GnRH analog, leuprorelin acetate, promotes regeneration of rat spermatogenesis after severe chemical damage

Udagawa, Koichi; Ogawa, Takehiko; Watanabe, Takeshi; Yumura, Yasushi; Takeda, Mitsumasa; Hosaka, Masahiko

doi:10.1046/j.1442-2042.2001.00382.x

Cited by 50 publications

(45 citation statements)

References 23 publications

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“…They found that the administration of GnRH agonist during cyclophosphamide chemotherapy may protect spermatogenesis. These promising results were reproduced 20 years later by Udagawa et al (15).…”

Section: Discussionmentioning

confidence: 68%

Preventive role of exogenous testosterone on cisplatin-induced gonadal toxicity: an experimental placebo-controlled prospective trial

Aminsharifi

Shakeri

Ariafar

et al. 2010

Fertility and Sterility

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Section: Discussionmentioning

confidence: 68%

Preventive role of exogenous testosterone on cisplatin-induced gonadal toxicity: an experimental placebo-controlled prospective trial

Aminsharifi

Shakeri

Ariafar

et al. 2010

Fertility and Sterility

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“…The reduction of gonadotropin secretion results in lower testosterone levels in testes, leading to the inhibition of spermatogenesis [40], particularly in postmeiotic phase [4,41,42]. In contrast, recent studies have shown that GnRH-analogues stimulate regeneration of spermatogenesis after testicular damage caused by irradia- tion or chemical toxins [3,6,8]. A study using irradiated testis model has suggested that GnRH-antagonist reduces spermatogonial apoptosis, thus increasing the number of spermatogonia [9].…”

Section: Discussionmentioning

confidence: 92%

“…This result was unexpected because the predominant effect of GnRH-analogues had been believed to inhibit spermatogenesis, as GnRH-analogue administration reduces LH and FSH, thereby suppressing testosterone level [4,5]. Subsequent studies, however, have confirmed that GnRH-analogues, both agonist and antagonist, can promote the regeneration process of spermatogenesis following testicular injuries by irradiation or cancer chemotherapy drugs [6][7][8]. Another study showed that GnRH-antagonist enhanced the proliferation and differentiation of type A spermatogonia, probably due to reduced levels of apoptotic cell death [9].…”

Section: Introductionmentioning

confidence: 93%

Increment of Murine Spermatogonial Cell Number by Gonadotropin-Releasing Hormone Analogue Is Independent of Stem Cell Factor c-kit Signal1

Ohmura

Ogawa

Ono

et al. 2003

Biology of Reproduction

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Recent studies have demonstrated that GnRH-analogues can stimulate regeneration of spermatogenesis of rats when administered after testicular damages. Although the mechanism of this phenomenon has not been elucidated yet, stem cell factor (SCF) produced by Sertoli cells was proposed to mediate the effects of GnRH-analogues on spermatogonial proliferation and/or survival. In the present study, we quantitatively evaluated the proliferation of spermatogonia and addressed whether SCF mediates the effect of GnRH-analogue on spermatogonial proliferation, using a novel approach combining spermatogonial transplantation and laser confocal microscopic observation. In the first experiment, using wild-type mice as recipients for spermatogonial transplantation, the number of donor spermatogonia per 100 Sertoli cells in each spermatogenic colony was significantly higher in the experimental group of mice treated with leuprorelin, a GnRH-agonist, than that of the control group at 4 and 5 wk after transplantation. In the second experiment, Steel/Steeldickie (Sl/Sld) mutant mice, which lack expression of membrane bound form SCF, were used as recipients. As seen in the first experiment, the number of undifferentiated spermatogonia was significantly higher in leuprorelin-treated than in the control group. Since undifferentiated spermatogonia do not express the receptor of SCF, the present study clearly demonstrates that neither membrane-bound nor secreted forms of SCF are involved in the mechanism of GnRH-analogue's effect on spermatogonial proliferation and/or survival.

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“…Nevertheless, when additional time without further suppressive treatment was allowed before the rats were killed, all tubules showed almost complete spermatogenic recovery, sperm counts increased, and the fertility of the rats significantly increased (Meistrich et al 2001). This phenomenon appears to be quite general: posttreatment with GnRH agonists or antagonists, with or without antiandrogen, low-dose systemic testosterone, estradiol, or hypophysectomy are all effective at stimulating recovery (Shetty et al 2002, and recovery has been stimulated following gonadal toxicity from anticancer agents, such as radiation, procarbazine (Meistrich et al 1999), or busulfan (Udagawa et al 2001), and environmental toxicants, such as hexanedione (Blanchard et al 1998) or dibromochloropropane (Meistrich et al 2003), an indenopyridine compound (Hild et al 2001), or heat treatment (Setchell et al 2001). The endogenous hormone primarily responsible for the inhibition of spermatogonial differentiation in toxicant-treated rats was testosterone, although follicle-stimulating hormone (FSH) also had a minor inhibitory effect , and other exogenously administered androgens were also inhibitory (Shetty et al 2002).…”

Section: Experimental Studies -Malesmentioning

confidence: 92%

Hormonal suppression for fertility preservation in males and females

Meistrich¹,

Shetty²

2008

Reproduction

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Methods to restore fertility of men and women sterilized by medical treatments and environmental toxicant exposures are under investigation. Rendering spermatogenesis and ovarian follicular development kinetically quiescent by suppression of gonadotropins has been proposed to protect them from damage by cytotoxic therapy. Although the method fails to protect the fertility of male mice and monkeys, gonadotropin and testosterone suppression in rats before or after cytotoxic therapy do enhance the recovery of spermatogenesis. However, the mechanism involves not the induction of quiescence but rather the reversal, by suppression of testosterone, of a block in differentiation of surviving spermatogonia caused by damage to the somatic environment. In men, only one of eight clinical trials was successful in protecting or restoring spermatogenesis after cytotoxic therapy. In women, protection of primordial follicles in several species from damage by cytotoxic agents using GnRH analogs has been claimed; however, only two studies in mice appear convincing. The protection cannot involve the induction of quiescence in the already dormant primordial follicle but may involve direct effects of GnRH analogs or indirect effects of gonadotropin suppression on the whole ovary. Although numerous studies in female patients undergoing chemotherapy indicate that GnRH analogs might be protective of ovarian function, none of the studies showing protection were prospective randomized clinical trials and thus they are inconclusive. Considering interspecies differences and similarities in the gonadal sensitivity to cytotoxic agents and hormones, mechanistic studies are needed to identify the specific beneficial effects of hormonal suppression in select animal models that may be applicable to humans.

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GnRH analog, leuprorelin acetate, promotes regeneration of rat spermatogenesis after severe chemical damage

Cited by 50 publications

References 23 publications

Preventive role of exogenous testosterone on cisplatin-induced gonadal toxicity: an experimental placebo-controlled prospective trial

Preventive role of exogenous testosterone on cisplatin-induced gonadal toxicity: an experimental placebo-controlled prospective trial

Increment of Murine Spermatogonial Cell Number by Gonadotropin-Releasing Hormone Analogue Is Independent of Stem Cell Factor c-kit Signal1

Hormonal suppression for fertility preservation in males and females

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