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首页> 外文期刊>Acta endocrinologica >Relationships between FSH, inhibin B, anti-Mullerian hormone, and testosterone during long-term treatment with the GnRH-agonist histrelin in patients with prostate cancer
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Relationships between FSH, inhibin B, anti-Mullerian hormone, and testosterone during long-term treatment with the GnRH-agonist histrelin in patients with prostate cancer

机译:GnRH-激动剂组蛋白在前列腺癌患者长期治疗过程中FSH,抑制素B,抗Mullerian激素和睾丸激素之间的关系

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Objectives Medical castration with long-acting GnRH-agonist (GnRHa) is a well-established treatment for metastatic prostate cancer. Our aim was to explore the relationships between FSH, inhibin B, anti-Mullerian hormone (AMH), and testosterone during treatment with an implant releasing GnRHa. Design Analysis of hormone levels in frozen serum samples. Methods Ten patients aged 77±7 (means±s.e.m.) years with prostate cancer were treated with the GnRHa histrelin for at least a year. Two weeks prior to insertion and for 3–4 months following removal the patients were treated with the antiandrogen flutamide. Serum inhibin B, FSH, testosterone, and AMH levels were measured retrospectively. Results FSH, inhibin B, and testosterone increased during antiandrogen administration and levels fell after implant insertion. Four weeks post insertion, FSH gradually increased while inhibin B and testosterone remained fully suppressed. AMH levels did not change during antiandrogen treatment, but increased following implant insertion and remained elevated for the duration of implant use. Following removal, FSH and testosterone increased, inhibin B remained low, while AMH decreased. Conclusions The secondary increase in FSH following initial suppression with the implant is probably related to impaired inhibin B secretion. The lack of inhibin B response to the secondary increase in FSH suggests that long-term exposure of Sertoli-cells to GnRHa impairs their function. This effect appears to be selective since unlike inhibin B, AMH increased. In the absence of testosterone, FSH has a role in AMH regulation.
机译:目的长效GnRH激动剂(GnRHa)的医学去势是一种公认​​的转移性前列腺癌治疗方法。我们的目的是探讨用释放GnRHa的植入物治疗期间FSH,抑制素B,抗穆勒激素(AMH)和睾丸激素之间的关系。冷冻血清样品中激素水平的设计分析。方法10例77±7(平均±s.e.m。)岁的前列腺癌患者接受GnRHa组蛋白治疗至少一年。插入前两周,取出后3-4个月,患者接受抗雄激素氟他胺治疗。回顾性测量血清抑制素B,FSH,睾丸激素和AMH水平。结果抗雄激素给药期间FSH,抑制素B和睾丸激素增加,而植入植入物后水平下降。插入后四周,FSH逐渐升高,而抑制素B和睾丸激素仍被完全抑制。在抗雄激素治疗期间,AMH水平没有变化,但在植入植入物后增加,在植入物使用期间仍保持升高。去除后,FSH和睾丸激素增加,抑制素B保持较低,而AMH下降。结论植入物最初被抑制后,FSH的继发性增加可能与抑制素B分泌受损有关。缺乏对FSH继发增加的抑制素B反应,表明Sertoli细胞长期暴露于GnRHa会损害其功能。这种作用似乎是选择性的,因为与抑制素B不同,AMH增加了。在没有睾丸激素的情况下,FSH在AMH调节中起作用。

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