Inhibition of growth of experimental prostate cancer with sustained delivery systems (microcapsules and microgranules) of the luteinizing hormone-releasing hormone antagonist SB-75.

Korkut, E.; Bokser, L.; Comaru-Schally, A. M.; Groot, Kate; Schally, A. V.

doi:10.1073/pnas.88.3.844

Cited by 26 publications

(11 citation statements)

References 27 publications

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“…Subse quently, we and others synthesized new LH-RH antagonists free of edematogenic effects and other anaphylactoid reactions in rats and human beings [6,7,9,[31][32][33][34][35]. Among these analogs, SB-75 proved to be one of the most potent as judged by the inhibition of LH levels in castrated rats in doses as small as 0.625 gg and by a marked suppression of testosterone to castra tion levels in intact rats [9], In oncological studies, SB-75 inhib ited the growth of experimental mammary cancers in mice [36] and rats [35], pancreatic cancer in hamsters [37] and prostate cancers in rats [38][39][40].…”

Section: Discussionmentioning

confidence: 99%

Recovery of Pituitary-Gonadal Function in Male and Female Rats after Prolonged Administration of a Potent Antagonist of Luteinizing Hormone-Releasing Hormone (SB-75)

Bokser¹,

Srkalović

Szepesházi

1991

Neuroendocrinology

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The reversibility of the antifertility effects induced by long-term administration of the LH-RH antagonistic analog [Ac-D-Nal(2)’, D-Phe(4Cl)², D-Pal(3)³, D-Cit⁶, D-Ala¹⁰]-LH-RH (SB-75) was investigated in male and female rats. Male rats were implanted with osmotic minipumps releasing 50 µg of SB-75/day for 60 days. The control rats were implanted with minipumps containing only vehicle. The treatment with the antagonist caused a significant decrease in the weights of the testes, seminal vesicles and ventral prostates (p < 0.01) and reduced serum LH and testosterone levels (p < 0.01). The histology of the testes from the treated rats showed that spermatogenesis was totally depressed. No mature elongated or round spermatids were found in the seminiferous tubules, spermatocytes being the most advanced germ cell form in 100% of the testicular tubules. These changes indicate that a total spermatogenetic arrest occurred in the treated animals. Ninety days after cessation of treatment with the LH-RH antagonist, there was a complete recovery of the weights of the testes, seminal vesicles and ventral prostates and LH and testosterone returned to control levels. Histological studies revealed a complete recovery of spermatogenesis, with 99.2% of seminiferous tubules containing mature elongated spermatids. Immediately after the discontinuation of treatment with SB-75, a significant down-regulation of the pituitary LH-RH receptors was found, but 90 days later, this phenomenon was completely reversed. Female rats were injected every 3 weeks for 6 weeks with SB-75 microcapsules, at a dose calculated to release 27 µg/day of the antagonist. The treatment with SB-75 disrupted the normal estrous cycle. Body weights were not affected, but ovarian and uterine weights were significantly decreased (p < 0.01 and p < 0.05, respectively) in the animals treated with the antagonist. Treated rats had significantly lower LH (p < 0.05) and estradiol (p < 0.01) levels than controls. The histology of the ovaries from the SB-75-treated group showed that the ratio of small to large maturing follicles increased significantly (p < 0.01) and corpora lutea were absent. Two months after the cessation of treatment, a complete recovery in the organ weights and in hormonal levels was observed and no histological differences were found between the ovaries in treated and untreated rats. These collective results indicate that the suppression of gonadal function induced by the treatment with LH-RH antagonist SB-75 is completely reversible both in male and female animals. These findings should facilitate the use of modern LH-RH antagonists, free of side effects, for the treatment of hormone-sensitive cancers, gynecologic conditions and other disorders where inhibition of the pituitary-gonadal axis is desirable.

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Section: Discussionmentioning

confidence: 99%

Recovery of Pituitary-Gonadal Function in Male and Female Rats after Prolonged Administration of a Potent Antagonist of Luteinizing Hormone-Releasing Hormone (SB-75)

Bokser¹,

Srkalović

Szepesházi

1991

Neuroendocrinology

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“…These analogues may have various practical applications, including treatment of gynecologic disorders and hormone-sensitive tumors such as prostate and breast cancers (1,2,(7)(8)(9). Although chronic administration of LHRH agonists is necessary for inhibition of LH, a single dose of a potent LHRH antagonist is sufficient to evoke the same effect (1, 2, 5-13).…”

mentioning

confidence: 99%

“…Some of them proved to be highly potent and free from edematogenic effects. The LHRH antagonists were also very effective in suppressing the growth of experimental mammary cancers and prostate tumors (7,9). To assess the bioactivity of these compounds, the dispersed rat pituitary superfusion system was initially used (5,6).…”

mentioning

confidence: 99%

Evaluation of luteinizing hormone-releasing hormone antagonistic activity in vitro.

Csernus¹

1992

Proc. Natl. Acad. Sci. U.S.A.

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Antagonistic analogues of luteinizing hormone-releasing hormone (LHRH) belong to a class of compounds that can be utilized for treatment of some hormonedependent cancers and gynecologic disorders. Recently, we synthesized and tested a large number of LHRH analogues for LHRH antagonistic activity in the dispersed pituitary cell superfusion system. This fast, reliable, and dynamic system made it possible for us not only to evaluate the relative amounts of an analogue required for suppression of the LH-releasing activity of exogenous LEIRH but also provided quantitative data on dynamic interactions between the LHRH analogue, LHRH receptors, and LH secretion. Three experimental paradigms were used: (i) LHRH responses after preincubation with the antagonist, (ii) pulsatile, simultaneous infusion of LHRH and the antagonistic analogue, and (iW) effects of the analogues on ongoing, continuous LH secretion induced by prolonged stimulation with LHRH. From the data obtained, we conclude that (') the suppression of the LHRH-induced LH release was more effective and longer lasting when the cells were preincubated with the antagonistic analogues before the LBRH stimulation than in the case of simultaneous exposure; (ui) not only the potency but also the time of onset and the duration of the LH release-suppressing activity varied according to the different peptides used, resulting in different shapes of response curves; and (ii) from the accurate data obtained in this dynamic system, quantitative parameters of the in vivo interactions between the antagonists and LBRH on the LHRH receptor can be calculated.In the past few years, a large number of antagonists of luteinizing hormone-releasing hormone (LHRH) has been synthesized and evaluated for therapeutic use (1-6). These analogues may have various practical applications, including treatment of gynecologic disorders and hormone-sensitive tumors such as prostate and breast cancers (1, 2, 7-9). Although chronic administration of LHRH agonists is necessary for inhibition of LH, a single dose of a potent LHRH antagonist is sufficient to evoke the same effect (1, 2, 5-13).

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“…The effectiveness of GnRH-a in cancer treatment, namely in prostate cancer and mammary gland tumors, was first established in animal models already 25 years ago (Redding et al 1982. The first studies with the cetrorelix (used in this study) were performed in the 1990s , Szende et al 1990, Korkut et al 1991. There are also reports showing the effectiveness of GnRH-a in benign prostate hyperplasia treatment (Lepor 2006) and they have been recently clinically tested in the treatment of human prostate cancer (Gittelman et al 2008, Klotz et al 2008, Huhtaniemi et al 2009).…”

Section: Discussionmentioning

confidence: 99%

Hecate-CGβ conjugate and gonadotropin suppression shows two distinct mechanisms of action in the treatment of adrenocortical tumors in transgenic mice expressing Simian Virus 40 T antigen under inhibin-α promoter

Vuorenoja

Mohanty²,

Arola³

et al. 2009

Endocrine-Related Cancer

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Lytic peptide Hecate (23-amino acid (AA)) fused with a 15-AA fragment of human chorionic gonadotropin-b (CG-b), Hecate-CGb conjugate (H-CGb-c) selectively binds to and destroys tumor cells expressing LH/chorionic gonadotropin receptor (Lhcgr). Transgenic mice (6.5 month old) expressing SV40 T-antigen under the inhibin-a promoter (inha/Tag) presenting with Lhcgr expressing adrenal tumors were treated either with H-CGb-c, GnRH antagonist (GnRH-a), estradiol (E 2 ; only females) or their combinations for 1 month. We expected that GnRH-a or E 2 in combination with H-CGb-c could improve the treatment efficacy especially in females by decreasing circulating LH and eliminating the potential competition of serum LH with the H-CGb-c. GnRH-a and H-CGb-c treatments were successful in males (adrenal weights 14G2.8 mg and 60G26 vs 237G59 mg in controls; P!0.05). Histopathologically, GnRH-a apparently destroyed the adrenal parenchyma leaving only the fibrotic capsule with few necrotic foci. In females, H-CGb-c was totally ineffective, whereas GnRH-a (19G5 mg) or E 2 (77G50 mg) significantly reduced the adrenal weights compared with controls (330G70 mg). Adrenal morphometry, cell proliferation markers, post-treatment suppression of serum progesterone, and quantitative RT-PCR of GATA-4, Lhcgr, and GATA-6 further supported the positive outcome. H-CGb-c selectively killed the Lhcgr expressing tumor cells, whereas GnRH-a blocked tumor progression through gonadotropin suppression, emphasizing the gonadotropin dependency of these adrenocortical tumors. If extrapolated to humans, H-CGb-c could be considered for the treatment of gonadotropin-dependent adrenal tumors in males, whereas in females gonadotropin suppression, but not H-CGb-c, would work better.

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Inhibition of growth of experimental prostate cancer with sustained delivery systems (microcapsules and microgranules) of the luteinizing hormone-releasing hormone antagonist SB-75.

Cited by 26 publications

References 27 publications

Recovery of Pituitary-Gonadal Function in Male and Female Rats after Prolonged Administration of a Potent Antagonist of Luteinizing Hormone-Releasing Hormone (SB-75)

Recovery of Pituitary-Gonadal Function in Male and Female Rats after Prolonged Administration of a Potent Antagonist of Luteinizing Hormone-Releasing Hormone (SB-75)

Evaluation of luteinizing hormone-releasing hormone antagonistic activity in vitro.

Hecate-CGβ conjugate and gonadotropin suppression shows two distinct mechanisms of action in the treatment of adrenocortical tumors in transgenic mice expressing Simian Virus 40 T antigen under inhibin-α promoter

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