CA1278748C - Pharmaceutical composition for combination therapy of hormone dependent cancers - Google Patents
Pharmaceutical composition for combination therapy of hormone dependent cancersInfo
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- CA1278748C CA1278748C CA000488048A CA488048A CA1278748C CA 1278748 C CA1278748 C CA 1278748C CA 000488048 A CA000488048 A CA 000488048A CA 488048 A CA488048 A CA 488048A CA 1278748 C CA1278748 C CA 1278748C
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- cancer
- sex steroid
- antiandrogen
- inhibitor
- antiestrogen
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Abstract
ABSTRACT
This invention relates to a method of treating sex steroid dependent cancers in a warm-blooded animal which comprises administering a pharmaceutically effective amount of an antiandrogen and/or an antiestrogen and/or at least one inhibitor of sex steroid biosynthesis to the animal whose hormone output of the testes or ovaries, respectively, is blocked, with the proviso that the method of treating prostate cancer comprises administering pharmaceutically effective amounts of an antiandrogen and at least one inhibitor of sex steroid biosynthesis and with the further proviso that, if antiestrogen is used in treating breast cancer it is used in association with an antiandrogen and/or at least one hinhibitor of sex steroid biosynthesis. The invention further relates to kits containing pharmaceutical compositions containing the active ingredients to be used in the novel combination therapy.
This invention relates to a method of treating sex steroid dependent cancers in a warm-blooded animal which comprises administering a pharmaceutically effective amount of an antiandrogen and/or an antiestrogen and/or at least one inhibitor of sex steroid biosynthesis to the animal whose hormone output of the testes or ovaries, respectively, is blocked, with the proviso that the method of treating prostate cancer comprises administering pharmaceutically effective amounts of an antiandrogen and at least one inhibitor of sex steroid biosynthesis and with the further proviso that, if antiestrogen is used in treating breast cancer it is used in association with an antiandrogen and/or at least one hinhibitor of sex steroid biosynthesis. The invention further relates to kits containing pharmaceutical compositions containing the active ingredients to be used in the novel combination therapy.
Description
1~787~8 PHARMACEUTICAL COMPOSITION FOR COMBINATION THERAPY
OF HORMONE DEPENDENT CANCERS
This invention relates to a combination therapy of sex steroid dependent cancers in susceptible warm-blooded animals including humans comprising administering to such animals whose hormone output of their testes or ovaries respectively is blocked a pharmaceutically effective amount of an antiandrogen and/or an antiestrogen and/or at least one inhibitor of sex steroid biosynthesis to the animal whose hormone output of the testes or ovarles, respectively, is blocked, wlth the provlso that the method of treating prostate cancer comprises admlnistering pharmaceutically effective amounts of an antiandrogen and at least one inhibitor of sex steroid biosynthesis and the method of treating breast cancer comprises administering a pharmaceutically effective amount of an antiandrogen or of at least one inhibitor of sex steroid biosynthesis or of an antiandrogen and an antiestrogen or of an antiandrogen and at least one inhibitor of sex steroid biosynthesis or of an antiestrogen and at least one inhibitor of sex steroid biosynthesis or of an intiandrogen and an antiestrogen and at least one inhibitor of sex steroid biosynthesis. In the therapy of sex steroid dependent l~7s7~a cancers such as testicular cancer, ovarian cancer, colon-rectal cancer, renal cancer, pancreatic cancer, liver cancer, stomach cancer, skin cancer, uterine cancer, brain cancer and larynx cancer all above listed combinations are applicable. The hormone output of the animal's testes or ovaries, respectively, can be blocked by surgical or chemical means. (In post-menopausal women~ the attending clinicians may decide that the hormone output of the ovaries need not be blocked.) While various investigators have been studying hormone~dependent breast and prostate cancer, none have proposed the combination therapy of this invention.
A. V. Schally et al., Cancer Treatment Reports, 68, (No. 1) 281-289 tl984), summarize the results of animal and clinical studies on growth inhibition of hormone-dependent mammary and prostate tumors by use of analogues of luteinizing hormone-releasiny hormones, the so-called LH-RH agonists and suggest that LH-RH analogs and/or antagonists may have potential for treating breast cancer.
T. W. Redding and A. V. Schally, Pro. Natl~
Acad. Sci. USA, R0, 14S9-1462 ~1983), disclose reduction of estrogen-dependent mammary tumors in rats and mice by use of an LH-RH agonist, [D-Trp6]LH-RH or of two specific antagonists and inhibition of prostate tumor growth in rats of chronic use of an LH-RH
agonist, [D-Trp6] LH-RH.
In U.S. Patent 4,071,622, it is disclosed that use of certain LH-RH agonists causes regression of DMBA-induced mammary carcinoma in rats.
In U.S. Patent 4,472,382, it is disclosed that prostate adenocarcinoma, benign prostate 1'~787~L8 hypertrophy and hormone-dependent mammary tumors may be treated with various LH-RH agonists and that prostate adenocarcinoma and benign hypertrophy may be treated by use of various LH-RH agonists and an antiandrogen.
However, there is no suggestion or disclosure of the present invention.
Some clinical improvement in premenopausal women with breast cancer by use of the two LH-RH
agonists, Buserelin and Leuprolide, is also reported by H.A. Harvey et al. "LH-RH analogs in the treatment of human breast cancer", LH-RH and its Analogs - A New Class of Contraceptive and Therapeutic Aqents (B.H.
Vickery and J.J. Nestor, Jr., and E.S.E. Hafez, eds) Lancester, MTP Press, ~1984) and by J.G.M. Klijn et al.
"Treatment with luteinizing hormone releasing hormone analogue (Buserelin) in premenopausal patients with metastatic breast cancer", Lancet, 1, 1213-1216 (1982).
Treatment of advanced breast cancer with aminoglutethimide after therapy with the antiestrogen, Tamoxifen is clisclosed by A.V. Buzdar et al., Cancer, 50, 170~-1712 (1982).
Il. Flax et al., Lancet, l204-1207, (1973), suggest some women's br~st cancers are androgen-dependent.
In U.S. Patent 4,329,364, it is disclosed that the antiandrogen, 4'-nitro-3'-trifourormethyl isobutyranilide may be used for treatment of prostatic cancer.
Some clinical improvement in men with prostate cancer by use of the two LH-RH agonists, Buserelin and Leuprolide, is also reported by N. Faure et al. at pages 337-350 and by R.J. Santen et al. at pages 351-364, respectively, LH-RH and its Analogs - A
New Class of Contraceptive and Therapeutic Aqents (B.H.
l~7a7~s Vickery and J.J. Nestor, Jr., and E.S.E. Hafez, eds) Lancester, MTP Press, (1984).
R. Santen et al., The Journal of Steroid Biochemistry, Volume 20, No 6B, at page 1375 (1984), disclose that use of ketoconazole in combination with chronic administration of Leuprolide in rodents decreased basal and Leuprolide stimulated testosterone levels.
D. Kerle et al., The IJournal of Steroid Biochemistry, Volume 20, No 6B, at page 1395 (1984) disclose that the combined use of a LH-RH analogue and ketoconazole produced objective responses in some prostate cancer patients who have relapsed or failed to respond to treatment with a LH-RH analogue alone.
F. Labrie et al., Abstracts of 7th International Congress of Endrocrinology, Excerpta ~1edica (1984) at page 98 discloses that treatment of prostate cancer patients with LH-RH agonists alone causes a transient increase in serum androgen levels lasting for 5 to 15 days before castration levels are reached. While F. Labrie et al. recommends that orchiectomy, estrogen and LH-RH agonists alone should not be further used for treatment of prostate cancer in the absen~e of a pure antiandrogen, there still is a need fo~ a method of treatment of prostate canceL that effects mOLe complete androgen blockage at the start as well as during the full period of treatment.
F. Labrie et al., The Prostate, 4, 579-594 ~1983), disclose that use of a combination therapy of an LH-RH agonist (Buserelin) and an antiandrogen (Anandron) to treat advanced prostate cancer in previously untreated patients effects simultaneous inhibition of androgens of both testicular and adrenal origin.
l~7a~s F. Labrie et al., J. Steroid Biochem., 19, 99-1007 (1983), disclose the treatment of prostate cancer by the combined administration of an LH-RH
agonist and an antiandrogen. Labrie et al. disclose animal and clinical data in support of the proposition that the combined LH-RH/antiandrogen treatment neutralizes the stimulatory influence of all androgens on the development and growth of androgen-dependent prostatic cancer.
In U.S. Patent 4~,094,994, it is disclosed that the use of antiestrogens such as meso-3,4-bis(3'-hydroxyphenyl)hexane inhibits MCF7 human breast tumor cells. In fact, the inhibitory activity of the anti-estrogen was antagonized by estradiol.
H. Mouridsen et al,. Cancer Treatment Review 5, 131-141, (1978), disclose that Tamoxifen, an antiestrogen is effective in remission of advanced breast cancer in about 30~ of the patients treated.
J.G.M. Klijn et al., ~J. Steroid Biochem, Vol. 20 l~o. 6B), 1381 ~198~), disclosed the combined use of the antiestrogen, Tamoxif0n, and the LH-RH
agonist, Buscrelin, for tr0atment of breast cancer is krlown, but obj0etiv~ remiss;on of such cancers remains low ~35'~).
The present invention provides a new combination therapy of sex steroid dependent cancers which inhibits tumor growth and metastases and causes in some instances complete remission. The invention is exemplified by detailed discussion of the therapy of breast cancer and prostate cancer. The therapy of other sex steroid dependent cancers (listed above) is carried out analogously.
In one aspect, the invention provides a method of treating sex steroid dependent cancers such l~7874a as, for example, breast cancer in a warm-blooded female animal in need of such treatment which comprises administering to said animal whose hormone output of the ovaries is blocked, a therapeutically effective amount of an antiandrogen or a pharmaceutical composition thereof. The ovarian hormonal secretions of said animal can be blocked by surgical or chemical means. In one aspect, the invention provides a method of treating sex steroid dependent cancers such as, for example, breast cancer in a castrated warm-blooded female animal, i.e., such a female animal whose ovaries are blocked by surgical or chemical means from secreting estrogen, which comprises administering to such a female in need of such treatment an antiandrogen in association with at least one inhibitor of sex steroid biosynthesis and, optionally, an antiestrogen, or pharmaceutical compositions thereof, in amounts sufficient to treat such cancers, e.g., breast cancer. In another aspect, the invention provides a method of treating sex steroid dependent cancers such as, for examplo, breast cancer in a warm-blooded animal in need of such treatment which comprises blocking the ovarian hormonal secretions of said animal hy surgical or chemical means and administering to said animal therapeutically effective amounts of an antiestrogen in association with at least one inhibitor of sex steroid biosynthesis, or pharmaceutical compositions thereof.
In one aspect, the invention provides a method of treating sex steroid dependent cancers such as, for example, breast cancer in a warm-blooded animal whose ovaries are blocked by surgical or chemical means from secreting estrogen, which comprises administering to an animal in need of such treatment an antiandrogen and an antiestrogen, or pharmaceutical compositions thereof, 1-~787~8 in amounts sufficient to treat such cancers, e.g., breast cancer.
By completely bloclcing sex steroids ~androgens and estrogens) production and/or action, the present invention provides a method of inhibiting the growth of sex steroid-sensitive tumors, e.g., breast tumors in warm-blooded animals having such tumors.
In female mammals, the ovaries may be surgic-ally removed ~oophorectomy) but preferably the secretion of estrogens from the ovaries is blocked by chemical castration by administering an effective amount of an LH-RH agonist or antagonist. Thus, in a preferred aspect, the present invention provides a method of treating sex steroid dependent cancers such as, for example, breast cancer in a warm-blooded female animal, which comprises administering to such a female in need of such treatment an LH-RH agonist or antagonist, in association with an antiandrogen and/or an antiestrogen and/or at least one inhihitor of sex steorid biosynthesis according to the invention, preferably an antiandrogen. Preferably in this treatment at least one inhibitor of sex steroid biosynthesis, or pharmaceutical compositions thereof, and/or antiestrogen is administered.
In its preferred aspect, the LH-RH agonist is administered parenterally ~subcutaneously or intra-muscularly or intranasal) and, in association there-with, the antiandrogen and the inhibitor of sex steroid biosynthesis and/or antiestrogen are each administered orally.
Thus, this invention provides a novel method for effective treatment of sex steroid dependent cancers such as, for example, female breast cancer, in the absence of antiestrogen. In addition, the amounts l~7s7~a of antiestrogen required when administered in association with this combined therapy are lower than normally used in prior art methods, e.g., J.G.M. Klijn et al., J. Steroid Biochem. 20 (No. 6B) 1381 ~1984), to treat breast cancer, and thus, the harmful effects of relatively large doses of antiestrogen are minimized.
In one preferred aspect, the present invention provides an effective method of treating sex steroid dependent cancers such as, for example, breast cancer in warm-blooded female animals in need of such treatment by administering an LH-RH agonist or antagonist, in association with an antiandrogen and an inhibitor of sex steroid biosynthesis or pharmaceutical compositions thereof in amounts sufficient to inhibit tumor growth. These active compounds can be administered together or in any order as discussed hereinafter.
To assist in determining the effect of the treatment, blood plasma concentrations of the sex steroids of adrenal and ovarian origin, i.e., precursor steroids, androgens and estrogens, and tumor size are measured. Lowered concentrations of sex steroids and reduction in tumor size are indicative of successful treatment, e.g. inhibition of tumor growth using active compounds described herein in accordance with the present invention. The concentrations of adrenal androgens and estrogens such as dehydroepiandrosterone (DHEA), DHEA-sulfate tDHEAS), androst-5-ene-3R,17B-diol (~5-diol) and, the ovarian estrogen, 17B-estradiol (E2) are measured by standard methods well known to those skilled in the art, see for example F. Labrie et al., The Prostate, _, 579-594 (1983).
The change in tumor size is measured by standard physical methods well known to those skilled l~7~74a in the art, e.g., bone scan, chest X-ray, skeletal survey, ultrasonography of the liver and liver scan (if needed), CAT-scan and physical examination.
While a LH-RH agonist or a LH-RH antagonist may be used in one preferred aspect of the present invention, the use of a LH-RH agonist is more preferred.
In another aspect, the invention provides a method of treating sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in a warm-blooded male animal in need of such treatment which comprises blocking the testicular hormonal secretions of said animal by surgical or chemical means and administering to said animal a therapeutically effective amount of an antiandrogen, or a pharmaceutical composition thereof. In another aspect, the invention provides a method of treating sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in a castrated warm-blooded mal0 animal, i.e., such a male animal whose teste~s are blockod by surg;cal or chemical means from secreting andro~en, which comprises administering to an animal in neod o such treatment therapeutically effective amounts of an antiandrogen in assocciation with at least one inhibitor of sex steroid biosynthesis, or a pharmaceutical composition thereof, in an amount sufficient to treat the cancer. In another aspect, the invention provides a method of testing sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in a castrated warm-blooded male animal, which comprises administering to an animal in need of such treatment therapeutically effective amounts of an antiandrogen and an antiestrogen, optionally in association with at 3',~787~La least one inhibitor of sex steroid biosynthesis. By simultaneously blocking sex-steroids (androgens and estrogens of testicular and adrenal origin) production and/or action, the present invention provides a method of inhibiting the growth of sex steroid-sensitive ~breast) tumors in warm-blooded male animals having such tumors.
In male mammals, the removal of testicular androgens may be achieved by surgical castration but preferably the secretion of androgens from the testes is blocked by chemical castration by administering to the warm-blooded male animal, an effective amount of an LH-RH agonist or antagonist. Thus, in a preferred aspect, the present invention provides a method of treating sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in a warm-blooded male animal, which comprises administering to an animal in need of such treatment an LH-RH agonist or antagonist in association with an antiandroyen and/or an antiestrogen and/or at least one inhibitor of sex steroid biosynthesis as discussed in the preceding paragraph, preferably in association with an antiAndrogen, or a pharmaceutical composition thereof, in amounts sufficient to treat the cancer.
In its preferred aspect, the LH-RH agonist or antagonist is administered parenterally (sub-cutaneously or intramuscularly) and the antiandrogen, the antiestrogen and the inhibitor(s) of sex steroid biosynthesis (if used) are administered orally.
In one preferred aspect, the present invention provides an effective method of treating sex steroid dependent cancers ~excluding prostate cancer) such as, for example, breast cancer in warm-blooded male animals in need of such treatment by administering ~7874a a LH-RH agonist or antagonist in association with an antiandro~en or pharmaceutical compositions thereof in amounts sufficient to inhibit tumor growth. The use of an LH-RH agonist in association with an antiandrogen produced almost complete blockage of testicular steroid secretion while simultaneously blocking about 25 to 60%
of the precursor sex steroids ~androgens and estrogens) of adrenal origin. See Figure 3 and Example 1. In still another preferred aspect, at least one inhibitor of sex steroid biosynthesis is administered to warm-blooded male animals having sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in association with surgical castration or chemical castration (by use of an LH-RH
agonist or antagonist) and the antiandrogen. These active compounds can be administered together or in any order as discussed hereinafter.
To assist in determining the effect of the treatment, blood plaYma concentrations of the testical and adrenal androgens and estrogens and tumor size are measured. Lowered concentrations of sex steroids and precurso~s and reduction in tumor size are indicative of successful treatment, e.g. lnhibition Oe tumor growth. The concentratlons of adrenal androgens and estrogens such as dehydroepLandrosterone ( DHEA), DHEA-sulfate ( DHEAS ), androst-5-ene-3~,17~-diol ~5-diol) and, the estrogen, 17~-estradiol ~E2) are measured by standard methods well known to those skilled in the art, see for example F. Labrie et al., The Prostate, 4, 579-594 (1983).
The active compounds described herein and used in accordance with the present invention exhibited tumor growth inhibition and lowered concentrations of sex steroids when tested in warm-blooded male animals ~,~7a~8 including man. See Figure 1-2 and 3 and the descriptions thereof in Example l.
The change in tumor size is measured by standard physical methods well known to those skilled in the art, e.g., bone scan, chest X-ray, skeletal survey, ultrasonography of the liver and liver scan (if needed), CAT-scan and physical examination.
While a LH-RH agonist or a LH-RH antagonist may be used in one preferred aspect of the present invention, the use of a LH-RH agonist is more preferred.
In another aspect, the invention provides a method of treating sex steroid dependent cancers such as, for example, pLOState cancer in a warm-blooded male animal including humans in need of such treatment which comprises blocking the testicular hormonal secretions of said animal by surgical or chemical means and administering to said animal a therapeutically effective amount of an antiandrogen in association with at least one inhibitor of sex steroid biosynthesis, or pharmaceutical compositions thereof. By simultaneously blockin(~ androgens o testicular and adLenal origin production and/or actlon, the present inventlon provides a method of inhibiting the growth of sex steroid-sensitive carcinomas in warm-blooded male animals having such carcinomas.
In male mammals, the removal of testicular androgens may be achieved by surgical castration torchiectomy) but preferably the secretion of androgens from the testes is blocked by chemical castration by administering to warm-blooded male animal, an effective amount of an LH-RH agonist or antagonist. In a preferred aspect, the present invention provides a method of treating sex steroid dependent cancers such 1~78~48 as, for example, prostate cancer in a warm-blooded male animal having such cancer, which comprises administering to said animal therapeutically effective amounts of an LH-RH agonist or antagonist in association with ar antiandroyen and at least one inhibitor of sex steroid biosynthesis, or pharmaceutical compositions thereof.
In its preferred aspect, the LH-RH agonist is administered parenterally (subcutaneously or intra-muscularly) and the antiandrogen and the inhibitor(s) or inhibitors of sex steroid biosynthesis are each administered orally.
In one preferred aspect, the present invention provides an effective method of treating sex steroid dependent cancers such as, for example, prostate cancer in warm-blooded male animals in need of such treatment by administering a LH-RH agonist or antagonist in association with an antiandrogen and an inhibitor of sex steroid biosynthesis of testicular origin or pharmaceutical compositlon~ thereo in amounts suf~ici0nt to inhibit such cancer. ~y use of an inhibito~ of te~ticular s0x steroid biosynthesis in association with an antiandro~J~n and a Ltl-RH ayonist or antagonist more complete androgen blockage is effected at an early stage in the treatment o such (particularly prostate) cancer than achieved by prior art methods. If an inhibitor of sex steroid biosynthesis of both testicular and adrenal origin (such as, for example, aminogluethimide) is used, the administration of the inhibitor is started on the first day o treatment and continued thereafter to block adrenal steroid synthesis.
In another preferred aspect, the use of an LH-RH agonist or antagonist in association with an 7~74l3 antiandrogen and two inhibitors of sex steroid biosynthesis, e.g an inhibitor of adrenal sex steroid biosynthesis such as aminoglutethimide and an inhibitor of testicular sex steroid biosynthesis such as ketoconazole, produced almost complete blockage of testicular steroid secretion while simultaneously blocking the precursor sex steroids ~androgens and estrogens) of adrenal origin at an early stage of the treatment. While such complete blockage of androgen secretion and/or action has not been achieved by prior art methods, such complete blockage can be achieved and maintained throughout the period of treatment in accordance with the present invention. These active compounds can be administered together or in any order as discussed hereinafter.
To assist in determining the effect of the treatment, blood plasma concentrations of the adrenal and testical androgens and estrogens and parameters of cancer evolution are measured according to known methods. Lowe~ed concentrations of sex steroids and reduction in pro.state or metastatic tumor size are indicative Oe successEul treatment, e,g. inhibition of prostatic cancer eell growth. The concentrations of adrenal steroids such as dehydroepiandrosterone ~DHEA), DHEA-sulfate ~DHEAS), androst-5-ene-3~,17~-diol (~5-diol) and, the estroyen, 17~-estradiol ~E2) are measured by standard methods well known to those skilled in the art, see for example F. Labrie et al., The Prostate, 4, 579-594 (1983).
P~ostatic size is measured by rectal examination and by transrectal ultrasonography.
Objective assessment of the effect of the treatment is also measured by standard physical methods well known to those skilled in the art, e.g., bone scanning, X-l~7s7~a ray, skeletal survey, intravenous pyelography, CAT-scan and physical examination. The response criteria for prostate cancer developed by the U.S.A. National Prostate Cancer Project (The Prostate, 1, 375-382) may also be used.
The use of therapeutically effective amounts of the inhibitor of testicular sex steroid biosynthesis such as ketoconazole or aminoglutethimide in associa-tion with the antiandrogen and the LH-RH agonist or LH-RH antagonist in accordance with the present invention effectively surpresses the serum sex steroid levels, especially serum testosterone and dihydrotestosterone concentrations stimulated by treatment with LH-RH
ayonist at the start of the treatment even in the presence of an antiandrogen.
While a LH-RH agonist or a LH-RH antagonist may be used in one preferred aspect of the present invention, the use of a LH-RH agonist is more preferred.
The components used in the above described aspects oE the inventlon are descrlbe~ in more detail:
Hy the term "LH-RH agonist" is meant synthetic analogues of the natural luteinizing hormone-releasin(~ hormone ~LH-RH), a decapeptide of the structure:
L-pyroylutamyl-L-histidyl-L-tryptophyl-L-seryl-L-tyrosyl-ylycyl-L-leucyl-L-arginyl-L-prolylglycyl-Typical suitable LH-RH agonists include nonapeptides and decapeptides represented by the formula:
L-pyroglutamyl-L-histidyl-L-tryptophyl-L-seryl-L-tyrosyl-X-Y-L-arginyl-L-prolyl-Z
1~7B7~3 wherein X is D-tryptophyl, D-leucyl, D-alanyl, iminobenzyl-D-histidyl, 3-(2-naphthyl)-D-alanyl, O-tert-butyl-D-seryl, D-tyrosyl, D-lysyl, D-phenylalanyl or N-methyl-D-alanyl and Y is L-leucyl, D-leucyl, N-methyl D-leucyl, Na-methyl-L-leucyl or D-alanyl and wherein Z is glycyl-NHRl or NHRl wherein Rl is H, lower alkyl or lower haloalkyl. Lower alkyl includes straight or branched chain alkyls having 1 to 6 carbon atoms, e.g., methyl, ethyl, propyl, pentyl or hexyls, iso-butyl, neopentyl and the like. Lower haloalkyl includes straight and branched chain alkyls of 1 to 6 carbon atoms having a halogen substituent, e.g., -CF3,-CH2CF3, -CF2CH3. Halogen means F, Cl, B~, with F being preferred.
Preferred nonapeptides wherein Y is L-leucyl and X is an optically active D-form of selected amino acids and ~ is NHC2H5 are [D-Trp6, des-gly-NH210]-LH-RH
ethylamide (X = D-Trp6); [D-Ser-~t-BuO~6, des-gly-NH210]- LH-RH ethylamide [X = D-Ser(t-BuO6)]; [D-Leu6, des-gly-NI-I210]-LH-REI ethylamide (X = D-Leu6), [D-His(i~z1)6, des-gly-NH210¦LH-RH ethylamide (X =
iminobenzyl-l)-liis6) and [i)-AIa6, des-gly-NH210]-LEI-RH
ethylamide ~X - D-Ala6).
PLeferred decapeptides include [D-Trp6]-LM-RH
wherein X = D-Trp, Y = L-leucyl, Z = glycyl-NH2, [D-Phe6]-LH-RH wherein X = D-phenylalanyl, Y = L-leucyl and Z = glycyl-HN2) or [D-Nal(2)6]LH-RH which is [(3-~2-naphthyl)-D-Ala6]LH-RH wherein X = 3-~2-naphthyl)-D-alanyl, Y = L-leucyl and Z = glycyl-NH2.
Other LH-RH agonists useful within the scope of this invention are the a-aza analogues of the natural LH-RH, especially, [D-Phe6,Azglyl0]-LH-RH, [D-Tyr~Me)6, Azglyl0]-LH-RH, and [D-Ser-~t-BuO)6, 1 ~787~
Azgly10]-LH-RH disclosed by A.S. Dutta et al. in J.
Med. Chem., 21, 1018 (1978) and US Patent 4,100,274 as well as those disclosed in U.S. Patent Nos. 4,024,248 and 4,118,483.
Typical suitable LH-RH antagonists include [N-Ac-D-p-Cl-Phel'2, D-Phe3, D-Arg6, D-Ala10]-LH-RH
disclosed by J. Ercheggi et al., Biochem. ~iophys.
Res. Commun. 100, 915-920, ~1981); [N-Ac-D-p-Cl-Phel'2, D-Trp3, D-Arg6, D-Ala10] LH-RH disclosed by D.H. Coy et al., Endocrinology, 110: 1445-1447, (1982); [N-Ac-D-~3-(2-naphthyl)-Ala)l, D-p-Cl-Phe2, D-Trp3, D-hArg(Et2)6,D-Ala10]-LH-RH and [N-Ac-Prol, D-p-F-Phe2, D-~3-~2-naphthyl)Ala3'6]-LH-RH disclosed by J.J. Nestor et al. J. Steroid Biochem., 20 (No. 6B), 1366 (1984);
the nona - and decapeptides analogs of LH-RH useful as LH-RH antagonists disclosed in U.S. Patent 4,481,190 (J.J. Nestor et al.); analogs of the highly constrained cyclic antagonist, cycle [~3 Prol, D-p-Cl-Phe2, D-Trp3'6, N-Me-Leu7, R-Ala10]-LH-RH disclosed by J.
Rivier, J. Steroid Biochem., 20, ~No. 6B), 1365 ~1984), and [N-Ac-D- ~ 3-~2-naphthyl)-Alal, D-p-F-Phe2, D-Trp3~
D-Arg6J-Lil-Rii disclosed by A. Corhin et al., J. Steroid Biochem. 2() ~No. 6B) 1369 ~1984).
Other LH-RH agonist and antagonist analogs are disclosed in LH-~H and Its Analogs, B.H. Vickory et al. editoL~s at pages 3-10 ~J.J. Nestor), 11-22 ~J.
Rivier et al.) and 23-33 ~J.J. Nestor et al.) The LH-RH agonists and antagonists useful in this invention may conveniently be prepared by the method described by Stewart et al. in "Solid Phase Peptide Synthesis" ~published in 1969 by Freeman ~ Co., San Francisco, page 1) but solution phase synthesis may also be used.
The nona- and decapeptides used in this ~787~3 invention are conveniently assembled on a solid resin support, such as 1% cross-linked Pro-Merrifield resin by use of an automatic peptide synthesizer. Typically, side-chain protecting groups, well known to those in the peptide arts, are used during the dicyclohexylcarbodiimide-cataylzed coupling of a tert-butyloxycarbonylamino acid to the growing peptide attached to a benzhydrylamine resin. The tert-butyloxycarbonyl protecting groups are removed at each stage with trifluoroacetic acid. The nona- or decapeptide is cleaved from the resin and deprotected by use of HF. The crude peptide is purified by the usual techniques, e.g., gel filtration, HPLC and partition chromatography and optionally lyophilization. See also D. H. Coy et al., J. Med.
Chem. _, pages 423-425, (197fi).
Typical suitable antiandrogens include non-steroidal antiandrogens such as the imidazolidines, especially 1-~3'-trifluoromethyl-4'-nitrophenyl)-4,4-dimethyl-imida2O1ine-2,5-dion~ ~also called Anandron) described in U.S. Patent No. 4,097,578, or 4'-nitro-3'-trifluoromethylisobutyranilide ~also called flutamide) described in U.S. Patent 4,329,364 as well as the N-(phenylalkanoyl)aniline derLvatives disclosed in U.S.
Patent 4,386,080 and the 3,4-disubstituted - branched-chain acylanilides disclosed in U.S. Patent 4,239,776 (A.T. Glen et al). Flutamide is the preferred antiandrogen.
Typical suitable steroidal antiandrogens include 6-chloro-1,2-dihydro-17-~acetyloxy)-3'H-cyclopropa[l,2]pregna-1,4,6-triene-3,20-dione, available under the trademark of Androcur from Schering A.G., ~. ~erlin and 17-acetyloxy-6-methylpregna-4,6-diene-3,20-diene, also called meg~strGl aceta~ and ~ S'i ~ 7s7~a available from Mead Johnson & Co., Evansille, Ind.
under the trademark of Megace.
Typical suitable antiestrogens include those steroidal and non-steroidal antiestrogens such as (lRS,2RS)-4,4'-diacetoxy-5,5'-difluoro-(1-ethyl-2-methylene)di-m-phenylenediacetate, which is available from Biorex under the tradename of Acefluranol, 6a-chloro-16a-methylpregn-4-ene-3,20-dione which is available from Eli Lilly & Co., Indianapolis, Ind.
under the tradename of Clometherone, 6-chloro-17-hydroxypregna-1,4,6-triene-3,20-dione which is available as the acetate salt from Syntex Labs, Palo Alto, Cal. as Delmadione Acetate, 17-hydroxy-6-methyl-l9-norpregna-4,6-diene-3,20-dione which is available from Theramex under the name of Lutenyl, 1-[2-[4-[1-(4-methoxyphenyl)-2-nitro-2-phenylethenyl]phenoxy]ethyl]-pyrrolidine which is available as the citrate salt from Parke-Davis Div. of Warner-Lambert Co., Morris Plains, N.J. under the name Oe Nitromifene Citrate, substituted aminoalkoxyphenylalkenes such as (Z)-2-[4-(1,2-diphenyl-l-butenyl)phenoxy]-N,N-dimethylethanamine which is available as the citrate salt from Stuart Pharmaceuticals, Wilmington, Del. as Tamoxifen Citrate (see also Belgian Patent 637,389, March 1964), 3,4-dihydro-2-(p-methoxyphenyl)-1-naphthyl p-[2-(1-pyrrolidinyl)ethoxy]phenyl ketone which is available as the methane sulfonate salt from Eli Lilly & Co. under the tradename of Trioxifene Mesylate, 1-[4'-(2-dimethylaminoethoxy)-phenyl)-l-(3'-hydroxyphenyl)-2-phenyl-but-l-ene, which is available from Klinge Pharma, 6-hydroxy-2-(p-hydroxyphenyl)-benzo(b)thien-3-yl[2-(1-pyrrolidinyl)-ethoxyphenyl]ketone which is available from Eli Lilly & Co. (LY-117~18), [6-hydroxy-2-(4-hydroxyphenyl)benæo(h!thien-3-yl]-~4-(2-(1-l~7~ 4a piperdinyl)-ethoxy)phenyl]methanone, which is available from Eli Lilly & Co. as the hydrogen chloride salt (LY-156758) and meso-3,4-bis(3'-hydroxyphenyl)hexane as well as the dimethyl, dipropyl and 3'-acetoxyphenyl analogues which are described in U.S. Patent 4,094,994 and a series of l-phenyl-alkane and -alkenes, e.g. (E)-3-cyclopentyl-1-(4-hydroxyphenyl)-1-phenyl-1-butene and 2-cyclopentyl-1-[4-hydroxy-or methoxyphenyl]-3-phenyl-2-propen-1-ol and FC-1157 which is available as the citrate salt from Farmos Group, Ltd., Turku, Finland (see also Eur. Pat. Appln. EP 7~,158). It is preferred to use an antiestrogen which shows minimal partial estrogen agonism. FC-1157, LY-117018,` LY-156578 and Tamoxifen are the preferred antiestrogens.
The inhibitors of sex steroid biosynthesis found useful in the present invention include those compounds which inhibit biosynthesis of sex steroids and precursor sex steroids of adrenal origin, and/or ovarian (or testicular respectively) preferably of ovarian (or testicular respectively) and adrenal origin.
Typical suitable inhibitors of sex steroid biosynthesis include 3-~4-aminophenyl)-3-ethyl-2,6-piperidinedione which is commonly called aminoglute-thimide, which is an inhibitor of sex steroid biosynthesis of adrenal but also ovarian and testicular origin and which is available from Ciba Pharmaceutical Co., Summit N.J. under trademark Cytadren, or ketoconazole an effective testicular but also adrenal sex steroid biosynthesis inhibitor which is available from Janssen Pharmaceutica, Piscataway, N.J. under the trademark Nizoral.
When an inhibitor of adrenal sex steroid bio-synthesis, e.g., aminoglutethimide is adm1nisteredf 87~3 cortisol biosynthesis is blocked. Accordingly, hydro-cortisone is administered in physiological amounts sufficient to maintain normal glucocorticoid levels.
In this invention, the LH-RH agonist or antagonist and antiandrogen and, where applicable, the inhibitor of steroid biosynthesis, hydrocortisone and antiestrogen are administered as pharmaceutical compositions via topical, parenteral or oral means.
The LH-RH agonist or antagonist is administered parenterally, i.e., intramuscularly, subcutaneously or intravenously by injection or infusion by nasal drops or by suppository, where applicable intra-vaginally.
The LH-RH agonist or antagonist also may be microencapsulated in or attached to a biocompatable, biodegradable polymer, e.g., poly~d,l-lactide-co-glycolide) and subcutaneously or intramuscularly injected by a techni~ue called subcutaneous or intramuscular depot to provide continuous, slow release of the LH-RH agonist or antagonist over a period of 30 days or longer. The most preferred route of administration of the LH-RH agonist or antagonist is subcutaneous depot injection. Preferably the antiandrogen will be administered orally. Preferably, the inhibitors of sex steroid biosynthesis such as aminoglutethimide and ketoconazole, and anti-estrogen when used, are administered orally.
The amount of each component administered is determined by the attending clinicians taking into consideration the etiology and severity of the disease, the patient's condition and age, the potency of each component and other factors. In the combination therapy of sex steroid dependent cancers, such as prostate cancer, breast cancer, testicular cancer, ovarian cancer, colon-rectal cancer, renal cancer, pancreatic cancer, liver cancer, stomach cancer, skin cancer, uterine cancer, brain cancer and larynx cancer especially prostate and breast cancer, according to this invention, the following dosage ranges are suitable.
The LH-RH agonist or antagonist is generally administered at from about 10 to 5000 ~g per day, with contemplated dosage ranges of about 10 to 1500 ~g per day and about 250 ~preferably 200 ~g in the therapy of female breast cancer using the combination with sex hormone biosynthesis inhibitor) to 500 ~g per day for the LH-RH agonist and to about 50 to 5000 ug per day for the LH-RH antagonist being preferred.
In the most preferred embodiment of this invention, the LH-RH agonist or antagonist is administered subcutaneously in a daily dose of 500 ug for the first 30 days and thereafter subcutaneously in a daily dose of 250 ~g regardless of the patients' body weight. When the LH-RH agonist or antagonist is administered, once every 30-day period or even longer, by intram~lscular or subcutaneous d0pot injection, a dose from about 300 to lSO,OnO ~g per 30-day period is ust-~d, with a tiose of 750 to 15,000 ~Ig per 30-day period being prefe L red.
The antiandrogen compositions are generally administe~etl in a dosage range of about 0.20 to 40 mg/kg (body weight) per day with 750 mg per day in three equally divided doses being preferred.
The aminoglutethimide compositions (when used) are administered initially in a dosage of 250 mg given at 8-hour intervals and the dosage may be increased in increments of 250 mg daily up to a total daily dose of 2 grams.
~ 787~8 The ketoconazole compositions ~when used) are administered orally in a dose of 250 mg given at 8-hour intervals and may be increased to a daily dose of 2 grams.
Other inhibitors of sex steroid biosynthesis are preferably administered in dosages being equivalent to the dosages given for aminoglutethimide and ketoconazole.
The antiestrogen compositions (when used) are administered in a dosage range of about 0.1 to 10 mg/ky body weight per day, with 10 mg, especially 20 mg, in two equally divided doses being preferred.
The glucocorticoide, especially hydrocortisone compositions (when used) are administered orally in a dosage range of about 0.1 to 20 mg/kg body weight per day. Preferably, the hydrocortisone is administered orally at the dose of about 10 mg in the morning and about 5 mg doses in the afternoon and in the evening.
The LH-RH agonist or antagonist and anti-androgen and inhibitor of sex steroid bisoynthesis and antiestrogen ~when used) each may be administered separately or when the modes of administration are the same, all or at lea~t two of them may be administered in the same composition, but in any case the preferred ratio of LH-I~H agonist to antiandrogen to antiestrogen ~when used) to inhibitor of sex steroid biosynthesis ~when used) administered daily will be about 250 ~9 of LH-RH agonist to about 750 mg of antiandrogen to about 15 mg, especially 20 mg, of anti-estrogen to about 750 mg of inhibitor of sex steroid biosynthesis.
In the therapy of sex steroid dependent cancers such as, for example, female breast cancer combining the administration of an LH-RH agonist or ~'~7a7~L8 antagonist, an antiandrogen and an antiestrogen the dosages preferable are as follows: The LH-RH agonist or antagonist is generally administered at rom about 10 to 2000 ~g per day, with contemplated dosage ranges of 10 to 500 ~g per day, 50-250 ~g per day and 250 to 500 ~g per day being preferred. In the most preferred embodiment of this aspect of the invention, the LH-RH
agonist or antagonist is administered subcutaneously in a daily dose of 500 ~g for the first 30 days and thereafter subcutaneously in a daily dose of 250 ~g regardless of the patients' body weight. When the LH-RH ayonist or antagonist is administered, once every 30-day period, by intramuscular or subcutaneous depot injection, a dose from about 300 to 60000 (occasionally 15000) ~g per 30-day period is used, with a dose of 750 to 6000 ~g per 30-day period being preferred. The antiandrogen compositions are generally administered in a dosage range of about 0.20 to 20 preferably 40 mg/kg ~body weight) per day with 375 especially 750 mg per day in th~ee equally divlded doses being preferred.
The antlestroyen compositions are administered in a dosage range of about 0.1 to 10 mg/kg body weight per day, with 15 mg in three, prefeLably with 20 mg in two, equally divided doses being preferred. The aminoglutethimide compositions when used are administe~ed initially in a dosage of 250 mg given at 6-hour, preferably 8-hour, intervals and the dosage may be increased in increments of 250 mg daily up to a total daily dose of 2 grams. The ketoconazole compositions when used are administered orally in a dose of 200 mg once per day and may be increased to 800 mg once peL day.
The LH-RH agonist or antagonist and antiandrogen and antiestrogen each may be administered 1.~787~8 separately or when the modes of administration are the same, all or two of them may be administered in the same composition, but in any case the preferred ratio of LH-RH agonist to antiandrogen to antiestrogen administered daily will be about 250 ~g of LH-RH
agonist to about 375 especially 750 mg of antiandrogen to about 15, preferably 20, mg of antiestrogen.
In the therapy of sex steroid dependent cancers, especially such as prostate and breast cancer, according to this invention, it is preferred that the LH-RH agonist is [D-Trp6,des-Gly NH210] LH-RH ethylamide which is administered subcutaneously in single daily dose of 500 ~9 for the first thirty ~30) days of treatment and thereafter in a single daily dose of 250 ~g; the antiandrogen is 4'-nitro-3'-trifluoromethyl-isobutyranilide, i.e. flutamide, which is administered orally in three equally divided daily doses of 2S0 mg each; and the lnhibltor of sex steroid biosynthesis is ketoconaxole and/or aminoglutethimide, each of which is administered orally in three equally divided doses of 250 mg ~very ~ hours; and the hydrocortison~ ~i ~Ised) is administered orally at a dose of about 10 mg in the morning and two equally divided doses of about 5 mg, ~ and 16 hours thereafter;
and the antiestrogen, when used, is ~Z)-2-[p-~1,2-diphenyl-l-hutenyl)phenoxy]-N,N-dimethyl ethylamine ~Tamoxifen) which is administered orally in two equally divided doses of about 10 mg every 12 hours. In the therapy of, for example, female breast cancer using the combination of the LH-RH agonist, the antiandrogen and antiestrogen discussed here, it is also useful to administer the antiandrogen ~flutamide) orally in three equally divided doses of 125, preferably 250 mg.
~'~7S7~
In the combination therapy of sex steroid dependent cancers according to this invention the administration of the antiandrogen, antiestrogen, inhibitor(s) of steroid biosynthesis, hydrocortisone and LH-RH agonist or LH-RH antagonist can be started in any order of sequence. Preferably the administration of the antiandrogen and/or the antiestrogen is started before (preferably one day before) the administration of the LH-RH agonist or LH-RH antagonist is started.
Preferably the administration of the inhibitor(s) of sex steroid biosynthesis is started on the same day as the administration of the LH-RH agonist or LH-RH
antagonist. However, the attending clinician may elect to start administration of the LH-RH agonist or antagonist on the first day of treatment.
When patients whose testes or ovaries respectively have already been surgically removed are treated according to this invention, the administration and dosage o~ the antlandrogen and the other components of the therapy (except the LH-RH agonist or antagonist) are the same as indicated for the therapy in which the LH-RH agonis~ or antagonist is used.
Normally, an lnhibitoL of testicular sex steroid biosynthesis such as ketoconazole may be administered to chemically but not surgically castrated patients.
Generally, the inhibitor of testicular sex steroid biosynthesis (when used), e.g., ketoconazole will be administered until the serum levels of T and DHT stimulated by the administration of the LH-RH
agonist are effectively suppressed, normally for one to three weeks. The inhibitor of adrenal sex steroid biosynthesis, e.g., aminoglutethimide may be administered at the start of treatment in the presence ~7a~748 or absence of the inhibitor of testicular sex steroid biosynthesis and thereafter continued throughout the period of treatment.
The LH-RH agonists or antagonists useful in the present invention are typically amorphous solids which are freely soluble in water or dilute acids, e.g., HCl, H2S04, citric, acetic, mandelic or fumaric. The LH-RH agonist or antagonist for subcutaneous injection is supplied in vials containing 5 mL of sterile solution with the LH-RH agonist or antagonist at a concentration of about 1.0 mg/mL.
A typical pharmaceutical composition of the LH-RH agonist or antagonist include the LH-RH agonist or antagonist or a pharmaceutically acceptable acid salt thereof, benzyl alcohol, a phosphate buffer (pH=6.9-7.2) and sterile water.
The LH-RH agonist or antagonist for intra-muscular or subcutaneous depot injection may be microencapsulated in a biocompatible, biodegradable polymer, e.g., poly ~d,l-lactide-co-glycolide~ by a phase separation process or foLmed into a pellet. The microspheLes may then be suspended in a carrier to provide an injectable preparation or the depot may be injected in the form of a pellet. See also European Patent Application EPA 58,481 published August 25, 1982 for solid compositions for subdermal injection or implantation or liquid formulations for intramuscular or subcutaneous injections; containing biocompatible, biodegradeable polymers such as lactide-glycolide copolymer and an LH-RH agonist, e.g., D-Ser-t-BuO6, Azglyln-LH-RH .
The inhibitors of sex steroid biosynthesis, e.g., aminoglutethimide and ketoconazole and the glucocorticoide, e.g., hydrocortisone (when used) are ~78~48 typically compounded in custornary ways for oral administration, e.g., in tablets, capsules and the like.
The antiandrogens useful in the present invention are typically formuLated with conventional pharmaceutical excipients, e.g., spray dried lactose and magnesium stearate into tablets or capsules for oral administration. The antiestrogens, when used with the invention, are typically compounded in customary ways for oral administration, e.g., in capsules, tablets, as dragees or even in liquid form, e.g., suspensions or syrups. One or more of the active substances, with or without additional types of active agents, can be worked into tablets or dragee cores by being mixed with solid, pulverulent carrier substances, such as sodium citrate, calcium carbonate or dicalcium phosphate, and binders such as polyvinyl pyrrolidone, gelatin or cellulose derivatives, possibly by adding also lubricants such as magnesium stearate, sodium lauryl sulEate, "Carbowax" or polyethylene glycols. Of course, taste-improvlng ~ubstances can be added in the case of oral-administration forms.
The therapeutically active antiestrogen compound should be present in a concentration of about 0.5-90~ by welght of the total mixture, i.e., in amounts that are sufficient for maintaining the above-mentioned dosage range.
As further forms of administration, one can use plug capsules, e.g., of hard gelatin, as well as closed soEt-gelatin capsules comprising a softener or plasticizer, e.g., glycerine. The plug capsules contain the active substance preferably in the form of granulate, e.g., in mixture with fillers, such as lactose, saccharose, mannitol, starches, such as potato 87~8 starch or amylopectin, cellulose derivatives or highly-dispersed silicic acids. In soft-gelatin capsules, the active substance is preferably dissolved or suspended in suitable liquids, such as vegetable oils or liquid polyethylene glycols.
In place of oral administration, the active compounds may be administered parenterally. In such case, one can use a solution of the active substance, e.g., in sesame oil or olive oil.
Following the above treatment using the described regimen, tumor growth and bone metastases of sex steroid dependent cancers is inhibited and in some instances complete remission occurs.
The invention also provides kits or single packages combining the pharmaceutical compositions useful for the combination treatment of sex-steroid dependent cancers discussed above. The kits or packages may also contain instructions to use the pharmaceutical compositions in accordance with the present invention. This aspect of the invention is exemplified by the following discussions: For the treatment of female breast cancer a two component kit provides the antiandrogen oral pharmaceutical composition and the LH-RH agonist or LM-RM antagonist parenteral compo~ition or the antiandrogen oral pharmaceutical composition and the antiestrogen oral composition or the oral compositions of the antiandroyen or antiestroyen and the inhibitor of sex steroid biosynthesis; a three component kit provides the LH-RH agonist or antagonist parenteral pharmaceutical composition, or the oral compositions of the antiandrogen, the antiestrogen and the inhibitor of sex steroid biosynthesis; the antiandrogen and the antiestrogen oral pharmaceutical composition, a four '11'~7~37~3 component kit provides the LH-RH agonist or LH-RH
antagonist parenteral pharmaceutical composition, the antiandrogen oral pharmaceutical composition, the sex steroid biosynthesis inhibitor oral pharmaceutical composition and the hydrocortisone oral pharmaceutical composition; and a five component kit provides the LH-RH agonist or LH-RH antagonist parenteral pharmaceutical composition, the antiandrogen oral pharmaceutical composition, the antiestrogen oral pharmaceutical composition, the sex steroid biosynthesis inhibitor oral composition and the hydrocortisone oral pharmaceutical composition.
Further kits are provided in accordance with the combination therapy of this invention.
For the treatment of prostate cancer, a three component kit provides the antiandrogen oral pharmaceutical composition, the LH-RH agonist or LH-RH
antagonist parenteral composition and the sex steroid biosynthesis inhibitor oral pharmaceutical composition;
a four component kit provides the LH-RH agonist or LH-RH antagonist parenteral pharmaceutical composition, the antlandro~en oral pharmaceutical composition, the adrenal sex steroid blosynthesLs inhihitor oral pharmaceutical composition and the hydrocortisone oral pharmaceutical composition; and a five component kit provides the LH-RH agonist or LH-RH antagonist parenteral pharmaceutical composition, the antiandrogen oral pharmaceutical composition and the testicular sex steroid biosynthesis inhibitor oral pharmaceutical composition, the adrenal sex steroid biosynthesis inhibitor oral pharmaceutical composition and the hydrocortisone oral pharmaceutical composition.
Further kits are provided in accordance with the combination therapy of this invention.
7~7'~8 For the treatment of other sex steroid dependent cancers analogous kits are provided according to this invention. The kits may also contain pharmaceutical compositions which contain more than one component of the combination treatment.
The following examples illustrate the invention.
~7~7~8 Figures l to 3 show the result of the combination therapy of a male patient having breast cancer according to the invention.
Figure l is a bone scintigraph showing multiple bone metastases in a male patient having breast cancer prior to treatment in accordance with an aspect of the present invention.
Figure 2 is a bone scintigraph of the same male patient after treatment for six and a half months in accordance with an aspect of the present invention.
Figure 3 graphically displays serum levels of testicular and adrenal steroids in the male patient treated in accordance with an aspect of the present invention.
Twelve months after modified radical mastectomy with axillary dissection ~4 out of 13 positive nodes) in a 66-year old man, bone scintigraphy ~Fig. l) ~howed multiple bone metastatic lesions in the third and fo~lrth cervical vertebrae, in the first, third and twelth thoracic vertebrae, in the third, fourth and fifth lumbar vertebrae, in both sacro-iliac areas, in both shoulders and in the anterior part of the second L ight rib. Chest X-Ray and abdominal echogram did not show evidence of additional extension of the disease. The pituitary ~LH, FSH and prolactin) as well as steroid [pregnenolone, 17-OH pregnenolone, dehydroepiandrosterone ~DHEA), DHEA-sulfate, androst-5-ene-38,17R-diol~5-diol), progesterone, 17-OH-progesterone, androstenedione~4-dione), testosterone (T), dihydrotestosterone (DHT), androstane-3~,17R-diol, androstane-3B,17R-diol, androsterone and cortisol]
hormones were within normal limits. Hormone 7~8 measurements and calculations were performed according to known methods. The serum concentration of carcinoembryonic antigen (CEA) as well as a series of laboratory analyses, including complete blood count, sequential multiple analyzer (SMA-12) and urinalysis were normal.
Combined antihormonal treatment with the LH-RH agonist [D-Ser-(tBuO)6, des-gly-NH210~LH-RH
ethylamide (500 ~9 daily, s.c.) in combination with the pure antiandrogen Flutamide (250 mg orally every 8h) was started. Six and a half months later bone scintigraphy showed a complete disappearance of increased uptake in all the areas identified 6 1/2 months earlier with no appearance of new lesion (Fig.
2). X-Ray, ultrasonography and clinical examination revealed no sign of any lesion. As illustrated in Fig.
3, the combined treatment caused 95~ reduction (compared to control) in serum testosterone (T) and a 25 to 60~. fall in the serum levels of adrenal steroids, namely DHEA, DHEAS, Q4-dione and Q5-diol while not affecting cortisol signlEicantly. S0rum levels of DHT
anA E2 were also d0creased by ~0 to 4n~. During hormonal therapy, no cllnical sign of the disease could be detected. The only side-effects were related to hypoandrogenicity. Thus, after four months of treatment, the patient developed mild climateric-like vasomotor phenomena consisting of perspiration and hot flushes, which did not require treatment. He also complained of loss of libido and sexual potency after two months of treatment.
The present data show a rapid and complete regression of bone metastases in a patient having wide-spread bone metastases from breast-cancer. A complete response could be seen within 6 1/2 months after ~.~'78748 starting the combined treatment with an LH-RH agonist and a pure antiandrogen.
INHIBITORY EFFECT OF AMIN~GLUTETHIMIDE OR
KETOCONAZOLE ON LHRH AGONIST-IND~CED SERUM
TESTOSTERONE IN THE DOG
Figures 4 to 6 show the result of the test.
Fig. 4. Serum levels of testosterone during the first 19 days of treatment of dogs with daily administration of 50 ~g of [D-Trp6]LHRH ethylamide.
Fig. 5. Serum levels of testosterone during the first 19 days o treatment of dogs with daily administration to 50 ~9 of [D-Trp6]LHRH ethylamide in association with ketoconazole.
Fig. 6. Serum levels of testosterone during the first 19 dàys of treatment of dogs with daily administration of 50 ~9 of [D-Trp6]LHRH ethylamide in association with amlnoglutethimide.
~ hile LH~H flgonists achieve castration levels of androgens during chronlc treatment in men, the first 5 to 10 days of administration of the peptide are associated with increased serum levels o testosterone and dihydrotestosterone ~Labrie et al., J. Androl. 1:
209-228, 1980). These increased levels of testicular androgens are accompanied by an exacerbation of the symptoms and signs of prostate cancer in significant proportion of cases ~Kahan et al., The Lancet i, 971-972, 1984).
The following experiment shows that the LHRH
agonist-induced rise in serum testosterone can be prevented by simultaneous administration of the steroid 78q4~
biosynthesis inhibitors aminoglutethimide or ketaconazole.
Eighteen mongrel dogs weighing between 20-30 kg were randomly divided into three groups. The animals were housed one per cage and fed Purina Dog Chow and tap water ad libitum.
The animals of group 1 were injected daily ~at 0700h) with 50 ~g of the LHRH agonist [D-Trp6, des-Gly-NH210]LHRH ethylamide (LHRH-A). In group 2, the animals were also injected daily with 50 ~g of LHRH-A
and took in addition 200 mg of ketoconazole per os at 0700h, 1500h and 2300h. The animals of group 3 received daily 50 ~g of LHRH-A and 125 mg of aminoglutethimide per os at 0700h, 1500h, 2300h plus 10 mg of hydrocortisone twice daily.
Blood samples were collected at 0700h, O900h, llOOh and 1500h one day before treatment and every day during the treatment. Plasma was extracted with diethyl ether and testosterone was separated on LH-20 columns before RIA mea~urements.
Fig. 4 shows that on one to six days following the start of treatment with the dailty injection of 50 ~g of the LHRH agonist ~D-Trp6]LHRH
ethylamide, there is an increase in serum testosterone up to approximately 500% above control. Thereafter, there is a decrease of the level of this androgen which reaches near-castration levels on day 19. It can be seen in Fig. 5 and 6 that the simultaneous administration of the steroid inhibitors ketoconazole or aminoglutethimide almost completely prevented this rise in serum testosterone which occur during the first days of treatment with a peptide.
These data clearly indicate the usefulness of the combined administration of inhibitors of steroid blosynthesis in order to pr~vent the rise of testicular serum androgens during the first days of treatment with LHRH agonist~.
Since dogs do not have adre~al p~odu~tlon of androgens the influence of the admlnistration o~ an antiand~ogen in combination with the ad~lnistratlon of the LH-RH a~onist and the inhLbitor~ of ~3ex steroid biosynthesis cannot be demonstrated in thi~ species.
Howeve~, it can be concl~ded from the te~t results that in men the admini6tration of an antiandrogen (especially flutamide) in combin~tion with the LH-RH
agonist or antagonist And the inhibitors of sex steroid biosynthesls which lnhibit the s~cretion of precursor adrenal androgens substantially or comp1etely decr~ases the content of andro~ens in the sy~tem and t`nus cont~-ibutes to the inhibition of and~ogen 5ensitive cancer ~rowth.
The ilnportant aspect~ of ~his lnvention can be summarized ~ follows:
The invcn~ion provid~s:
l~ A method of treating sex st~roid dependent cancers in a warm-bloodcd animal which comprises admlnistering a phar~aceutically efective amount oi an ant~androgen and/or an antiestrogen and~or at lea~t one ~nhibitor of sex ~teroid biosynthesi~ to the animal whose hormone output o~ the testes or ovaries, is blocked, with the proviso that ~he method of treating prostate cancer ccmprises administering pharmace~tically e~fective a~ounts o~ an anti~ndrogen and at least one inhibitor of sex steroid biosynthesis and the method of treating breast cancer comprises a~ministering a pharmaceu-tically effective a~ount (l) of an an~landrogen o~ (2) of at least one inhibitor of sex steroid biosynthesls ~ ~7~8 or (3) of an antiandrogen and an antiestrogen or (4) o~
an antiandrogen and at least one inhibitor of sex steroid biosynthesls or t5~ of an antiestrogen and at least one inhibitor of sex steroid biosynthesis or (6) of an antiandrogen and an antiestrogen and at least one inhibitor of sex steroid biosynthesis.
~) A kit c~mprislng a combination of pharmaceutical composition~ for combination therapy of sex steriod dependent cancers in a warm-blooded animal whose hormone output of the testes or ovaries, is blocked, the combination consisting Oe pharmaceuti~al compositions co~p~ising (1) an antiandro~ein and ~n antiestrogen or (2) an antiand~ogen and at least one inhibitor of sex ste~old blosynthesi~ or (3) an antie.st~ogen and at least one inhi~itor of sex ~teroid biosynthesis ot (4) an antiandror~en ~nd an anties~rogen and at l~ast on~ inhibitor Of ~ex ~teroid b.iosynthesis.
3~ A kit comprising a pharmaccutic~l composition comprising fln ar~ti~ndro~en an~/or ~ ~harmaceutical composition comprising ~n ~nties~rogerl and/or one or mOre phar~ac~utical composi~ion(s) comprisiny an inhi~itor of sex steroid ~iosynthesis co~ether with instructions for `using the composition(s) or each of these compositions for the tr~atment o~ sex steroid dependent cancer.s in a warm-blooded animal by a combination therapy involvlng administering a pharmaceutically e~fective a~ount of an antiandrogen and/or an antiestrogen and/ot at least o.ne inhibitor of sex steroid biosynthesis to the animal whose hormone output of the testes or ovarie.s, is blocked, w~th the proviso that the instructions for treating prostate cancer recommend administerlng pharmaceutically effective a~ounts of an antiandrogen and at least one ~nhibltor of sex steroid biosynthesis and the instructions for treating beeast: cancer recommend administering a pharma~eutically effective amount (1) of an anttandror~en or (2) of at least one inhibitor of sex ster~id bio~ynthesiS or (3) of an antiandro~en and an antiestro~en or (4) of an antiandrogen and at least one inhibitor of sex steroid biosynthesis or (5) of an antiestrogen and at least one inhibitor of sex steroid biosynthesis or (6) of an antiandrogen and an antiesttogen and at least one inhibitor of sex steroi~
biosyntl-esis.
OF HORMONE DEPENDENT CANCERS
This invention relates to a combination therapy of sex steroid dependent cancers in susceptible warm-blooded animals including humans comprising administering to such animals whose hormone output of their testes or ovaries respectively is blocked a pharmaceutically effective amount of an antiandrogen and/or an antiestrogen and/or at least one inhibitor of sex steroid biosynthesis to the animal whose hormone output of the testes or ovarles, respectively, is blocked, wlth the provlso that the method of treating prostate cancer comprises admlnistering pharmaceutically effective amounts of an antiandrogen and at least one inhibitor of sex steroid biosynthesis and the method of treating breast cancer comprises administering a pharmaceutically effective amount of an antiandrogen or of at least one inhibitor of sex steroid biosynthesis or of an antiandrogen and an antiestrogen or of an antiandrogen and at least one inhibitor of sex steroid biosynthesis or of an antiestrogen and at least one inhibitor of sex steroid biosynthesis or of an intiandrogen and an antiestrogen and at least one inhibitor of sex steroid biosynthesis. In the therapy of sex steroid dependent l~7s7~a cancers such as testicular cancer, ovarian cancer, colon-rectal cancer, renal cancer, pancreatic cancer, liver cancer, stomach cancer, skin cancer, uterine cancer, brain cancer and larynx cancer all above listed combinations are applicable. The hormone output of the animal's testes or ovaries, respectively, can be blocked by surgical or chemical means. (In post-menopausal women~ the attending clinicians may decide that the hormone output of the ovaries need not be blocked.) While various investigators have been studying hormone~dependent breast and prostate cancer, none have proposed the combination therapy of this invention.
A. V. Schally et al., Cancer Treatment Reports, 68, (No. 1) 281-289 tl984), summarize the results of animal and clinical studies on growth inhibition of hormone-dependent mammary and prostate tumors by use of analogues of luteinizing hormone-releasiny hormones, the so-called LH-RH agonists and suggest that LH-RH analogs and/or antagonists may have potential for treating breast cancer.
T. W. Redding and A. V. Schally, Pro. Natl~
Acad. Sci. USA, R0, 14S9-1462 ~1983), disclose reduction of estrogen-dependent mammary tumors in rats and mice by use of an LH-RH agonist, [D-Trp6]LH-RH or of two specific antagonists and inhibition of prostate tumor growth in rats of chronic use of an LH-RH
agonist, [D-Trp6] LH-RH.
In U.S. Patent 4,071,622, it is disclosed that use of certain LH-RH agonists causes regression of DMBA-induced mammary carcinoma in rats.
In U.S. Patent 4,472,382, it is disclosed that prostate adenocarcinoma, benign prostate 1'~787~L8 hypertrophy and hormone-dependent mammary tumors may be treated with various LH-RH agonists and that prostate adenocarcinoma and benign hypertrophy may be treated by use of various LH-RH agonists and an antiandrogen.
However, there is no suggestion or disclosure of the present invention.
Some clinical improvement in premenopausal women with breast cancer by use of the two LH-RH
agonists, Buserelin and Leuprolide, is also reported by H.A. Harvey et al. "LH-RH analogs in the treatment of human breast cancer", LH-RH and its Analogs - A New Class of Contraceptive and Therapeutic Aqents (B.H.
Vickery and J.J. Nestor, Jr., and E.S.E. Hafez, eds) Lancester, MTP Press, ~1984) and by J.G.M. Klijn et al.
"Treatment with luteinizing hormone releasing hormone analogue (Buserelin) in premenopausal patients with metastatic breast cancer", Lancet, 1, 1213-1216 (1982).
Treatment of advanced breast cancer with aminoglutethimide after therapy with the antiestrogen, Tamoxifen is clisclosed by A.V. Buzdar et al., Cancer, 50, 170~-1712 (1982).
Il. Flax et al., Lancet, l204-1207, (1973), suggest some women's br~st cancers are androgen-dependent.
In U.S. Patent 4,329,364, it is disclosed that the antiandrogen, 4'-nitro-3'-trifourormethyl isobutyranilide may be used for treatment of prostatic cancer.
Some clinical improvement in men with prostate cancer by use of the two LH-RH agonists, Buserelin and Leuprolide, is also reported by N. Faure et al. at pages 337-350 and by R.J. Santen et al. at pages 351-364, respectively, LH-RH and its Analogs - A
New Class of Contraceptive and Therapeutic Aqents (B.H.
l~7a7~s Vickery and J.J. Nestor, Jr., and E.S.E. Hafez, eds) Lancester, MTP Press, (1984).
R. Santen et al., The Journal of Steroid Biochemistry, Volume 20, No 6B, at page 1375 (1984), disclose that use of ketoconazole in combination with chronic administration of Leuprolide in rodents decreased basal and Leuprolide stimulated testosterone levels.
D. Kerle et al., The IJournal of Steroid Biochemistry, Volume 20, No 6B, at page 1395 (1984) disclose that the combined use of a LH-RH analogue and ketoconazole produced objective responses in some prostate cancer patients who have relapsed or failed to respond to treatment with a LH-RH analogue alone.
F. Labrie et al., Abstracts of 7th International Congress of Endrocrinology, Excerpta ~1edica (1984) at page 98 discloses that treatment of prostate cancer patients with LH-RH agonists alone causes a transient increase in serum androgen levels lasting for 5 to 15 days before castration levels are reached. While F. Labrie et al. recommends that orchiectomy, estrogen and LH-RH agonists alone should not be further used for treatment of prostate cancer in the absen~e of a pure antiandrogen, there still is a need fo~ a method of treatment of prostate canceL that effects mOLe complete androgen blockage at the start as well as during the full period of treatment.
F. Labrie et al., The Prostate, 4, 579-594 ~1983), disclose that use of a combination therapy of an LH-RH agonist (Buserelin) and an antiandrogen (Anandron) to treat advanced prostate cancer in previously untreated patients effects simultaneous inhibition of androgens of both testicular and adrenal origin.
l~7a~s F. Labrie et al., J. Steroid Biochem., 19, 99-1007 (1983), disclose the treatment of prostate cancer by the combined administration of an LH-RH
agonist and an antiandrogen. Labrie et al. disclose animal and clinical data in support of the proposition that the combined LH-RH/antiandrogen treatment neutralizes the stimulatory influence of all androgens on the development and growth of androgen-dependent prostatic cancer.
In U.S. Patent 4~,094,994, it is disclosed that the use of antiestrogens such as meso-3,4-bis(3'-hydroxyphenyl)hexane inhibits MCF7 human breast tumor cells. In fact, the inhibitory activity of the anti-estrogen was antagonized by estradiol.
H. Mouridsen et al,. Cancer Treatment Review 5, 131-141, (1978), disclose that Tamoxifen, an antiestrogen is effective in remission of advanced breast cancer in about 30~ of the patients treated.
J.G.M. Klijn et al., ~J. Steroid Biochem, Vol. 20 l~o. 6B), 1381 ~198~), disclosed the combined use of the antiestrogen, Tamoxif0n, and the LH-RH
agonist, Buscrelin, for tr0atment of breast cancer is krlown, but obj0etiv~ remiss;on of such cancers remains low ~35'~).
The present invention provides a new combination therapy of sex steroid dependent cancers which inhibits tumor growth and metastases and causes in some instances complete remission. The invention is exemplified by detailed discussion of the therapy of breast cancer and prostate cancer. The therapy of other sex steroid dependent cancers (listed above) is carried out analogously.
In one aspect, the invention provides a method of treating sex steroid dependent cancers such l~7874a as, for example, breast cancer in a warm-blooded female animal in need of such treatment which comprises administering to said animal whose hormone output of the ovaries is blocked, a therapeutically effective amount of an antiandrogen or a pharmaceutical composition thereof. The ovarian hormonal secretions of said animal can be blocked by surgical or chemical means. In one aspect, the invention provides a method of treating sex steroid dependent cancers such as, for example, breast cancer in a castrated warm-blooded female animal, i.e., such a female animal whose ovaries are blocked by surgical or chemical means from secreting estrogen, which comprises administering to such a female in need of such treatment an antiandrogen in association with at least one inhibitor of sex steroid biosynthesis and, optionally, an antiestrogen, or pharmaceutical compositions thereof, in amounts sufficient to treat such cancers, e.g., breast cancer. In another aspect, the invention provides a method of treating sex steroid dependent cancers such as, for examplo, breast cancer in a warm-blooded animal in need of such treatment which comprises blocking the ovarian hormonal secretions of said animal hy surgical or chemical means and administering to said animal therapeutically effective amounts of an antiestrogen in association with at least one inhibitor of sex steroid biosynthesis, or pharmaceutical compositions thereof.
In one aspect, the invention provides a method of treating sex steroid dependent cancers such as, for example, breast cancer in a warm-blooded animal whose ovaries are blocked by surgical or chemical means from secreting estrogen, which comprises administering to an animal in need of such treatment an antiandrogen and an antiestrogen, or pharmaceutical compositions thereof, 1-~787~8 in amounts sufficient to treat such cancers, e.g., breast cancer.
By completely bloclcing sex steroids ~androgens and estrogens) production and/or action, the present invention provides a method of inhibiting the growth of sex steroid-sensitive tumors, e.g., breast tumors in warm-blooded animals having such tumors.
In female mammals, the ovaries may be surgic-ally removed ~oophorectomy) but preferably the secretion of estrogens from the ovaries is blocked by chemical castration by administering an effective amount of an LH-RH agonist or antagonist. Thus, in a preferred aspect, the present invention provides a method of treating sex steroid dependent cancers such as, for example, breast cancer in a warm-blooded female animal, which comprises administering to such a female in need of such treatment an LH-RH agonist or antagonist, in association with an antiandrogen and/or an antiestrogen and/or at least one inhihitor of sex steorid biosynthesis according to the invention, preferably an antiandrogen. Preferably in this treatment at least one inhibitor of sex steroid biosynthesis, or pharmaceutical compositions thereof, and/or antiestrogen is administered.
In its preferred aspect, the LH-RH agonist is administered parenterally ~subcutaneously or intra-muscularly or intranasal) and, in association there-with, the antiandrogen and the inhibitor of sex steroid biosynthesis and/or antiestrogen are each administered orally.
Thus, this invention provides a novel method for effective treatment of sex steroid dependent cancers such as, for example, female breast cancer, in the absence of antiestrogen. In addition, the amounts l~7s7~a of antiestrogen required when administered in association with this combined therapy are lower than normally used in prior art methods, e.g., J.G.M. Klijn et al., J. Steroid Biochem. 20 (No. 6B) 1381 ~1984), to treat breast cancer, and thus, the harmful effects of relatively large doses of antiestrogen are minimized.
In one preferred aspect, the present invention provides an effective method of treating sex steroid dependent cancers such as, for example, breast cancer in warm-blooded female animals in need of such treatment by administering an LH-RH agonist or antagonist, in association with an antiandrogen and an inhibitor of sex steroid biosynthesis or pharmaceutical compositions thereof in amounts sufficient to inhibit tumor growth. These active compounds can be administered together or in any order as discussed hereinafter.
To assist in determining the effect of the treatment, blood plasma concentrations of the sex steroids of adrenal and ovarian origin, i.e., precursor steroids, androgens and estrogens, and tumor size are measured. Lowered concentrations of sex steroids and reduction in tumor size are indicative of successful treatment, e.g. inhibition of tumor growth using active compounds described herein in accordance with the present invention. The concentrations of adrenal androgens and estrogens such as dehydroepiandrosterone (DHEA), DHEA-sulfate tDHEAS), androst-5-ene-3R,17B-diol (~5-diol) and, the ovarian estrogen, 17B-estradiol (E2) are measured by standard methods well known to those skilled in the art, see for example F. Labrie et al., The Prostate, _, 579-594 (1983).
The change in tumor size is measured by standard physical methods well known to those skilled l~7~74a in the art, e.g., bone scan, chest X-ray, skeletal survey, ultrasonography of the liver and liver scan (if needed), CAT-scan and physical examination.
While a LH-RH agonist or a LH-RH antagonist may be used in one preferred aspect of the present invention, the use of a LH-RH agonist is more preferred.
In another aspect, the invention provides a method of treating sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in a warm-blooded male animal in need of such treatment which comprises blocking the testicular hormonal secretions of said animal by surgical or chemical means and administering to said animal a therapeutically effective amount of an antiandrogen, or a pharmaceutical composition thereof. In another aspect, the invention provides a method of treating sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in a castrated warm-blooded mal0 animal, i.e., such a male animal whose teste~s are blockod by surg;cal or chemical means from secreting andro~en, which comprises administering to an animal in neod o such treatment therapeutically effective amounts of an antiandrogen in assocciation with at least one inhibitor of sex steroid biosynthesis, or a pharmaceutical composition thereof, in an amount sufficient to treat the cancer. In another aspect, the invention provides a method of testing sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in a castrated warm-blooded male animal, which comprises administering to an animal in need of such treatment therapeutically effective amounts of an antiandrogen and an antiestrogen, optionally in association with at 3',~787~La least one inhibitor of sex steroid biosynthesis. By simultaneously blocking sex-steroids (androgens and estrogens of testicular and adrenal origin) production and/or action, the present invention provides a method of inhibiting the growth of sex steroid-sensitive ~breast) tumors in warm-blooded male animals having such tumors.
In male mammals, the removal of testicular androgens may be achieved by surgical castration but preferably the secretion of androgens from the testes is blocked by chemical castration by administering to the warm-blooded male animal, an effective amount of an LH-RH agonist or antagonist. Thus, in a preferred aspect, the present invention provides a method of treating sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in a warm-blooded male animal, which comprises administering to an animal in need of such treatment an LH-RH agonist or antagonist in association with an antiandroyen and/or an antiestrogen and/or at least one inhibitor of sex steroid biosynthesis as discussed in the preceding paragraph, preferably in association with an antiAndrogen, or a pharmaceutical composition thereof, in amounts sufficient to treat the cancer.
In its preferred aspect, the LH-RH agonist or antagonist is administered parenterally (sub-cutaneously or intramuscularly) and the antiandrogen, the antiestrogen and the inhibitor(s) of sex steroid biosynthesis (if used) are administered orally.
In one preferred aspect, the present invention provides an effective method of treating sex steroid dependent cancers ~excluding prostate cancer) such as, for example, breast cancer in warm-blooded male animals in need of such treatment by administering ~7874a a LH-RH agonist or antagonist in association with an antiandro~en or pharmaceutical compositions thereof in amounts sufficient to inhibit tumor growth. The use of an LH-RH agonist in association with an antiandrogen produced almost complete blockage of testicular steroid secretion while simultaneously blocking about 25 to 60%
of the precursor sex steroids ~androgens and estrogens) of adrenal origin. See Figure 3 and Example 1. In still another preferred aspect, at least one inhibitor of sex steroid biosynthesis is administered to warm-blooded male animals having sex steroid dependent cancers (excluding prostate cancer) such as, for example, breast cancer in association with surgical castration or chemical castration (by use of an LH-RH
agonist or antagonist) and the antiandrogen. These active compounds can be administered together or in any order as discussed hereinafter.
To assist in determining the effect of the treatment, blood plaYma concentrations of the testical and adrenal androgens and estrogens and tumor size are measured. Lowered concentrations of sex steroids and precurso~s and reduction in tumor size are indicative of successful treatment, e.g. lnhibition Oe tumor growth. The concentratlons of adrenal androgens and estrogens such as dehydroepLandrosterone ( DHEA), DHEA-sulfate ( DHEAS ), androst-5-ene-3~,17~-diol ~5-diol) and, the estrogen, 17~-estradiol ~E2) are measured by standard methods well known to those skilled in the art, see for example F. Labrie et al., The Prostate, 4, 579-594 (1983).
The active compounds described herein and used in accordance with the present invention exhibited tumor growth inhibition and lowered concentrations of sex steroids when tested in warm-blooded male animals ~,~7a~8 including man. See Figure 1-2 and 3 and the descriptions thereof in Example l.
The change in tumor size is measured by standard physical methods well known to those skilled in the art, e.g., bone scan, chest X-ray, skeletal survey, ultrasonography of the liver and liver scan (if needed), CAT-scan and physical examination.
While a LH-RH agonist or a LH-RH antagonist may be used in one preferred aspect of the present invention, the use of a LH-RH agonist is more preferred.
In another aspect, the invention provides a method of treating sex steroid dependent cancers such as, for example, pLOState cancer in a warm-blooded male animal including humans in need of such treatment which comprises blocking the testicular hormonal secretions of said animal by surgical or chemical means and administering to said animal a therapeutically effective amount of an antiandrogen in association with at least one inhibitor of sex steroid biosynthesis, or pharmaceutical compositions thereof. By simultaneously blockin(~ androgens o testicular and adLenal origin production and/or actlon, the present inventlon provides a method of inhibiting the growth of sex steroid-sensitive carcinomas in warm-blooded male animals having such carcinomas.
In male mammals, the removal of testicular androgens may be achieved by surgical castration torchiectomy) but preferably the secretion of androgens from the testes is blocked by chemical castration by administering to warm-blooded male animal, an effective amount of an LH-RH agonist or antagonist. In a preferred aspect, the present invention provides a method of treating sex steroid dependent cancers such 1~78~48 as, for example, prostate cancer in a warm-blooded male animal having such cancer, which comprises administering to said animal therapeutically effective amounts of an LH-RH agonist or antagonist in association with ar antiandroyen and at least one inhibitor of sex steroid biosynthesis, or pharmaceutical compositions thereof.
In its preferred aspect, the LH-RH agonist is administered parenterally (subcutaneously or intra-muscularly) and the antiandrogen and the inhibitor(s) or inhibitors of sex steroid biosynthesis are each administered orally.
In one preferred aspect, the present invention provides an effective method of treating sex steroid dependent cancers such as, for example, prostate cancer in warm-blooded male animals in need of such treatment by administering a LH-RH agonist or antagonist in association with an antiandrogen and an inhibitor of sex steroid biosynthesis of testicular origin or pharmaceutical compositlon~ thereo in amounts suf~ici0nt to inhibit such cancer. ~y use of an inhibito~ of te~ticular s0x steroid biosynthesis in association with an antiandro~J~n and a Ltl-RH ayonist or antagonist more complete androgen blockage is effected at an early stage in the treatment o such (particularly prostate) cancer than achieved by prior art methods. If an inhibitor of sex steroid biosynthesis of both testicular and adrenal origin (such as, for example, aminogluethimide) is used, the administration of the inhibitor is started on the first day o treatment and continued thereafter to block adrenal steroid synthesis.
In another preferred aspect, the use of an LH-RH agonist or antagonist in association with an 7~74l3 antiandrogen and two inhibitors of sex steroid biosynthesis, e.g an inhibitor of adrenal sex steroid biosynthesis such as aminoglutethimide and an inhibitor of testicular sex steroid biosynthesis such as ketoconazole, produced almost complete blockage of testicular steroid secretion while simultaneously blocking the precursor sex steroids ~androgens and estrogens) of adrenal origin at an early stage of the treatment. While such complete blockage of androgen secretion and/or action has not been achieved by prior art methods, such complete blockage can be achieved and maintained throughout the period of treatment in accordance with the present invention. These active compounds can be administered together or in any order as discussed hereinafter.
To assist in determining the effect of the treatment, blood plasma concentrations of the adrenal and testical androgens and estrogens and parameters of cancer evolution are measured according to known methods. Lowe~ed concentrations of sex steroids and reduction in pro.state or metastatic tumor size are indicative Oe successEul treatment, e,g. inhibition of prostatic cancer eell growth. The concentrations of adrenal steroids such as dehydroepiandrosterone ~DHEA), DHEA-sulfate ~DHEAS), androst-5-ene-3~,17~-diol (~5-diol) and, the estroyen, 17~-estradiol ~E2) are measured by standard methods well known to those skilled in the art, see for example F. Labrie et al., The Prostate, 4, 579-594 (1983).
P~ostatic size is measured by rectal examination and by transrectal ultrasonography.
Objective assessment of the effect of the treatment is also measured by standard physical methods well known to those skilled in the art, e.g., bone scanning, X-l~7s7~a ray, skeletal survey, intravenous pyelography, CAT-scan and physical examination. The response criteria for prostate cancer developed by the U.S.A. National Prostate Cancer Project (The Prostate, 1, 375-382) may also be used.
The use of therapeutically effective amounts of the inhibitor of testicular sex steroid biosynthesis such as ketoconazole or aminoglutethimide in associa-tion with the antiandrogen and the LH-RH agonist or LH-RH antagonist in accordance with the present invention effectively surpresses the serum sex steroid levels, especially serum testosterone and dihydrotestosterone concentrations stimulated by treatment with LH-RH
ayonist at the start of the treatment even in the presence of an antiandrogen.
While a LH-RH agonist or a LH-RH antagonist may be used in one preferred aspect of the present invention, the use of a LH-RH agonist is more preferred.
The components used in the above described aspects oE the inventlon are descrlbe~ in more detail:
Hy the term "LH-RH agonist" is meant synthetic analogues of the natural luteinizing hormone-releasin(~ hormone ~LH-RH), a decapeptide of the structure:
L-pyroylutamyl-L-histidyl-L-tryptophyl-L-seryl-L-tyrosyl-ylycyl-L-leucyl-L-arginyl-L-prolylglycyl-Typical suitable LH-RH agonists include nonapeptides and decapeptides represented by the formula:
L-pyroglutamyl-L-histidyl-L-tryptophyl-L-seryl-L-tyrosyl-X-Y-L-arginyl-L-prolyl-Z
1~7B7~3 wherein X is D-tryptophyl, D-leucyl, D-alanyl, iminobenzyl-D-histidyl, 3-(2-naphthyl)-D-alanyl, O-tert-butyl-D-seryl, D-tyrosyl, D-lysyl, D-phenylalanyl or N-methyl-D-alanyl and Y is L-leucyl, D-leucyl, N-methyl D-leucyl, Na-methyl-L-leucyl or D-alanyl and wherein Z is glycyl-NHRl or NHRl wherein Rl is H, lower alkyl or lower haloalkyl. Lower alkyl includes straight or branched chain alkyls having 1 to 6 carbon atoms, e.g., methyl, ethyl, propyl, pentyl or hexyls, iso-butyl, neopentyl and the like. Lower haloalkyl includes straight and branched chain alkyls of 1 to 6 carbon atoms having a halogen substituent, e.g., -CF3,-CH2CF3, -CF2CH3. Halogen means F, Cl, B~, with F being preferred.
Preferred nonapeptides wherein Y is L-leucyl and X is an optically active D-form of selected amino acids and ~ is NHC2H5 are [D-Trp6, des-gly-NH210]-LH-RH
ethylamide (X = D-Trp6); [D-Ser-~t-BuO~6, des-gly-NH210]- LH-RH ethylamide [X = D-Ser(t-BuO6)]; [D-Leu6, des-gly-NI-I210]-LH-REI ethylamide (X = D-Leu6), [D-His(i~z1)6, des-gly-NH210¦LH-RH ethylamide (X =
iminobenzyl-l)-liis6) and [i)-AIa6, des-gly-NH210]-LEI-RH
ethylamide ~X - D-Ala6).
PLeferred decapeptides include [D-Trp6]-LM-RH
wherein X = D-Trp, Y = L-leucyl, Z = glycyl-NH2, [D-Phe6]-LH-RH wherein X = D-phenylalanyl, Y = L-leucyl and Z = glycyl-HN2) or [D-Nal(2)6]LH-RH which is [(3-~2-naphthyl)-D-Ala6]LH-RH wherein X = 3-~2-naphthyl)-D-alanyl, Y = L-leucyl and Z = glycyl-NH2.
Other LH-RH agonists useful within the scope of this invention are the a-aza analogues of the natural LH-RH, especially, [D-Phe6,Azglyl0]-LH-RH, [D-Tyr~Me)6, Azglyl0]-LH-RH, and [D-Ser-~t-BuO)6, 1 ~787~
Azgly10]-LH-RH disclosed by A.S. Dutta et al. in J.
Med. Chem., 21, 1018 (1978) and US Patent 4,100,274 as well as those disclosed in U.S. Patent Nos. 4,024,248 and 4,118,483.
Typical suitable LH-RH antagonists include [N-Ac-D-p-Cl-Phel'2, D-Phe3, D-Arg6, D-Ala10]-LH-RH
disclosed by J. Ercheggi et al., Biochem. ~iophys.
Res. Commun. 100, 915-920, ~1981); [N-Ac-D-p-Cl-Phel'2, D-Trp3, D-Arg6, D-Ala10] LH-RH disclosed by D.H. Coy et al., Endocrinology, 110: 1445-1447, (1982); [N-Ac-D-~3-(2-naphthyl)-Ala)l, D-p-Cl-Phe2, D-Trp3, D-hArg(Et2)6,D-Ala10]-LH-RH and [N-Ac-Prol, D-p-F-Phe2, D-~3-~2-naphthyl)Ala3'6]-LH-RH disclosed by J.J. Nestor et al. J. Steroid Biochem., 20 (No. 6B), 1366 (1984);
the nona - and decapeptides analogs of LH-RH useful as LH-RH antagonists disclosed in U.S. Patent 4,481,190 (J.J. Nestor et al.); analogs of the highly constrained cyclic antagonist, cycle [~3 Prol, D-p-Cl-Phe2, D-Trp3'6, N-Me-Leu7, R-Ala10]-LH-RH disclosed by J.
Rivier, J. Steroid Biochem., 20, ~No. 6B), 1365 ~1984), and [N-Ac-D- ~ 3-~2-naphthyl)-Alal, D-p-F-Phe2, D-Trp3~
D-Arg6J-Lil-Rii disclosed by A. Corhin et al., J. Steroid Biochem. 2() ~No. 6B) 1369 ~1984).
Other LH-RH agonist and antagonist analogs are disclosed in LH-~H and Its Analogs, B.H. Vickory et al. editoL~s at pages 3-10 ~J.J. Nestor), 11-22 ~J.
Rivier et al.) and 23-33 ~J.J. Nestor et al.) The LH-RH agonists and antagonists useful in this invention may conveniently be prepared by the method described by Stewart et al. in "Solid Phase Peptide Synthesis" ~published in 1969 by Freeman ~ Co., San Francisco, page 1) but solution phase synthesis may also be used.
The nona- and decapeptides used in this ~787~3 invention are conveniently assembled on a solid resin support, such as 1% cross-linked Pro-Merrifield resin by use of an automatic peptide synthesizer. Typically, side-chain protecting groups, well known to those in the peptide arts, are used during the dicyclohexylcarbodiimide-cataylzed coupling of a tert-butyloxycarbonylamino acid to the growing peptide attached to a benzhydrylamine resin. The tert-butyloxycarbonyl protecting groups are removed at each stage with trifluoroacetic acid. The nona- or decapeptide is cleaved from the resin and deprotected by use of HF. The crude peptide is purified by the usual techniques, e.g., gel filtration, HPLC and partition chromatography and optionally lyophilization. See also D. H. Coy et al., J. Med.
Chem. _, pages 423-425, (197fi).
Typical suitable antiandrogens include non-steroidal antiandrogens such as the imidazolidines, especially 1-~3'-trifluoromethyl-4'-nitrophenyl)-4,4-dimethyl-imida2O1ine-2,5-dion~ ~also called Anandron) described in U.S. Patent No. 4,097,578, or 4'-nitro-3'-trifluoromethylisobutyranilide ~also called flutamide) described in U.S. Patent 4,329,364 as well as the N-(phenylalkanoyl)aniline derLvatives disclosed in U.S.
Patent 4,386,080 and the 3,4-disubstituted - branched-chain acylanilides disclosed in U.S. Patent 4,239,776 (A.T. Glen et al). Flutamide is the preferred antiandrogen.
Typical suitable steroidal antiandrogens include 6-chloro-1,2-dihydro-17-~acetyloxy)-3'H-cyclopropa[l,2]pregna-1,4,6-triene-3,20-dione, available under the trademark of Androcur from Schering A.G., ~. ~erlin and 17-acetyloxy-6-methylpregna-4,6-diene-3,20-diene, also called meg~strGl aceta~ and ~ S'i ~ 7s7~a available from Mead Johnson & Co., Evansille, Ind.
under the trademark of Megace.
Typical suitable antiestrogens include those steroidal and non-steroidal antiestrogens such as (lRS,2RS)-4,4'-diacetoxy-5,5'-difluoro-(1-ethyl-2-methylene)di-m-phenylenediacetate, which is available from Biorex under the tradename of Acefluranol, 6a-chloro-16a-methylpregn-4-ene-3,20-dione which is available from Eli Lilly & Co., Indianapolis, Ind.
under the tradename of Clometherone, 6-chloro-17-hydroxypregna-1,4,6-triene-3,20-dione which is available as the acetate salt from Syntex Labs, Palo Alto, Cal. as Delmadione Acetate, 17-hydroxy-6-methyl-l9-norpregna-4,6-diene-3,20-dione which is available from Theramex under the name of Lutenyl, 1-[2-[4-[1-(4-methoxyphenyl)-2-nitro-2-phenylethenyl]phenoxy]ethyl]-pyrrolidine which is available as the citrate salt from Parke-Davis Div. of Warner-Lambert Co., Morris Plains, N.J. under the name Oe Nitromifene Citrate, substituted aminoalkoxyphenylalkenes such as (Z)-2-[4-(1,2-diphenyl-l-butenyl)phenoxy]-N,N-dimethylethanamine which is available as the citrate salt from Stuart Pharmaceuticals, Wilmington, Del. as Tamoxifen Citrate (see also Belgian Patent 637,389, March 1964), 3,4-dihydro-2-(p-methoxyphenyl)-1-naphthyl p-[2-(1-pyrrolidinyl)ethoxy]phenyl ketone which is available as the methane sulfonate salt from Eli Lilly & Co. under the tradename of Trioxifene Mesylate, 1-[4'-(2-dimethylaminoethoxy)-phenyl)-l-(3'-hydroxyphenyl)-2-phenyl-but-l-ene, which is available from Klinge Pharma, 6-hydroxy-2-(p-hydroxyphenyl)-benzo(b)thien-3-yl[2-(1-pyrrolidinyl)-ethoxyphenyl]ketone which is available from Eli Lilly & Co. (LY-117~18), [6-hydroxy-2-(4-hydroxyphenyl)benæo(h!thien-3-yl]-~4-(2-(1-l~7~ 4a piperdinyl)-ethoxy)phenyl]methanone, which is available from Eli Lilly & Co. as the hydrogen chloride salt (LY-156758) and meso-3,4-bis(3'-hydroxyphenyl)hexane as well as the dimethyl, dipropyl and 3'-acetoxyphenyl analogues which are described in U.S. Patent 4,094,994 and a series of l-phenyl-alkane and -alkenes, e.g. (E)-3-cyclopentyl-1-(4-hydroxyphenyl)-1-phenyl-1-butene and 2-cyclopentyl-1-[4-hydroxy-or methoxyphenyl]-3-phenyl-2-propen-1-ol and FC-1157 which is available as the citrate salt from Farmos Group, Ltd., Turku, Finland (see also Eur. Pat. Appln. EP 7~,158). It is preferred to use an antiestrogen which shows minimal partial estrogen agonism. FC-1157, LY-117018,` LY-156578 and Tamoxifen are the preferred antiestrogens.
The inhibitors of sex steroid biosynthesis found useful in the present invention include those compounds which inhibit biosynthesis of sex steroids and precursor sex steroids of adrenal origin, and/or ovarian (or testicular respectively) preferably of ovarian (or testicular respectively) and adrenal origin.
Typical suitable inhibitors of sex steroid biosynthesis include 3-~4-aminophenyl)-3-ethyl-2,6-piperidinedione which is commonly called aminoglute-thimide, which is an inhibitor of sex steroid biosynthesis of adrenal but also ovarian and testicular origin and which is available from Ciba Pharmaceutical Co., Summit N.J. under trademark Cytadren, or ketoconazole an effective testicular but also adrenal sex steroid biosynthesis inhibitor which is available from Janssen Pharmaceutica, Piscataway, N.J. under the trademark Nizoral.
When an inhibitor of adrenal sex steroid bio-synthesis, e.g., aminoglutethimide is adm1nisteredf 87~3 cortisol biosynthesis is blocked. Accordingly, hydro-cortisone is administered in physiological amounts sufficient to maintain normal glucocorticoid levels.
In this invention, the LH-RH agonist or antagonist and antiandrogen and, where applicable, the inhibitor of steroid biosynthesis, hydrocortisone and antiestrogen are administered as pharmaceutical compositions via topical, parenteral or oral means.
The LH-RH agonist or antagonist is administered parenterally, i.e., intramuscularly, subcutaneously or intravenously by injection or infusion by nasal drops or by suppository, where applicable intra-vaginally.
The LH-RH agonist or antagonist also may be microencapsulated in or attached to a biocompatable, biodegradable polymer, e.g., poly~d,l-lactide-co-glycolide) and subcutaneously or intramuscularly injected by a techni~ue called subcutaneous or intramuscular depot to provide continuous, slow release of the LH-RH agonist or antagonist over a period of 30 days or longer. The most preferred route of administration of the LH-RH agonist or antagonist is subcutaneous depot injection. Preferably the antiandrogen will be administered orally. Preferably, the inhibitors of sex steroid biosynthesis such as aminoglutethimide and ketoconazole, and anti-estrogen when used, are administered orally.
The amount of each component administered is determined by the attending clinicians taking into consideration the etiology and severity of the disease, the patient's condition and age, the potency of each component and other factors. In the combination therapy of sex steroid dependent cancers, such as prostate cancer, breast cancer, testicular cancer, ovarian cancer, colon-rectal cancer, renal cancer, pancreatic cancer, liver cancer, stomach cancer, skin cancer, uterine cancer, brain cancer and larynx cancer especially prostate and breast cancer, according to this invention, the following dosage ranges are suitable.
The LH-RH agonist or antagonist is generally administered at from about 10 to 5000 ~g per day, with contemplated dosage ranges of about 10 to 1500 ~g per day and about 250 ~preferably 200 ~g in the therapy of female breast cancer using the combination with sex hormone biosynthesis inhibitor) to 500 ~g per day for the LH-RH agonist and to about 50 to 5000 ug per day for the LH-RH antagonist being preferred.
In the most preferred embodiment of this invention, the LH-RH agonist or antagonist is administered subcutaneously in a daily dose of 500 ug for the first 30 days and thereafter subcutaneously in a daily dose of 250 ~g regardless of the patients' body weight. When the LH-RH agonist or antagonist is administered, once every 30-day period or even longer, by intram~lscular or subcutaneous d0pot injection, a dose from about 300 to lSO,OnO ~g per 30-day period is ust-~d, with a tiose of 750 to 15,000 ~Ig per 30-day period being prefe L red.
The antiandrogen compositions are generally administe~etl in a dosage range of about 0.20 to 40 mg/kg (body weight) per day with 750 mg per day in three equally divided doses being preferred.
The aminoglutethimide compositions (when used) are administered initially in a dosage of 250 mg given at 8-hour intervals and the dosage may be increased in increments of 250 mg daily up to a total daily dose of 2 grams.
~ 787~8 The ketoconazole compositions ~when used) are administered orally in a dose of 250 mg given at 8-hour intervals and may be increased to a daily dose of 2 grams.
Other inhibitors of sex steroid biosynthesis are preferably administered in dosages being equivalent to the dosages given for aminoglutethimide and ketoconazole.
The antiestrogen compositions (when used) are administered in a dosage range of about 0.1 to 10 mg/ky body weight per day, with 10 mg, especially 20 mg, in two equally divided doses being preferred.
The glucocorticoide, especially hydrocortisone compositions (when used) are administered orally in a dosage range of about 0.1 to 20 mg/kg body weight per day. Preferably, the hydrocortisone is administered orally at the dose of about 10 mg in the morning and about 5 mg doses in the afternoon and in the evening.
The LH-RH agonist or antagonist and anti-androgen and inhibitor of sex steroid bisoynthesis and antiestrogen ~when used) each may be administered separately or when the modes of administration are the same, all or at lea~t two of them may be administered in the same composition, but in any case the preferred ratio of LH-I~H agonist to antiandrogen to antiestrogen ~when used) to inhibitor of sex steroid biosynthesis ~when used) administered daily will be about 250 ~9 of LH-RH agonist to about 750 mg of antiandrogen to about 15 mg, especially 20 mg, of anti-estrogen to about 750 mg of inhibitor of sex steroid biosynthesis.
In the therapy of sex steroid dependent cancers such as, for example, female breast cancer combining the administration of an LH-RH agonist or ~'~7a7~L8 antagonist, an antiandrogen and an antiestrogen the dosages preferable are as follows: The LH-RH agonist or antagonist is generally administered at rom about 10 to 2000 ~g per day, with contemplated dosage ranges of 10 to 500 ~g per day, 50-250 ~g per day and 250 to 500 ~g per day being preferred. In the most preferred embodiment of this aspect of the invention, the LH-RH
agonist or antagonist is administered subcutaneously in a daily dose of 500 ~g for the first 30 days and thereafter subcutaneously in a daily dose of 250 ~g regardless of the patients' body weight. When the LH-RH ayonist or antagonist is administered, once every 30-day period, by intramuscular or subcutaneous depot injection, a dose from about 300 to 60000 (occasionally 15000) ~g per 30-day period is used, with a dose of 750 to 6000 ~g per 30-day period being preferred. The antiandrogen compositions are generally administered in a dosage range of about 0.20 to 20 preferably 40 mg/kg ~body weight) per day with 375 especially 750 mg per day in th~ee equally divlded doses being preferred.
The antlestroyen compositions are administered in a dosage range of about 0.1 to 10 mg/kg body weight per day, with 15 mg in three, prefeLably with 20 mg in two, equally divided doses being preferred. The aminoglutethimide compositions when used are administe~ed initially in a dosage of 250 mg given at 6-hour, preferably 8-hour, intervals and the dosage may be increased in increments of 250 mg daily up to a total daily dose of 2 grams. The ketoconazole compositions when used are administered orally in a dose of 200 mg once per day and may be increased to 800 mg once peL day.
The LH-RH agonist or antagonist and antiandrogen and antiestrogen each may be administered 1.~787~8 separately or when the modes of administration are the same, all or two of them may be administered in the same composition, but in any case the preferred ratio of LH-RH agonist to antiandrogen to antiestrogen administered daily will be about 250 ~g of LH-RH
agonist to about 375 especially 750 mg of antiandrogen to about 15, preferably 20, mg of antiestrogen.
In the therapy of sex steroid dependent cancers, especially such as prostate and breast cancer, according to this invention, it is preferred that the LH-RH agonist is [D-Trp6,des-Gly NH210] LH-RH ethylamide which is administered subcutaneously in single daily dose of 500 ~9 for the first thirty ~30) days of treatment and thereafter in a single daily dose of 250 ~g; the antiandrogen is 4'-nitro-3'-trifluoromethyl-isobutyranilide, i.e. flutamide, which is administered orally in three equally divided daily doses of 2S0 mg each; and the lnhibltor of sex steroid biosynthesis is ketoconaxole and/or aminoglutethimide, each of which is administered orally in three equally divided doses of 250 mg ~very ~ hours; and the hydrocortison~ ~i ~Ised) is administered orally at a dose of about 10 mg in the morning and two equally divided doses of about 5 mg, ~ and 16 hours thereafter;
and the antiestrogen, when used, is ~Z)-2-[p-~1,2-diphenyl-l-hutenyl)phenoxy]-N,N-dimethyl ethylamine ~Tamoxifen) which is administered orally in two equally divided doses of about 10 mg every 12 hours. In the therapy of, for example, female breast cancer using the combination of the LH-RH agonist, the antiandrogen and antiestrogen discussed here, it is also useful to administer the antiandrogen ~flutamide) orally in three equally divided doses of 125, preferably 250 mg.
~'~7S7~
In the combination therapy of sex steroid dependent cancers according to this invention the administration of the antiandrogen, antiestrogen, inhibitor(s) of steroid biosynthesis, hydrocortisone and LH-RH agonist or LH-RH antagonist can be started in any order of sequence. Preferably the administration of the antiandrogen and/or the antiestrogen is started before (preferably one day before) the administration of the LH-RH agonist or LH-RH antagonist is started.
Preferably the administration of the inhibitor(s) of sex steroid biosynthesis is started on the same day as the administration of the LH-RH agonist or LH-RH
antagonist. However, the attending clinician may elect to start administration of the LH-RH agonist or antagonist on the first day of treatment.
When patients whose testes or ovaries respectively have already been surgically removed are treated according to this invention, the administration and dosage o~ the antlandrogen and the other components of the therapy (except the LH-RH agonist or antagonist) are the same as indicated for the therapy in which the LH-RH agonis~ or antagonist is used.
Normally, an lnhibitoL of testicular sex steroid biosynthesis such as ketoconazole may be administered to chemically but not surgically castrated patients.
Generally, the inhibitor of testicular sex steroid biosynthesis (when used), e.g., ketoconazole will be administered until the serum levels of T and DHT stimulated by the administration of the LH-RH
agonist are effectively suppressed, normally for one to three weeks. The inhibitor of adrenal sex steroid biosynthesis, e.g., aminoglutethimide may be administered at the start of treatment in the presence ~7a~748 or absence of the inhibitor of testicular sex steroid biosynthesis and thereafter continued throughout the period of treatment.
The LH-RH agonists or antagonists useful in the present invention are typically amorphous solids which are freely soluble in water or dilute acids, e.g., HCl, H2S04, citric, acetic, mandelic or fumaric. The LH-RH agonist or antagonist for subcutaneous injection is supplied in vials containing 5 mL of sterile solution with the LH-RH agonist or antagonist at a concentration of about 1.0 mg/mL.
A typical pharmaceutical composition of the LH-RH agonist or antagonist include the LH-RH agonist or antagonist or a pharmaceutically acceptable acid salt thereof, benzyl alcohol, a phosphate buffer (pH=6.9-7.2) and sterile water.
The LH-RH agonist or antagonist for intra-muscular or subcutaneous depot injection may be microencapsulated in a biocompatible, biodegradable polymer, e.g., poly ~d,l-lactide-co-glycolide~ by a phase separation process or foLmed into a pellet. The microspheLes may then be suspended in a carrier to provide an injectable preparation or the depot may be injected in the form of a pellet. See also European Patent Application EPA 58,481 published August 25, 1982 for solid compositions for subdermal injection or implantation or liquid formulations for intramuscular or subcutaneous injections; containing biocompatible, biodegradeable polymers such as lactide-glycolide copolymer and an LH-RH agonist, e.g., D-Ser-t-BuO6, Azglyln-LH-RH .
The inhibitors of sex steroid biosynthesis, e.g., aminoglutethimide and ketoconazole and the glucocorticoide, e.g., hydrocortisone (when used) are ~78~48 typically compounded in custornary ways for oral administration, e.g., in tablets, capsules and the like.
The antiandrogens useful in the present invention are typically formuLated with conventional pharmaceutical excipients, e.g., spray dried lactose and magnesium stearate into tablets or capsules for oral administration. The antiestrogens, when used with the invention, are typically compounded in customary ways for oral administration, e.g., in capsules, tablets, as dragees or even in liquid form, e.g., suspensions or syrups. One or more of the active substances, with or without additional types of active agents, can be worked into tablets or dragee cores by being mixed with solid, pulverulent carrier substances, such as sodium citrate, calcium carbonate or dicalcium phosphate, and binders such as polyvinyl pyrrolidone, gelatin or cellulose derivatives, possibly by adding also lubricants such as magnesium stearate, sodium lauryl sulEate, "Carbowax" or polyethylene glycols. Of course, taste-improvlng ~ubstances can be added in the case of oral-administration forms.
The therapeutically active antiestrogen compound should be present in a concentration of about 0.5-90~ by welght of the total mixture, i.e., in amounts that are sufficient for maintaining the above-mentioned dosage range.
As further forms of administration, one can use plug capsules, e.g., of hard gelatin, as well as closed soEt-gelatin capsules comprising a softener or plasticizer, e.g., glycerine. The plug capsules contain the active substance preferably in the form of granulate, e.g., in mixture with fillers, such as lactose, saccharose, mannitol, starches, such as potato 87~8 starch or amylopectin, cellulose derivatives or highly-dispersed silicic acids. In soft-gelatin capsules, the active substance is preferably dissolved or suspended in suitable liquids, such as vegetable oils or liquid polyethylene glycols.
In place of oral administration, the active compounds may be administered parenterally. In such case, one can use a solution of the active substance, e.g., in sesame oil or olive oil.
Following the above treatment using the described regimen, tumor growth and bone metastases of sex steroid dependent cancers is inhibited and in some instances complete remission occurs.
The invention also provides kits or single packages combining the pharmaceutical compositions useful for the combination treatment of sex-steroid dependent cancers discussed above. The kits or packages may also contain instructions to use the pharmaceutical compositions in accordance with the present invention. This aspect of the invention is exemplified by the following discussions: For the treatment of female breast cancer a two component kit provides the antiandrogen oral pharmaceutical composition and the LH-RH agonist or LM-RM antagonist parenteral compo~ition or the antiandrogen oral pharmaceutical composition and the antiestrogen oral composition or the oral compositions of the antiandroyen or antiestroyen and the inhibitor of sex steroid biosynthesis; a three component kit provides the LH-RH agonist or antagonist parenteral pharmaceutical composition, or the oral compositions of the antiandrogen, the antiestrogen and the inhibitor of sex steroid biosynthesis; the antiandrogen and the antiestrogen oral pharmaceutical composition, a four '11'~7~37~3 component kit provides the LH-RH agonist or LH-RH
antagonist parenteral pharmaceutical composition, the antiandrogen oral pharmaceutical composition, the sex steroid biosynthesis inhibitor oral pharmaceutical composition and the hydrocortisone oral pharmaceutical composition; and a five component kit provides the LH-RH agonist or LH-RH antagonist parenteral pharmaceutical composition, the antiandrogen oral pharmaceutical composition, the antiestrogen oral pharmaceutical composition, the sex steroid biosynthesis inhibitor oral composition and the hydrocortisone oral pharmaceutical composition.
Further kits are provided in accordance with the combination therapy of this invention.
For the treatment of prostate cancer, a three component kit provides the antiandrogen oral pharmaceutical composition, the LH-RH agonist or LH-RH
antagonist parenteral composition and the sex steroid biosynthesis inhibitor oral pharmaceutical composition;
a four component kit provides the LH-RH agonist or LH-RH antagonist parenteral pharmaceutical composition, the antlandro~en oral pharmaceutical composition, the adrenal sex steroid blosynthesLs inhihitor oral pharmaceutical composition and the hydrocortisone oral pharmaceutical composition; and a five component kit provides the LH-RH agonist or LH-RH antagonist parenteral pharmaceutical composition, the antiandrogen oral pharmaceutical composition and the testicular sex steroid biosynthesis inhibitor oral pharmaceutical composition, the adrenal sex steroid biosynthesis inhibitor oral pharmaceutical composition and the hydrocortisone oral pharmaceutical composition.
Further kits are provided in accordance with the combination therapy of this invention.
7~7'~8 For the treatment of other sex steroid dependent cancers analogous kits are provided according to this invention. The kits may also contain pharmaceutical compositions which contain more than one component of the combination treatment.
The following examples illustrate the invention.
~7~7~8 Figures l to 3 show the result of the combination therapy of a male patient having breast cancer according to the invention.
Figure l is a bone scintigraph showing multiple bone metastases in a male patient having breast cancer prior to treatment in accordance with an aspect of the present invention.
Figure 2 is a bone scintigraph of the same male patient after treatment for six and a half months in accordance with an aspect of the present invention.
Figure 3 graphically displays serum levels of testicular and adrenal steroids in the male patient treated in accordance with an aspect of the present invention.
Twelve months after modified radical mastectomy with axillary dissection ~4 out of 13 positive nodes) in a 66-year old man, bone scintigraphy ~Fig. l) ~howed multiple bone metastatic lesions in the third and fo~lrth cervical vertebrae, in the first, third and twelth thoracic vertebrae, in the third, fourth and fifth lumbar vertebrae, in both sacro-iliac areas, in both shoulders and in the anterior part of the second L ight rib. Chest X-Ray and abdominal echogram did not show evidence of additional extension of the disease. The pituitary ~LH, FSH and prolactin) as well as steroid [pregnenolone, 17-OH pregnenolone, dehydroepiandrosterone ~DHEA), DHEA-sulfate, androst-5-ene-38,17R-diol~5-diol), progesterone, 17-OH-progesterone, androstenedione~4-dione), testosterone (T), dihydrotestosterone (DHT), androstane-3~,17R-diol, androstane-3B,17R-diol, androsterone and cortisol]
hormones were within normal limits. Hormone 7~8 measurements and calculations were performed according to known methods. The serum concentration of carcinoembryonic antigen (CEA) as well as a series of laboratory analyses, including complete blood count, sequential multiple analyzer (SMA-12) and urinalysis were normal.
Combined antihormonal treatment with the LH-RH agonist [D-Ser-(tBuO)6, des-gly-NH210~LH-RH
ethylamide (500 ~9 daily, s.c.) in combination with the pure antiandrogen Flutamide (250 mg orally every 8h) was started. Six and a half months later bone scintigraphy showed a complete disappearance of increased uptake in all the areas identified 6 1/2 months earlier with no appearance of new lesion (Fig.
2). X-Ray, ultrasonography and clinical examination revealed no sign of any lesion. As illustrated in Fig.
3, the combined treatment caused 95~ reduction (compared to control) in serum testosterone (T) and a 25 to 60~. fall in the serum levels of adrenal steroids, namely DHEA, DHEAS, Q4-dione and Q5-diol while not affecting cortisol signlEicantly. S0rum levels of DHT
anA E2 were also d0creased by ~0 to 4n~. During hormonal therapy, no cllnical sign of the disease could be detected. The only side-effects were related to hypoandrogenicity. Thus, after four months of treatment, the patient developed mild climateric-like vasomotor phenomena consisting of perspiration and hot flushes, which did not require treatment. He also complained of loss of libido and sexual potency after two months of treatment.
The present data show a rapid and complete regression of bone metastases in a patient having wide-spread bone metastases from breast-cancer. A complete response could be seen within 6 1/2 months after ~.~'78748 starting the combined treatment with an LH-RH agonist and a pure antiandrogen.
INHIBITORY EFFECT OF AMIN~GLUTETHIMIDE OR
KETOCONAZOLE ON LHRH AGONIST-IND~CED SERUM
TESTOSTERONE IN THE DOG
Figures 4 to 6 show the result of the test.
Fig. 4. Serum levels of testosterone during the first 19 days of treatment of dogs with daily administration of 50 ~g of [D-Trp6]LHRH ethylamide.
Fig. 5. Serum levels of testosterone during the first 19 days o treatment of dogs with daily administration to 50 ~9 of [D-Trp6]LHRH ethylamide in association with ketoconazole.
Fig. 6. Serum levels of testosterone during the first 19 dàys of treatment of dogs with daily administration of 50 ~9 of [D-Trp6]LHRH ethylamide in association with amlnoglutethimide.
~ hile LH~H flgonists achieve castration levels of androgens during chronlc treatment in men, the first 5 to 10 days of administration of the peptide are associated with increased serum levels o testosterone and dihydrotestosterone ~Labrie et al., J. Androl. 1:
209-228, 1980). These increased levels of testicular androgens are accompanied by an exacerbation of the symptoms and signs of prostate cancer in significant proportion of cases ~Kahan et al., The Lancet i, 971-972, 1984).
The following experiment shows that the LHRH
agonist-induced rise in serum testosterone can be prevented by simultaneous administration of the steroid 78q4~
biosynthesis inhibitors aminoglutethimide or ketaconazole.
Eighteen mongrel dogs weighing between 20-30 kg were randomly divided into three groups. The animals were housed one per cage and fed Purina Dog Chow and tap water ad libitum.
The animals of group 1 were injected daily ~at 0700h) with 50 ~g of the LHRH agonist [D-Trp6, des-Gly-NH210]LHRH ethylamide (LHRH-A). In group 2, the animals were also injected daily with 50 ~g of LHRH-A
and took in addition 200 mg of ketoconazole per os at 0700h, 1500h and 2300h. The animals of group 3 received daily 50 ~g of LHRH-A and 125 mg of aminoglutethimide per os at 0700h, 1500h, 2300h plus 10 mg of hydrocortisone twice daily.
Blood samples were collected at 0700h, O900h, llOOh and 1500h one day before treatment and every day during the treatment. Plasma was extracted with diethyl ether and testosterone was separated on LH-20 columns before RIA mea~urements.
Fig. 4 shows that on one to six days following the start of treatment with the dailty injection of 50 ~g of the LHRH agonist ~D-Trp6]LHRH
ethylamide, there is an increase in serum testosterone up to approximately 500% above control. Thereafter, there is a decrease of the level of this androgen which reaches near-castration levels on day 19. It can be seen in Fig. 5 and 6 that the simultaneous administration of the steroid inhibitors ketoconazole or aminoglutethimide almost completely prevented this rise in serum testosterone which occur during the first days of treatment with a peptide.
These data clearly indicate the usefulness of the combined administration of inhibitors of steroid blosynthesis in order to pr~vent the rise of testicular serum androgens during the first days of treatment with LHRH agonist~.
Since dogs do not have adre~al p~odu~tlon of androgens the influence of the admlnistration o~ an antiand~ogen in combination with the ad~lnistratlon of the LH-RH a~onist and the inhLbitor~ of ~3ex steroid biosynthesis cannot be demonstrated in thi~ species.
Howeve~, it can be concl~ded from the te~t results that in men the admini6tration of an antiandrogen (especially flutamide) in combin~tion with the LH-RH
agonist or antagonist And the inhibitors of sex steroid biosynthesls which lnhibit the s~cretion of precursor adrenal androgens substantially or comp1etely decr~ases the content of andro~ens in the sy~tem and t`nus cont~-ibutes to the inhibition of and~ogen 5ensitive cancer ~rowth.
The ilnportant aspect~ of ~his lnvention can be summarized ~ follows:
The invcn~ion provid~s:
l~ A method of treating sex st~roid dependent cancers in a warm-bloodcd animal which comprises admlnistering a phar~aceutically efective amount oi an ant~androgen and/or an antiestrogen and~or at lea~t one ~nhibitor of sex ~teroid biosynthesi~ to the animal whose hormone output o~ the testes or ovaries, is blocked, with the proviso that ~he method of treating prostate cancer ccmprises administering pharmace~tically e~fective a~ounts o~ an anti~ndrogen and at least one inhibitor of sex steroid biosynthesis and the method of treating breast cancer comprises a~ministering a pharmaceu-tically effective a~ount (l) of an an~landrogen o~ (2) of at least one inhibitor of sex steroid biosynthesls ~ ~7~8 or (3) of an antiandrogen and an antiestrogen or (4) o~
an antiandrogen and at least one inhibitor of sex steroid biosynthesls or t5~ of an antiestrogen and at least one inhibitor of sex steroid biosynthesis or (6) of an antiandrogen and an antiestrogen and at least one inhibitor of sex steroid biosynthesis.
~) A kit c~mprislng a combination of pharmaceutical composition~ for combination therapy of sex steriod dependent cancers in a warm-blooded animal whose hormone output of the testes or ovaries, is blocked, the combination consisting Oe pharmaceuti~al compositions co~p~ising (1) an antiandro~ein and ~n antiestrogen or (2) an antiand~ogen and at least one inhibitor of sex ste~old blosynthesi~ or (3) an antie.st~ogen and at least one inhi~itor of sex ~teroid biosynthesis ot (4) an antiandror~en ~nd an anties~rogen and at l~ast on~ inhibitor Of ~ex ~teroid b.iosynthesis.
3~ A kit comprising a pharmaccutic~l composition comprising fln ar~ti~ndro~en an~/or ~ ~harmaceutical composition comprising ~n ~nties~rogerl and/or one or mOre phar~ac~utical composi~ion(s) comprisiny an inhi~itor of sex steroid ~iosynthesis co~ether with instructions for `using the composition(s) or each of these compositions for the tr~atment o~ sex steroid dependent cancer.s in a warm-blooded animal by a combination therapy involvlng administering a pharmaceutically e~fective a~ount of an antiandrogen and/or an antiestrogen and/ot at least o.ne inhibitor of sex steroid biosynthesis to the animal whose hormone output of the testes or ovarie.s, is blocked, w~th the proviso that the instructions for treating prostate cancer recommend administerlng pharmaceutically effective a~ounts of an antiandrogen and at least one ~nhibltor of sex steroid biosynthesis and the instructions for treating beeast: cancer recommend administering a pharma~eutically effective amount (1) of an anttandror~en or (2) of at least one inhibitor of sex ster~id bio~ynthesiS or (3) of an antiandro~en and an antiestro~en or (4) of an antiandrogen and at least one inhibitor of sex steroid biosynthesis or (5) of an antiestrogen and at least one inhibitor of sex steroid biosynthesis or (6) of an antiandrogen and an antiesttogen and at least one inhibitor of sex steroi~
biosyntl-esis.
4) Use of a~ antiandro~en and~or an anties~royen and/or at least one inhibitor o sex steroid bio.synthesis for treating sex steroid dependent eancers in a warm-blooded animal by administering a pharmaceutically ef~ective amount of an antiandrogen and/or an antiestrogen and/or at le~t one inhibitor of sex steroi~ biosyntheSis to the animal whose hormone output o~ t~ teste~ or ovaries is blocked with the proviso that tre~ting prostate cancet comprises administering pharma~eutically ef~ective amounts of an antiandro~en and at least one inhibito~ of sex steroid hiosynthesis and treating breast cancer ~o~prises administering a p~larmace~tieally e~fective amount (1) of a~ a~tiandro-~en or (2) of at least one inhibit~r of sex steroid hiosynthesis or (3) of an antiand~ogen and an antiestrogen or (4~ of an antiandro~en and at least one lnhibitor of sex steroid biosynth~is or (5) of an antiestrogen and at least one inhibitor of sex steroid biosynthesis or (6~ of an antiandrogen and an antiestrogen and at least one inhibito~ of sex steroid biosynthesis, ~7874~3 5) The use of an antiandrogen and/or an antiestrogen and/or at least one inhibitor of sex steroid biosyn-thesis for the manufacture of a medicament for combination therapy of sex steroid dependent cancers in a warm-blooded animal which therapy comprises adminis-tering a pharmaceutically effective amount of an antiandrogen and/or an antiestrogen and/or at least one inhibi-tor of sex steroid biosynthesis to the animal whose hormone output of the testes or ovaries is blocked, with the proviso that the therapy of prostate cancer comprises administering pharmaceu-tically effective amounts of an antiandrogen and at least one inhibitor of sex steroid biosynthesis and the therapy of breast cancer comprises administering a pharmaceutically effective amount (1) of an anti-androgen or (2) of at least one inhibitor of sex steroid biosynthesis or (3) of an antiandrogen and an antiestrogen or (4) of an antiandrogen and at least one inhibitor of sex steroid biosynthesis or (5) of an antiestrogen and at least one inhibitor of sex steroid biosynthesi.s or (6) of an antiandrogen and an anti.estroyen and at least one :inhibitor of sex steroi.d biosyntllesis.
6) A combination of pha.rmaceuti.cal composit:Lons for combi.nation therapy of sex steroid dependent cancers in a warm-blooded an:imal whose hormone output of the testes or ovaries is blocked, the combination consisting of pharmaceutical compositions comprising an antiandrogen and antiestrogen or an antiandrogen and at least one inhibitor of sex steroid biosyn-thesis or an antiestrogen and at least one inhibitor of sex steroid biosynthesis or an antiandrogen and an antiestrogen and at least one inhibitor of sex steroid biosynthesis.
~787~
Prefer~ed aspects of the invention can be su.~narized as follows:
a) For trea~ing testicular cancer, ovarian cancer, colon-~eotal cancer, renal cancer, pa~creatic cancer, liver cancer, stomach cancer, ski~ cancer, uteri~e cancer, braln cancer and lary?x cance~: admi.~isterlng an antiandrogen ~nd/or an antiestrogen and/or at least on* inhibitor of sex steroid biosynthesis.
b) ~or ~reati~g breast ca~cer, testicular cancer~
ovarian cancer, colon-rectal c~ncer, L-enal cancer, pancreatic cance~, liver CaneeL-, s~omaoh cancer, skin cancet, uterine ca~cer, brain cancer and larynx cancer: a~ministtation of an antiandro~e? vr of an antiandro~en an~ an a~tiestro~en or of ~n antian,~rogen and at leas~ one inhibitor of sex steroid biosynthesis or of an antiestro~en an~ at least one inhibitor o~ sex steroid biosynthe~is or o~ an ~n~iandrogen and ~n antiestrogen and at lea~t o~e inhibitor of sex steroid biosynthesis.
c) Ad~inist.r~tion of the a~tiandrogen and/or the a.~tiestroge.? and/oc at le~st one inhibitor of .sex steroid biosy~thesis and, if used, the glucocorticoid such ~s hydtocorti~one, to an animal who~e hormone output of tll~ testes or ovaries, has been blocked by su~-yical ren)oval thereof.
d) Admini~stration of ~he a~?tia~dro(~e., and/or the a~tiestroge, and/ or at least one i;?hibitor of sex steroid bios~:lthesis a~d, if use~, the glucocorticoid, such as hydrocortisone to an anim~l whose hormone output of the testes or ova~-ies, is blo~ke-~ by chemical 1'~7~
--ql--mean~ such as ~y an LH-RH agon~st or L~-RH antagonist of whlch a pharmace~tically ef~ective amount is adminl~tered ~o the animal in a~sociatlon with ~he antlandrogen and/or the ~tiestrogen and/or the inhibi~orts) of s~eroid biosy~thesi~ and/or the glucoc~Itlcoid.
e) Admlni~tratlon of the antiandrogen, the a~tiestrogen, the inhibitor(s) of sex ste~old biosynthesis, the LH-RH agonist or LH-RH antagonist and the gluco~orticoid (if appli~able) in the form of individual eompositions.
~) Pre~erably the antiandrogen a~d/or the a~tiestro~en i~ started one day before the administration of tha LH-RH agonist o~ LH-RH antagonist and of the inhibitoL-(s) of sex ste~oid biosynthesis ~i used) and the ~lucocortiooid tif used).
g) Admin~stratlon of the ~-RH a~onist or l.H-RH
ant~yonist in the orm of a p~nt~ral compo.sition.
h~ Administration o~ the a~.ia~ro~en, antiestroye."
the inhi~itor(~) of sex steroid biosynthesis a~d the glucocorticoid Quch a~ the hydroco~tisone in the for~
of oral compositions.
1) The preferred antiandrogen is 4'-nitro-3'-tri-fl~oromethylisobutyranilide or 1-~3'-tri~luorometh~l-4'-nitrophe,yl)-4,4-dimethylimidazoline-2,S-dione.
j) The preferred LH-RH a~onist is a nonapeptide or a decapeptide represented by the formula : L-pyto-glutamyl-L-histi~yl-L-tryptophyl-L-seryl-L-~yrosyl-X-Y-1~7~
L-arginyl~~-prolyl-z~ wherein X ls D-tryptophyl, D-leucyl, ~-alanyl, iminoben~yl-D-histidyl, 3-(2-naph-thyl)-D-alanyl~ 0-tert-butyl-D-seryl, D-tyrosyl, ~-lysyl, D-phenylal~nyl or N-methyl-D-alanyl and wherein Y is L-leucyl, ~-methyl-L-leucyl, D-leucyl, N-methyl-D-le~cyl, or D alanyl and wh~rein ~ is glycyl-NHRl o~
N~Rl wherein Rl is H, lower alkyl or haloloweralkyl.
k) Preferably aminoglutethimide and/or ketokona201e is/are u~ed ~s in~ibitors of~sex steroid biosynthes1s.
1) The preferted antiestrogen i~ (z)-2-~4-(1,2-diphenyl-l-b~tenyl)phenoxy~-~,N-dimethylethanamlne or LY-117018.
Rel~ing to these pre~erred aspe~ts the inventio~ ~rovides kits compri~ing compositions containing the relevant ac~ive ~ul)stance~, possibiy together with ingtruction to use them.
~787~
Prefer~ed aspects of the invention can be su.~narized as follows:
a) For trea~ing testicular cancer, ovarian cancer, colon-~eotal cancer, renal cancer, pa~creatic cancer, liver cancer, stomach cancer, ski~ cancer, uteri~e cancer, braln cancer and lary?x cance~: admi.~isterlng an antiandrogen ~nd/or an antiestrogen and/or at least on* inhibitor of sex steroid biosynthesis.
b) ~or ~reati~g breast ca~cer, testicular cancer~
ovarian cancer, colon-rectal c~ncer, L-enal cancer, pancreatic cance~, liver CaneeL-, s~omaoh cancer, skin cancet, uterine ca~cer, brain cancer and larynx cancer: a~ministtation of an antiandro~e? vr of an antiandro~en an~ an a~tiestro~en or of ~n antian,~rogen and at leas~ one inhibitor of sex steroid biosynthesis or of an antiestro~en an~ at least one inhibitor o~ sex steroid biosynthe~is or o~ an ~n~iandrogen and ~n antiestrogen and at lea~t o~e inhibitor of sex steroid biosynthesis.
c) Ad~inist.r~tion of the a~tiandrogen and/or the a.~tiestroge.? and/oc at le~st one inhibitor of .sex steroid biosy~thesis and, if used, the glucocorticoid such ~s hydtocorti~one, to an animal who~e hormone output of tll~ testes or ovaries, has been blocked by su~-yical ren)oval thereof.
d) Admini~stration of ~he a~?tia~dro(~e., and/or the a~tiestroge, and/ or at least one i;?hibitor of sex steroid bios~:lthesis a~d, if use~, the glucocorticoid, such as hydrocortisone to an anim~l whose hormone output of the testes or ova~-ies, is blo~ke-~ by chemical 1'~7~
--ql--mean~ such as ~y an LH-RH agon~st or L~-RH antagonist of whlch a pharmace~tically ef~ective amount is adminl~tered ~o the animal in a~sociatlon with ~he antlandrogen and/or the ~tiestrogen and/or the inhibi~orts) of s~eroid biosy~thesi~ and/or the glucoc~Itlcoid.
e) Admlni~tratlon of the antiandrogen, the a~tiestrogen, the inhibitor(s) of sex ste~old biosynthesis, the LH-RH agonist or LH-RH antagonist and the gluco~orticoid (if appli~able) in the form of individual eompositions.
~) Pre~erably the antiandrogen a~d/or the a~tiestro~en i~ started one day before the administration of tha LH-RH agonist o~ LH-RH antagonist and of the inhibitoL-(s) of sex ste~oid biosynthesis ~i used) and the ~lucocortiooid tif used).
g) Admin~stratlon of the ~-RH a~onist or l.H-RH
ant~yonist in the orm of a p~nt~ral compo.sition.
h~ Administration o~ the a~.ia~ro~en, antiestroye."
the inhi~itor(~) of sex steroid biosynthesis a~d the glucocorticoid Quch a~ the hydroco~tisone in the for~
of oral compositions.
1) The preferred antiandrogen is 4'-nitro-3'-tri-fl~oromethylisobutyranilide or 1-~3'-tri~luorometh~l-4'-nitrophe,yl)-4,4-dimethylimidazoline-2,S-dione.
j) The preferred LH-RH a~onist is a nonapeptide or a decapeptide represented by the formula : L-pyto-glutamyl-L-histi~yl-L-tryptophyl-L-seryl-L-~yrosyl-X-Y-1~7~
L-arginyl~~-prolyl-z~ wherein X ls D-tryptophyl, D-leucyl, ~-alanyl, iminoben~yl-D-histidyl, 3-(2-naph-thyl)-D-alanyl~ 0-tert-butyl-D-seryl, D-tyrosyl, ~-lysyl, D-phenylal~nyl or N-methyl-D-alanyl and wherein Y is L-leucyl, ~-methyl-L-leucyl, D-leucyl, N-methyl-D-le~cyl, or D alanyl and wh~rein ~ is glycyl-NHRl o~
N~Rl wherein Rl is H, lower alkyl or haloloweralkyl.
k) Preferably aminoglutethimide and/or ketokona201e is/are u~ed ~s in~ibitors of~sex steroid biosynthes1s.
1) The preferted antiestrogen i~ (z)-2-~4-(1,2-diphenyl-l-b~tenyl)phenoxy~-~,N-dimethylethanamlne or LY-117018.
Rel~ing to these pre~erred aspe~ts the inventio~ ~rovides kits compri~ing compositions containing the relevant ac~ive ~ul)stance~, possibiy together with ingtruction to use them.
Claims (15)
1. A composition for treating sex steroid dependent cancers in a warm-blooded animal which comprises a pharmaceutically effective amount of an antiandrogen and/or an antiestrogen and/or at least one inhibitor of sex steroid biosynthesis, and a carrier, with the proviso that the composition for treating prostate cancer comprises pharmaceutically effective amounts of an antiandrogen and at least one inhibitor of sex steroid biosynthesis and the compo-sition for treating breast cancer comprises a pharma-ceutically effective amount of an antiandrogen, or of at least one inhibitor of sex steroid bio-synthesis, or of an antiandrogen and an antiestrogen, or of an antiandrogen and at least one inhibitor of sex steroid biosynthesis, or of an antiestrogen and at least one inhibitor of sex steroid biosynthesis, or of an antiandrogen and an antiestrogen and at least one inhibitor of sex steroid biosynthesis and with the further proviso that in the composition for treating breast cancer in a female animal, an anti-androgen and an antiestrogen is excluded and an anti-androgen, an antiestrogen and at least one inhibitor of sex steroid biosynthesis is also excluded.
2. The composition according to claim 1 for treating testicular cancer, ovarian cancer, colon-rectal cancer, renal cancer, pancreatic cancer, liver cancer, stomach cancer, skin cancer, uterine cancer, brain cancer and larynx cancer which comprises an antiandrogen and/or an antiestrogen and/or at least one inhibitor of sex steroid bio-synthesis.
3. The composition according to claim 1 or 2 for treating breast cancer, testicular cancer, ovarian cancer, colon-rectal cancer, renal cancer, pancreatic cancer, liver cancer, stomach cancer, skin cancer, uterine cancer, brain cancer and larynx cancer which comprises an antiandrogen or an anti-androgen and an antiestrogen or an antiandrogen and at least one inhibitor of sex steroid biosynthesis or an antiestrogen and at least one inhibitor of sex steroid biosynthesis or an antiandrogen and an anti-estrogen and at least one inhibitor of sex steroid biosynthesis.
4. The composition according to claim 1 which further comprises a qlucocorticoide.
5. The composition according to claim 4 wherein said glucocorticoide is hydrocortisone.
6. The composition according to any one of claims 1, 2 or 4 wherein the antiandrogen and/or the antiestrogen and/or at least one inhibitor of sex steroid biosynthesis and, if used, the gluco-corticoide, such as hydrocortisone, is/are intended for the treatment of all an animal whose hormone output of the testes or ovaries, respectively, has been blocked by surgical removal of the testes or ovaries, respectively.
7. The composition according to claim 4 wherein the antiandrogen and/or the antiestrogen and/or at least one inhibitor of sex steroid bio-synthesis and, whenever used, the glucocorticoide, is/are intended for the treatment of an animal whose hormone output of the testes or ovaries, respectively, is blocked by chemical means such as by an LH-RH
agonist or LH-RH antagonist of which a pharma-ceutically effective amount is used in association with the listed substances.
agonist or LH-RH antagonist of which a pharma-ceutically effective amount is used in association with the listed substances.
8. The composition according to claim 7, wherein said glucocorticoid is hydrocortisone.
9. The composition according to claim 4 wherein the antiandrogen, the antiestrogen, the inhibitor(s) of sex steroid biosynthesis, the LH-RH
agonist or LH-RH antagonist and the glucocorticoide, whenever present, are in the form of individual compositions.
agonist or LH-RH antagonist and the glucocorticoide, whenever present, are in the form of individual compositions.
10. The composition according to claims 7 or 9 wherein the LH-RH agonist or LH-RH antagonist is in the form of a parenteral composition.
11. The composition according to claim 4 wherein the antiandrogen, antiestrogen, the inhibi-tor(s) of sex steroid synthesis and the gluco-corticoide such as the hydrocortisone are in the form of oral compositions.
12. The composition according to any one of claims 1, 2 or 4 wherein the antiandrogen is 4'-nitro-3'-trifluoromethyliobutyranilide or 1-(3'-tri-fluoromethyl-4'-nitrophenyl)-4,4-dimethylimidazoline-2,5-dione.
13. The composition according to any one of claims 1, 7 or 9 wherein the LH-RH agonist is a nonapeptide or a decapeptide represented by the formula: L-pyroglutamyl-L-histidyl-L-tryptophyl-L-seryl-L-tyrosyl-X-Y-L-arginyl-L-propyl-Z, wherein X
i.s D-tryptophyl, D-leucyl, D-alanyl, iminobenzyl-D-hi.stidyl, 3-(2-naphthyl)-D-alanyl, 0-tert-butyl-D-seryl, D-tyrosyl, D-lysyl, D-phenylalanyl or N-methyl-D-alanyl and wherein Y is L-leucyl, N
methyl-L-leucyl, D-leucyl Na-methyl-D-leucyl, or D-alanyl and wherein Z i.s glycil-NHRl or NHRl wherein Rl is H, lower alkyl or haloloweralkyl.
i.s D-tryptophyl, D-leucyl, D-alanyl, iminobenzyl-D-hi.stidyl, 3-(2-naphthyl)-D-alanyl, 0-tert-butyl-D-seryl, D-tyrosyl, D-lysyl, D-phenylalanyl or N-methyl-D-alanyl and wherein Y is L-leucyl, N
methyl-L-leucyl, D-leucyl Na-methyl-D-leucyl, or D-alanyl and wherein Z i.s glycil-NHRl or NHRl wherein Rl is H, lower alkyl or haloloweralkyl.
14. The composition according to any one of claims 1, 7 or 9 wherein aminoglutethimide and/or ketokonazole are used as inhibitors of sex steroid biosynthesis.
15. The composition according to any one of claims 1, 7 or 9 wherein the antiestrogen is (Z)-2-[4-(1,2-di.phenyl-1-butenyl)phenoxy]-N,N-dimethyl-ethanamlne or LY-117018.
Applications Claiming Priority (6)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| US699,702 | 1976-06-25 | ||
| US06/699,710 US5023234A (en) | 1985-02-08 | 1985-02-08 | Combination male breast cancer therapy |
| US699,711 | 1985-02-08 | ||
| US699,710 | 1985-02-08 | ||
| US06/699,702 US4666885A (en) | 1985-02-08 | 1985-02-08 | Combination therapy for treatment of female breast cancer |
| US06/699,711 US4659695A (en) | 1985-02-08 | 1985-02-08 | Method of treatment of prostate cancer |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| CA1278748C true CA1278748C (en) | 1991-01-08 |
Family
ID=27418692
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA000488048A Expired - Lifetime CA1278748C (en) | 1985-02-08 | 1985-08-02 | Pharmaceutical composition for combination therapy of hormone dependent cancers |
Country Status (1)
| Country | Link |
|---|---|
| CA (1) | CA1278748C (en) |
-
1985
- 1985-08-02 CA CA000488048A patent/CA1278748C/en not_active Expired - Lifetime
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