 2002 | A1 |
20020034539 | Esposito et al. | Mar 2002 | A1 |
20030129219 | Hong et al. | Jul 2003 | A1 |
20050250833 | Attali et al. | Nov 2005 | A1 |
20050272704 | Kelly | Dec 2005 | A1 |
Number | Date | Country |
---|---|---|
0 950 408 | Oct 1999 | EP |
1 201 232 | May 2002 | EP |
2 362 825 | Dec 2001 | GB |
61-280426 | Dec 1986 | JP |
04-193826 | Jul 1992 | JP |
4-321624 | Nov 1992 | JP |
O5-178763 | Jul 1993 | JP |
06-056660 | Mar 1994 | JP |
6-205839 | Jul 1994 | JP |
7-89853 | Apr 1995 | JP |
9-143062 | Jun 1997 | JP |
10-182440 | Jul 1998 | JP |
10-182450 | Jul 1998 | JP |
11-35458 | Feb 1999 | JP |
2852816 | Feb 1999 | JP |
11-222443 | Aug 1999 | JP |
11-255644 | Sep 1999 | JP |
2001-64205 | Mar 2001 | JP |
2002-0009845 | Feb 2002 | KR |
WO 0105381 | Jan 2001 | WO |
WO 0107018 | Feb 2001 | WO |
WO 0222109 | Mar 2002 | WO |
WO 0222109 | Mar 2002 | WO |
Number | Date | Country | |
---|---|---|---|
20100055160 A1 | Mar 2010 | US |
Number | Date | Country | |
---|---|---|---|
Parent | 10332978 | US | |
Child | 12614816 | US |