TREA

Treatment of endometriosis

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Information

  • Patent Grant
  • 5166200
  • Patent Number
    5,166,200
  • Date Filed
    Thursday, April 11, 1991
    33 years ago
  • Date Issued
    Tuesday, November 24, 1992
    32 years ago
Information
Abstract
A remedy for endometriosis comprising, as an active ingredient, 14.alpha.-hydroxy-4-androstene-3,6,17-trione or an ester derivative thereof, can effectively treat endometriosis by the strong aromatase-inhibitory activity without giving serious side effects.
Description

BACKGROUND OF THE INVENTION
(1) Field of the Invention
The present invention relates to a novel method for the treatment of endometriosis.
(2) Description of the Prior Art
Endometriosis appears as a product of atopic proliferation of endometrium. Internal endometriosis includes adenomyosis of uterus and endosalpingosis, and external endometriosis includes endometriosis of pelvic cavity and ectopic endometriosis. Endometriosis appears at a high incidence in females of 20-45 years old and its incidence has shown a steady increase in recent years, i.e., endometriosis is seen in 15-20% of females of 20-35 years old. Endometriosis is generally accompanied by dysmenorrhea and has a close relation to acyesis. Endometriosis is generally treated by pseudomenopausal treatment using danazol [Bonzal (trade name) manufactured by Tokyo Tanabe Seiyaku]. Buserelin [Suprecur (trade name) manufactured by Hoechst Japan] which is a LH-RH derivative has also been tried. However, danazol gives side effects such as dyshepatia, masculinization and the like and buserelin gives side effects such as hyposexuality, hot flushes and the like.
When medicinal treatments show no effect, a surgical treatment such as hysterectomy, lesion removal or the like is adopted but is not a desirable approach in view of the patient's response, the after effect, etc.
Therefore, development of an effective a drug is desired.
Meanwhile, the present inventors have for many years studied aromatase (a steroidogenesis enzyme) inhibitor.
It is known that 14.alpha.-hydroxy-4-androstene-3,6,17-trione and ester derivatives thereof have a strong aromatase-inhibitory activity. These compounds are disclosed in Japanese Patent Application Laid-Open Nos. 192794/1988, 131193/1989, etc. The present inventors studied the pharmacological activities of the compounds and found that the aromatase-inhibitory activity shown by the compounds is effective for treatment of endometriosis.
SUMMARY OF THE INVENTION
The object of the present invention is to provide a remedy for endometriosis showing a strong aromatase-inhibitory activity.
The above object of the present invention can be achieved by treating endometriosis with, 14.alpha.-hydroxy-4-androstene-3,6,17-trione or an ester derivative thereof.





DETAILED DESCRIPTION OF PREFERRED EMBODIMENTS
The active ingredients used in the present invention are represented by the following structural formulas ##STR1## wherein R represents a --OCOR.sub.1 group (R.sub.1 is a lower alkyl group, an aryl group or an aralkyl group).
In the present invention, the lower alkyl group refers to a straight or branched carbon chain of 1-6 carbon atoms, unless otherwise specified. Therefore, the lower alkyl group includes, for example, methyl, ethyl, propyl, butyl, pentyl, hexyl, isobutyl, tert-butyl and isopropyl. The aryl group includes, for example, phenyl and tolyl. The aralkyl group includes, for example, benzyl and phenylethyl. The ester group thereof (--OCOR.sub.1) includes, for example, the followings. ##STR2## The ester derivative is preferably a propionate (6-OAp) or a benzoate (6-OAb).
The above compounds can be synthesized by the methods described in Japanese Patent Application Laid-Open Nos. 192794/1988 and 131193/1989. That is, 14.alpha.-hydroxy-4-androstene-3,6,17-trione is synthesized from 6.beta.,14.alpha.-dihydroxy-4-androstene-3,17-dione according to an ordinary oxidation reaction (for example, Jones' oxidation reaction) and then is reacted with propionic anhydride or benzoyl chloride to obtain a propionate or a benzoate.
These compounds are made into pharmaceutical preparations and then administered in forms such as by an oral agent, suppository, injection and the like. In preparing an oral agent, there are used carriers such as mannitol, lactose, starch, magnesium stearate, cellulose, glucose, saccharose and the like; and an absorption accelerator, etc. can be added as necessary. The oral agent can be used in combination with a conventional remedy for endometriosis.
In the treatment of endometriosis, the active compound is administered daily for 1-6 months in an amount of 10 mg to 1 g per day.
The remedy for endometriosis according to the present invention specifically inhibits aromatase (a steroidogenesis enzyme) to reduce estradiol (Ez), thereby exhibiting a therapeutic effect for endometriosis This action mechanism is different from those of danazol and buserelin, and the present remedy for endometriosis provides very high utility.
6-OA has very low toxicity and animal tests indicated its LD.sub.50 is more than 2,000 mg/kg. The ester derivatives of 6-OA have low toxicity as well. Therefore, these compounds can provide a very safe remedy.
The present invention is hereinafter described in more detail by way of Examples and Test Examples.
______________________________________Example 1 (Tablets)______________________________________14.alpha.-Hydroxy-4-androstene-3,6,17-trione (6-OA) 200 mgHydroxy propyl cellulose (HPC) 30 mgLactose 67 mgMagnesium stearate 3 mgTotal 300 mg______________________________________
The above components were mixed to prepare tablets so that each tablet contained them in the above amounts.
______________________________________Example 2 (Tablets)______________________________________6-OA 200 mgHPC 30 mgHydroxy propyl methyl cellulose (TC-5) 6 mgLactose 61 mgMagnesium stearate 3 mgTotal 300 mg______________________________________
The above components were mixed to prepare tablets so that each tablet contained them in the above amounts. In this case, an aqueous TC-5 solution was used as a binder, and granules were prepared according to a wet method and made into tablets.
______________________________________Example 3 (Tablets)______________________________________14.alpha.-Hydroxy-androsta-4,6-diene-3,17-dione-6- 235.4 mg*propionate(6-OAp)HPC 30 mgLactose 80.6 mgMagnesium stearate 4 mgTotal 350 mg______________________________________ (*Equivalent to 200 mg of 6OA.)
The above components were mixed to prepare tablets so that each tablet contained them in the above amounts.
______________________________________Example 4 (Tablets)______________________________________6-OAp 235.4 mgHPC 30 mgTC-5 6 mgLactose 74.6 mgMagnesium stearate 4 mgTotal 350 mg______________________________________
The above components were mixed to prepare tablets so that each tablet contained them in the above amounts. In this case, an aqueous TC-5 solution was used as a binder, and granules were prepared according to a wet method and made into tablets.
______________________________________Example 5 (Capsules)______________________________________6-OA 200 mgHPC 30 mgLactose 116 mgMagnesium stearate 4 mgTotal 350 mg______________________________________
The above components were mixed and packed into hard capsules specified by the Japanese Pharmacopoeia, to obtain each capsule containing the above components in the above amounts.
______________________________________Example 6 (Capsules)______________________________________6-OA 200 mgHPC 30 mgTC-5 8 mgLactose 108 mgMagnesium stearate 4 mgTotal 350 mg______________________________________
The above components were mixed and packed into hard capsules specified by the Japanese Pharmacopoeia, to obtain each capsule containing the above components in the above amounts. In this case, an aqueous TC-5 solution was used as a binder, and granules were prepared according to a wet method and packed into capsules.
______________________________________Example 7 (Capsules)______________________________________6-OAp 235.4 mgHPC 30 mgLactose 130.6 mgMagnesium stearate 4 mgTotal 400 mg______________________________________
The above components were mixed and packed into hard capsules specified by the Japanese Pharmacopoeia, to obtain each capsule containing the above components in the above amounts.
______________________________________Example 8 (Capsules)______________________________________6-OAp 235.4 mgHPC 30 mgTC-5 8 mgLactose 122.6 mgMagnesium stearate 4 mgTotal 400 mg______________________________________
The above components were mixed and packed into hard capsules specified by the Japanese Pharmacopoeia, to obtain each capsule containing the above components in the above amounts. In this case, an aqueous TC-5 solution was used as a binder, and granules were prepared according to a wet method and packed into capsules.
TEST EXAMPLE 1
In this Test Example, effects of administration of 6-OA and 6-enol ester compounds thereof on estradiol (Ez) reduction were examined.
Test method
Test (1) Comparison by subcutaneous administration
20 SD strain female rats of 8-week old were used as test animals. They were divided into four groups each consisting of 5 rats. To all the rats was subcutaneously injected pregnant mare serum gonatropin (PMSG) in an amount of 100 IU/body once every other day (6 times in total). In the beforenoon of the next day of the final (6th) administration of PMSG, 0.5 ml of a solvent, 50 mg/kg of 6-OA, 50 mg/kg of 6-OAp and 50 mg/kg of 6-OAb were subcutaneously administered to group I (control group), group II, group III and group IV, respectively.
After 3 hours from the administration, the rats were subjected to abdomen opening under etherization and then to exsanguination from the main vein. The blood collected from each rat was subjected to serum separation, and the Ez in the serum was determined by radioimmunoassay.
A physiological saline solution containing 0.3% of hydroxy propyl cellulose (HPC) was used as the solvent. 6-OA, 6-OAp and 6-OAb were each suspended in the solvent in such a concentration that the administration amount of the resulting suspension per rat became 0.5 ml.
Test (2) Comparison by oral administration
The type, age, number and grouping of test animals were the same as in Test (1).
All of the rats were subcutaneously injected with PMSG, in the same manner as in Test (1), in an amount of 100 IU/body once every other day (6 times in total).
Before noon of the next day of the final (6th) administration of PMSG, 0.5 ml of a solvent, 100 mg/kg of 6-OA, 100 mg/kg of 6-OAp and 100 mg/kg of 6-OAb were orally administered to group I (control group), group II, group III and group IV, respectively.
Aftr 6 hours from the administration, the rats were subjected to exsanguination. The blood collected from each rat was subjected to serum separation, and the Ez in the serum was determined by radioimmunoassay.
The solvent used was the same as in Test (1). 6-OA, 6-OAp and 6-OAb were each suspended in the solvent in such a concentration that the administration amount of the resulting suspension per rat became 0.5 ml.
Results
The Ez concentrations in serum of Test (1) and Test (2) are shown in Table 1 and Table 2.
TABLE 1______________________________________Test (1) Subcutaneous administrationI (HPC) II (6-OA) III (6-OAp) IV (6-OAb)______________________________________Average 0.572 0.262 0.230 0.390S.D. .+-.0.079 .+-.0.049 .+-.0.035 .+-.0.083 (unit: ng/ml)______________________________________
TABLE 2______________________________________Test (2) Oral administrationI (HPC) II (6-OA) III (6-OAp) IV (6-OAb)______________________________________Average 0.522 0.291 0.226 0.422S.D. .+-.0.072 .+-.0.038 .+-.0.036 .+-.0.041 (unit: ng/ml)______________________________________
Conclusion
The 6-OA group, the 6-OAp group and the 6-OAb group, as compared with the control group, showed a strong Ez-reducing effect in both cases of subcutaneous administration and oral administration. The 6-OAp group showed a stronger Ez-reducing effect than the 6-OA group and the 6-OAb group.
TEST EXAMPLE 2
In this Test example, effect of administration of 6-OAp on model rats of endometriosis was examined.
SD strain female rats of 7-week old weighing 170-210 g were used as test animals. In these rats, an endometrial segment (about 5 mm.times.5 mm) was removed from the left uterine horn and autoplanted under the left renal capsule, and formation of cysts in the transplanted endometrium was examined. Those rats which had developed cysts of 0.5-2.0 mm in height in the transplanted endometrium, were used for test.
The rats were divided into three groups. To group I (control group) was orally administered a physiological saline solution containing 0.3% of hydroxy propyl cellulose (HPC) daily in an amount of 0.5 ml/day. To group II was orally administered 6-OAp daily in an amount of 100 mg/kg/day. In this case, 6-OAp was suspended in a physiological saline solution containing 0.3% of HPC in such a concentration that the administration amount of the resulting suspension per rat became 0.5 ml. Group III (positive control) was subjected to ovary removal.
Each rat was subjected to abdomen opening after 3 weeks from the start of administration or after the ovary removal and examined for the presence of cysts.
Chi-square test was used for the statistical analysis of the test data obtained.
The results of the above test are shown in Table 3.
TABLE 3______________________________________6-OAp administration Cysts Cysts present absent Total Disappearance______________________________________Control group 20 rats 2 rats 22 rats 9%6-OAp group* 13 9 22 41Ovary-removed 0 9 9 100group**______________________________________ *There is a significant difference (significant level: 5% relative to control group). **There is a significant difference (significant level: 1% relative to control group).
6-OAp was effective for experimental endometriosis of rats when orally administered daily for 3 weeks in an amount of 100 mg/kg/day.
The present invention provides a remedy for endometriosis employing 14.alpha.-hydroxy-4-androstene-3,6,17-trione or 6-enol ester derivative thereof. This remedy has an action mechanism different from those of conventional remedies for endometriosis and can treat endometriosis effectively without serious side effects.
As a result, endometriosis can be treated effectively without any surgical treatment.
Claims
  • 1. A method for treating endometriosis, which comprises administering to a woman suffering therefrom an effective amount of 14.alpha.-hydroxy-4-androstene-3,6,17-trione represented by the following general formula (I) or an enol ester derivative thereof represented by the following general formula (II) ##STR3## wherein R represents a --OCOR.sub.1 group in which R.sub.1 is lower alkyl, aryl or aralkyl.
  • 2. The method according to claim 1, wherein the compound of Formula (I) or Formula (II) is administered orally.
  • 3. The method according to claim 1, wherein the compound administered is 14.alpha.-hydroxy-4-androstene-3,6,17-trione.
  • 4. The method according to claim 1, wherein the compound administered is 14.alpha.-hydroxy-androsta-4,6-diene-3,17-dione-6-propionate.
  • 5. The method of claim 4, wherein the compound is administered orally.
  • 6. The method of claim 5, wherein the compound administered is 14.alpha.-hydroxy-androsta-4,6-diene,3-17-dione-6-benzoate.
Priority Claims (1)
Number Date Country Kind
2-97379 Apr 1990 JPX
Foreign Referenced Citations (2)
Number Date Country
0265119 Apr 1988 EPX
0300062 Jan 1989 EPX
Non-Patent Literature Citations (5)
Entry
Patent Abstracts of Japan, vol. 13, No. 379 (C-628)[3727]Aug. 22, 1989.
Yamamoto et al., "Inhibitory Effect of a New Androstenedione Derivative, 14.alpha.-hydroxy-4-Androstene-3,6,17-Trione (14.alpha.-OHAT) on Aromatase Activity of Human Uterine Tumors," J. Steroid Biochem., vol. 36, No. 6, pp. 517-521 (1990).
Dictionnaire des Termes Techniques de Medecine, 20th ed., pp. 414-415 (1983).
CA: 110(21)-191258n-Yoshihama et al. (May 1989).
CA: 110(23)-2148112-Nakakoshi et al. (Dec. 1989).