TREA

Rectal flunisolide compositions for treating inflammatory intestinal disorders

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Information

  • Patent Grant
  • 5721228
  • Patent Number
    5,721,228
  • Date Filed
    Wednesday, May 17, 1995
    29 years ago
  • Date Issued
    Tuesday, February 24, 1998
    27 years ago
Information
Abstract
Topical rectal therapeutic composition containing, as the active ingredient, flunisolide and/or one or more ester derivatives of same, in combination with suitable excipients and/or diluents, for the treatment of inflammatory intestinal disorders.
Description

This is a 371 of PCT/EP93/03228 filed Nov. 18, 1993.
FIELD OF THE INVENTION
The present invention relates to topical rectal therapeutic compositions containing, the as active ingredient, flunisolide and/or ester derivatives of same in combination with suitable excipients and/or diluents, for the treatment of inflammatory intestinal disorders.
STATE OF THE ART
Among all inflammatory intestinal diseases, ulcerative colitis is certainly the best known. It essentially affects the large intestine, in particular and most severely the rectum, but sometimes, either marginally or entirely, the colon too.
Other types of inflammatory intestinal diseases may affect the rectum and result in a mild ulcerative colitis or in a slightly different, but pathologically similar syndrome, such as proctitis and sigmoiditis.
Another inflammatory intestinal disease is the so-called Crohn's disease, which affects the large intestine only marginally.
A known treatment of the above pathologies consists in the systemic and topical administration of corticosteroids, such as hydrocortisone, betamethasone, and prednisolone.
However, the systemic administration of the aforesaid drugs produces serious side effects, mainly related to the interference with the hypothalamus-hypophysis-adrenal gland axis.
Also the topical administration of said corticosteroids causes interference with the hypothalamus-hypophysis-adrenal gland axis, since said drugs are inevitably absorbed by the systemic route. The side effects more frequently arising from the topical treatment of ulcerative colitis with the aforesaid traditional corticosteroids are: transient or prolonged depression of adrenal gland functionality, weight increase, acne, and facies lunaris. It is to be noted that a characteristic of ulcerative colitis is an inflammed intestinal mucosa, which facilitates the systemic absorption of the drugs which are usually administered over an extended period of time. Therefore, the need of developing a corticosteroid exerting a high therapeutic activity in the treatment of inflammatory intestinal diseases and involving a reduced systemic absorption was deeply felt.
Takai et al. (J. Pharmacobiodyn. vol. 5, no. 3, 1982, pages 200-207, database Medline abstract) teach that flunisolide is highly active in topical use, while systemically it is relatively weak; these characteristics could be attributable to its rapid metabolic inactivation in the liver. Nevertheless it gives no indication of the absorption levels of fluticasone and its noxious effects, and there is no suggestion that it would be of use in treating inflammatory intestinal disorders.
Flunisolide is a corticosteroid having formula ##STR1## and is used for the treatment of asthma chiefly as nasal and bronchial topical preparations, of glaucoma as ophthalmic topical preparations, of allergic or inflammatory conditions of the skin as creams and ointments.
This molecule is characterized by not high absorption levels and by a metabolic process (hepatic first pass) which rapidly transforms same into the metabolite 6-.beta.-hydroxyderivative, whose glucocorticoid activity is approx. 350 times lower than that of flunisolide.
In other words, the amount of flunisolide inevitably absorbed by the systemic way after topical application can never reach plasma levels interfering with the hypothalamus-hypophysis-adrenal gland axis.
THE PRESENT INVENTION
It has surprisingly been found that flunisolide and its esters administered by the topical rectal way are very active in the treatment of the aforesaid intestinal disorders and--unlike the steroids known so far--do not cause the adverse effects related to the interference with the hypothalamus-hypophysis-adrenal gland axis.
In fact, clinical trials carried out by the Applicant evidenced that an improvement of the basal symptomatology was obtained as early as after a 15-day topical rectal treatment at doses of 2 mg/die and that a 3-mg/die administration for 30 days did not cause any appreciable clinical modification to cortisol plasmatic concentrations, an indicator of the interference, if any, with the hypothalamus-hypophysis-adrenal gland axis.
Object of the present invention is, therefore, a topical rectal therapeutic composition containing, as active ingredient, flunisolide and/or one or more ester derivatives of same, in combination with suitable excipients and/or diluents, for the treatment of inflammatory intestinal disorders.
DETAILED DESCRIPTION OF THE INVENTION
The flunisolide used for the compositions of this invention is either anhydrous or in the corresponding hemihydrated form.
The expression "flunisolide ester derivatives" is used herein to mean the derivatives in which one or both hydroxylic functions in positions 11 and 21 of the aforesaid active ingredient have been esterified with C.sub.2 -C.sub.20 alkyl-, aryl- or arylalkyl- mono and/or polycarboxylic acids, with alkyl- or aryl mono and/or polysulphonic acids, aryl acids containing one or more carboxylic functions and one or more sulphonic functions and, in case of carboxylic and/or sulphonic polyfunctional acids, the remaining acid functions are either partially or completely salified with pharmaceutically acceptable cations, preferably sodium, potassium, magnesium, calcium.
Particularly preferred flunisolide esters are those formed with acetic acid, propionic acid, hexanoic acid, meta-sulfobenzoic acid and relative sodium meta-sulfobenzoate.
The compositions of the present invention are preferably in the form of enemas, suppositories, and foams.
The suppositories of this invention contain from 0.5 to 10 mg each, preferably from 1 to 5 mg each of flunisolide and/or its ester derivatives.
In addition to the active ingredient, the suppositories of the present invention contain excipients preferably consisting of semisynthetic solid glycerides of vegetable saturated fatty acids.
The rectal enemas of this invention are generally liquid compositions, solutions, emulsions or aqueous suspensions having an active ingredient content from 0-5 to 10 mg each, more preferably from 1 to 5 mg each, and generally containing preservatives, preferably selected among Parabens, chelating agents, such as for example ethylenediaminetetraacetic acid or the relative sodium salt. Should said enemas be emulsions or suspensions, they would also contain thickeners, such as carboxymethylcellulose, and should they be solutions they would contain thickeners-solubilizers, such as propylene glycol.
Said enemas may also contain compounds acting as pH regulators, preferably mineral or organic acids and/or pharmaceutically acceptable salts.
The rectal foams have an active ingredient content preferably from 0.5 to 10 mg/dose more preferably from 1 to 5 mg unitary dose.
Preferably, the rectal foams of this invention also contain:
traditional solubilizers, such as purified water and propylene glycol (the latter also acts as a thickener and is used for enemas) and solubilizers also protecting the skin, essentially consisting of partial glycerides of polyoxyethylenic saturated fatty acids;
emulsifiers, such as polysorbate 20 and mixtures of cetostearylic alcohol with sorbitan esterified with polyoxyethylenic fatty acids;
chelating agents, such as ethylenediaminetetraacetic acid, also in the form of sodium salt;
preservatives, such as Parabens--also used for enemas;
acidifying buffers, such as phosphoric acid and monobasic sodium or potassium phosphate;
propellants, such as hydrocarbons, e.g. isobutane, or fluorocarbons, e.g. dichlorodifluoromethane and dichlorotetrafluoroethane, or hydrochlorofluorocarbons or hydrofluorocarbons.
As concerns the pharmaceutical formulation, rectal foams--compared with enemas--have a lower water content and contain propellants, which are indispensable for dispensing the dose of drug to be administered.
It is just the presence of propellants that allows the dose dispensed at each release of the pressure valve--in case of multidose bottles--or on pressure release valve--in case of single-dose bottles--to spread out and reach the inmost regions of the intestine, e.g. the colon left splenic flexure.
The propelling properties can vary depending on the type and quantity of propellant used and, consequently, the foam can reach more or less distant regions of the intestine.





The following examples of therapeutic compositions for topical rectal use that are the object of this invention are conveyed by way of indication, not of limitation.
A) Rectal foam
1) One 14-dose pressure bottle (2 mg anhydrous flunisolide/dose) and one single-dose (2 mg anhydrous flunisolide) pressure bottle contain:
______________________________________ Multidose Single-dose______________________________________Anhydrous flunisolide 28 mg 2 mgCetostearylic alcohol + 830 mg 59.3 mgsorbitan polyoxyethylenicestersPolysorbate 20 553 mg 39.5 mgPropylene glycol 11.38 g 956 mgGlycerides of polyoxyethylenic 6.85 489 mgsaturated fatty acidsPurified water 10.17 g 726 mgMethyl p-hydroxybenzoate 39.5 mg 2.8 mgPropyl p-hydroxybenzoate 7.9 mg 0.56 mgEthylenediaminetetraacetic acid 15.8 mg 1.13 mgdisodium saltMonobasic sodium phosphate 313 mg 22.4 mgPhosphoric acid q.s. to pH 5Dichlorodifluoromethane 2.53 g 616 mgDichlorotetrafluoroethane 3.79 g 922 mg______________________________________
2) One 14-dose pressure bottle (2 mg hemihydrated flunisolide/dose) and one single-dose (2 mg hemihydrated flunisolide) pressure bottle contain:
______________________________________ Multidose Single-dose______________________________________Hemihydrated flunisolide 28.58 mg 2.04 mgCetostearylic alcohol + 830 mg 59.3 mgsorbitan polyoxyethylenicestersPolysorbate 20 553 mg 39.5 mgPropylene glycol 13.38 g 956 mgGlycerides of polyoxyethylenic 6.85 g 489 mgsaturated fatty acidsPurified water 10.17 g 726 mgMethyl p-hydroxybenzoate 39.5 mg 2.8 mgPropyl p-hydroxybenzoate 7.9 mg 0.56 mgEthylenediaminetetraacetic acid 15.8 mg 1.13 mgdisodium saltMonobasic sodium phosphate 313 mg 22.4 mgPhosphoric acid q.s. to pH 5Dichlorodifluoromethane 2.53 g 616 mgDichlorotetrafluoroethane 3.79 g 922 mg______________________________________
3) One 14-dose pressure bottle (2 mg anhydrous flunisolide/dose) and one single-dose (2 mg anhydrous flunisolide) pressure bottle contain:
______________________________________ Multidose Single-dose______________________________________Anhydrous flunisolide 28 mg 2 mgCetostearylic alcohol + 830 mg 59.3 mgsorbitan polyoxyethylenicestersPolysorbate 20 553 mg 39.5 mgPropylene glycol 13.38 g 956 mgGlycerides of polyoxyethylenic 6.85 g 489 mgsaturated fatty acidsPurified water 10.17 g 726 mgMethyl p-hydroxybenzoate 39.5 mg 2.8 mgPropyl p-hydroxybenzoate 7.9 mg 0.56 mgEthylenediaminetetraacetic acid 15.8 mg 1.13 mgdisodium saltMonobasic sodium phosphate 313 mg 22.4 mgPhosphoric acid q.s. to pH 5Isobutane 3.16 g 769 mg______________________________________
4) One 14-dose pressure bottle (2 mg hemihydrated flunisolide/dose) and one single-dose (2 mg hemihydrated flunisolide) pressure bottle contain:
______________________________________ Multidose Single-dose______________________________________Hemihydrated flunisolide 28.58 mg 2.04 mgCetostearylic alcohol + 830 mg 59.3 mgsorbitan polyoxyethylenicestersPolysorbate 20 553 mg 39.5 mgPropylene glycol 13.38 g 956 mgGlycerides of polyoxyethylenic 6.85 g 489 mgsaturated fatty acidsPurified water 10.17 g 726 mgMethyl p-hydroxybenzoate 39.5 mg 2.8 mgPropyl p-hydroxybenzoate 7.9 mg 0.56 mgEthylenediaminetetraacetic acid 15.8 mg 1.13 mgdisodium saltMonobasic sodium phosphate 313 mg 22.4 mgPhosphoric acid q.s. to pH 5Isobutane 3.16 g 769 mg______________________________________
B) Suppositories
5) One suppository (2 mg anhydrous flunisolide) contains:
______________________________________Anhydrous flunisolide 2 mgGlyceric esters of 1498 mgsaturated fatty acids______________________________________
6) One suppository (2 mg hemihydrated flunisolide) contains:
______________________________________Hemihydrated flunisolide 2.04 mgGlyceric esters of 1498 mgsaturated fatty acids______________________________________
C) Enema
7) One 60 ml single-dose bottle (2 mg anhydrous flunisolide) contains:
______________________________________Anhydrous flunisolide 2 mgpropylene glycol 24 gEthylenediaminetetraacetic acid 15 mgsodium saltHydrochloric acid q.s. to pH 5Purified water q.s. to 60 ml______________________________________
8) One 60 ml single-dose bottle (2 mg hemihydrated flunisolide) contains:
______________________________________Hemihydrated flunisolide 2.04 mgPropylene glycol 24 gEthylenediaminetetraacetic acid 15 mgsodium saltHydrochloric acid q.s. to pH 5Purified water q.s. to 60 ml______________________________________
The excipients of the above compositions are reported below.
Rectal foam
______________________________________EXCIPIENT FUNCTION______________________________________Cetostearyl alcohol containing emulsifiersorbitan esterified withpolyoxyethylenic fatty acidsPolysorbate 20 emulsifierPartial glycerides of polyoxyethylenic solubilizer-skin protectorsaturated fatty acidsPropylene glycol solubilizer-thickenerMethyl p-hydroxybenzoate sodium salt preservativePropyl p-hydroxybenzoate sodium salt preservativeEthylenediaminetetraacetic acid chelating agentdisodium saltPurified water solubilizing vehicleMonobasic sodium phosphate and pH regulating bufferphosphoric acidDichlorodifluoromethane propellantDichlorotetrafluoroethane propellantIsobutane propellant______________________________________
Suppository
______________________________________EXCIPIENT FUNCTION______________________________________Semisynthetic solid glycerides mass for supporitory (solid vehicle)______________________________________
Enema
______________________________________EXCIPIENT FUNCTION______________________________________Propylene glycol solubilizer-thickenerEthylenediaminetetraacetic acid chelating agentsodium saltHydrochloric acid acidifierPurified water solubilizing vehicle______________________________________
CLINICAL TRIALS
FLUNISOLIDE ENEMA (2 and 3 mg)
Preliminary clinical trials were conducted with Flunisolide in the form of enema using No. 18 patients of both sexes suffering from ulcerative colitis, limited to the splenic flexure. Patients were divided into two groups and treated with 2 mg/die and 3 mg/die, respectively, for 30 days.
The obtained results clearly indicate that the drug has an excellent therapeutic efficacy and above all is well tolerated, especially in relation to the inferference with the hypothalamus-hypophysis-adrenal gland axis.
In particular treatments with Flunisolide at a dose of 2 mg/die and 3 mg/die for 15 and 30 days always produced statistically significant improvements (Mann-Whitney's "U" test) of the basal sympotomatology as far as the clinical and the sigmoidoscopic parameters are concerned (cf. Table 1 attached hereto).
As concerns drug toleration to the treatment and in particular the interference with the hypothalamus-hypophysis-adrenal gland axis, the treatment with flunisolide at the higher dose (3 mg/die) for 30 days never determined cortisolemia values below normality.
TABLE 1______________________________________Average values .+-. standard error of the mean of scores detectedbasally (T.sub.0) and after 15 (T.sub.15) and 30 (T.sub.30) days oftreatmentwith flunisolide at the dose of 2 and 3 mg/die. Results of thestatistical evaluation made by Mann-Whitney's "U" test comparedwith the respective basal values.(score 1 = normal; score 2 = mild; score 3 = moderate)PARAMETERS T.sub.0 T.sub.15 T.sub.30______________________________________Flunisolide 2 mg/die (No. 10)CLINICAL 2.7 .+-. 0.2 1.9 .+-. 0.2 1.5 .+-. 0.2 -- * **SIGMOIDOSCOPIC 2.7 .+-. 0.2 2.2 .+-. 0.1 1.6 .+-. 0.2 -- * **Flunisolide 3 mg/die (No. 8)CLINICAL 2.9 .+-. 0.1 2.0 .+-. 0.2 1.6 .+-. 0.2 -- ** **SIGMOIDOSCOPIC 3.0 .+-. -- 2.4 .+-. 0.2 2.1 .+-. 0.2 -- ** **______________________________________ *P .ltoreq. 0.05; **P .ltoreq. 0.01
Claims
  • 1. A method of locally treating inflammatory intestinal diseases comprising administering to a patient in need of such treatment a pharmaceutically effective amount of flunisolide or a flunisolide ester, said pharmaceutically effective amount being administered by a topical rectal route.
  • 2. Therapeutic method for the treatment of ulcerative colitis, inflammatory intestinal diseases resulting in mild ulcerative colitis or in a slightly different, but pathologically similar syndrome or of Chron's disease, comprising the topical, rectal application of a pharmaceutical composition containing as active ingredient anhydrous or hemihydrated flunisolide and/or one or more ester derivatives of same, in combination with suitable excipients and/or diluents, said pharmaceutical composition containing between 0.5 and 1 mg of active ingredient per unitary posological dose.
  • 3. Therapeutic method according to claim 2 wherein the unitary posological dose is between 1 and 5 mg.
  • 4. Therapeutic method according to claim 2 wherein the pharmaceutical composition is in the suppository form.
  • 5. The therapeutic method according to claim 4 wherein said suppository form contains excipients selected from the group consisting of semisynthetic glycerides of vegetable saturated fatty acids.
  • 6. The therapeutical method according to claim 2 wherein the pharmaceutical composition is in the rectal enema form.
  • 7. The therapeutic method according to claim 6 wherein said rectal enema form is a solution, which contains preservatives chelating agents, pH regulators and thickeners-solubilizers.
  • 8. The therapeutic method according to claim 6 wherein said rectal enema form is an emulsion or an aqueous suspension, which contains preservatives chelating agents, and thickeners-emulsifiers.
  • 9. The therapeutic method according to claim 2 wherein the pharmaceutical composition is in the rectal foam form.
  • 10. The therapeutic method according to claim 9 wherein said rectal foam form further comprises emulsifiers, water, thickeners-solubilizers, and thickeners-solubilizers also exerting a skin protective action, preservatives, chelating agents, acidifying buffers, and propellents.
  • 11. The therapeutic method according to claim 2 wherein the flunisolide ester derivatives are those having one or both hydroxylic functions in positions 11 and 21 of the aforesaid active ingredient eserified with C.sub.2 -C.sub.20 alkyl-, aryl- or arylalkyl- mono and/or polycarboxylic acids, with alkyl- or aryl mono and/or polysulphonic acids, aryl acids containing one or more carboxylic functions andone or more sulphonic functions and, in case of carboxylic and/or sulphonic polyfunctional acids, the remaining acid functions are either partially or completely salified with pharmaceutically acceptable cations.
  • 12. The therapeutic method according to claim 2 wherein the used flunisolide esters are the esters formed with acetic acid, propionic acid, hexanoic acid, meta-sulfobenzoic acid and relevant sodium meta-sulfobenzoate.
Priority Claims (1)
Number Date Country Kind
MI92A2657 Nov 1992 ITX
PCT Information
Filing Document Filing Date Country Kind 102e Date 371c Date
PCT/EP93/03228 11/18/1993 5/17/1995 5/17/1995
Publishing Document Publishing Date Country Kind
WO94/12187 6/9/1994
US Referenced Citations (3)
Number Name Date Kind
3124571 Ringold et al. Mar 1964
4427670 Ofuchi et al. Jan 1984
4552872 Cooper et al. Nov 1985
Foreign Referenced Citations (1)
Number Date Country
0 278 174 Aug 1988 EPX
Non-Patent Literature Citations (3)
Entry
Physicians Desk Reference, 46th ed. pp. 2244-2245, 1992.
Craig et al., "Modern Pharmacology", pp. 15-16, 1982.
Takai, et al., "The Predominance of Flunisolide In The Topical Use Of Anti-Inflammatory Steroids", J. Pharmacobiodyn, vol. 5, No. 3, 1982,pp. 200-207 (Abstract)*.