Jerry Ann Ward scite author profile

A sustained-release formulation of a potent gonadotropin-releasing hormone (GnRH) agonist, Zoladex (D-Ser(But),6 Aza Gly10-GnRH; ICI 118,630; goserelin), was administered subcutaneously (3.6 mg/depot) to male rats once every 28 days for 2-24 wk to determine the extent to which pituitary-testis function could be suppressed and whether suppression was maintained throughout the period of treatment. Administration of Zoladex resulted in sustained decreases in weight of the testis, epididymis, seminal vesicles and prostate gland. The decreases were apparent within 2 wk of initiating treatment. Patchy degeneration of the seminiferous tubules and atrophy of the Leydig cells were observed, but did not progress beyond the degree observed after 1 month of treatment. Serum and testis testosterone were markedly depressed after 2 wk of treatment, as was testis [125I]hCG binding. Serum gonadotropins were also reduced by treatment. Serum androgen binding protein (ABP) was elevated, testis ABP content remained unchanged, and epididymal ABP content was reduced. The changes are consistent with the hypothesis that this compound affects both the anterior pituitary gland and the testis. These findings indicate that depot delivery systems are a convenient way to administer GnRH analogs for sustained treatment schedules.

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Prolonged suppression of spermatogenesis by oestrogen does not preserve the seminiferous epithelium in procarbazine‐treated rats

Morris

Bardin

Gunsalus

et al. 1990

Int J of Andrology

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We examined the hypothesis that induction of reversible testicular atrophy, subsequent to withdrawal of gonadotrophin support, would alleviate the testicular toxicity of the anti-cancer drug procarbazine. In rats, severe but reversible testicular atrophy and suppression of spermatogenesis were induced 56 days after the subcutaneous insertion of a silastic implant containing oestradiol-17 beta. The effect of this treatment upon the testicular toxicity of four weekly doses of procarbazine (200 mg kg-1) was examined 56 days after the termination of procarbazine/oestrogen treatment. At this time the testicular endocrine and spermatogenic functions were close to normal in rats which has received only oestradiol-17 beta. Procarbazine produced severe testicular atrophy which was associated with azoospermia and destruction of the germinal epithelium. Serum LH and FSH concentrations were raised and were associated with low serum concentrations of both testosterone and androgen-binding protein. The combination of procarbazine with the oestrogen treatment did not change any of the testicular toxicity and in some cases it appeared to be exacerbated. In contrast to these experiments other studies have indicated that the testis can be protected if spermatogenesis is reversibly suppressed by other agents which are also active via the pituitary endocrine system. The data would therefore suggest that protection is achieved either by some testicular change other than withdrawal of pituitary gonadotrophin support or that oestradiol-17 beta has additional activity which is permissive for the development of the testicular toxicity of procarbazine.

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Strain-dependency of procarbazine-induced testicular toxicity

Ward

Robinson

Morris

1989

Reproductive Toxicology

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Relative Concentration and Daily Rhythms of Excretion of Epinephrine and Norepinephrine in Men With a Complete Section of the Spinal Cord

Walker¹,

Carter²,

Vallbona³

et al. 1969

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Jerry Ann Ward

Delayed effects of doxorubicin on spermatogenesis and endocrine function in rats

Prolonged Suppression of Rat Testis Function by a Depot Formulation of Zoladex,® a GnRH Agonist

Prolonged suppression of spermatogenesis by oestrogen does not preserve the seminiferous epithelium in procarbazine‐treated rats

Strain-dependency of procarbazine-induced testicular toxicity

Relative Concentration and Daily Rhythms of Excretion of Epinephrine and Norepinephrine in Men With a Complete Section of the Spinal Cord

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