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促性腺激素治疗男性低促性腺激素性性腺功能减退症。

Gonadotropin Treatment for the Male Hypogonadotropic Hypogonadism.

机构信息

Division of Experimental Oncology/Unit of Urology, URI, IRCCS Ospedale San Raffaele, Milan, Italy.

出版信息

Curr Pharm Des. 2021;27(24):2775-2783. doi: 10.2174/1381612826666200523175806.

Abstract

Hypogonadotropic hypogonadism (HH) is caused by a dysfunction in the hypothalamus and/or the pituitary gland and it can be congenital or acquired. This condition is biochemically characterized by low or inappropriately normal gonadotropin levels along with low total testosterone levels. If fertility is not an issue, testosterone therapy is the treatment of choice to induce and maintain secondary sexual characteristics and sexual function. Spermatogenesis is frequently impaired in patients with HH, but usually responsive to hormonal therapy such as gonadotropin therapy or GnRH supplementary/replacement therapy. When gonadotropins are the choice of treatment, conventional therapy includes human chorionic gonadotropin (hCG) along with different FSH formulations: human menopausal gonadotropins (hMG), highly purified urinary FSH preparations (hpFSH) (e.g., urofollitropin) or recombinant FSH (rFSH). The combination of FSH and hCG demonstrated to be associated with better outcomes than single compounds, whereas similar results were obtained with different FSH preparations in male individuals; both regarding the ability to stimulate spermatogenesis and eventually inducing physiology pregnancy. Gonadotropins can be administered either subcutaneously or intramuscularly. The combination therapy with hCG and FSH for a period of 12-24 months was found to promote testicular growth in almost all patients, spermatogenesis in approximately 80% and pregnancy rates in the range of 50%. Gynecomastia is the most common side effect of gonadotropin therapy and is due to hCG stimulation of aromatase causing increased secretion of estradiol. The therapeutic success is higher in patients with post-pubertal HH, in those without previously undescended testes, in patients with higher baseline testicular volume, who underwent repeated cycles of therapy and in patients with higher baseline inhibin B serum concentrations. Reversal of hypogonadism can occur in up to 10% of patients but its physiopathologic mechanism has yet to be elucidated. In conclusion, gonadotropin therapy is effective in promoting puberty and in supporting spermatogenesis onset and preservation in HH patients with either hypothalamic or pituitary conditions.

摘要

低促性腺激素性性腺功能减退症(HH)是由下丘脑和/或垂体功能障碍引起的,可分为先天性或获得性。这种情况在生化上表现为低或不适当的正常促性腺激素水平,同时伴有总睾酮水平降低。如果生育不是问题,睾酮治疗是诱导和维持第二性征和性功能的首选治疗方法。HH 患者的精子发生通常受损,但通常对激素治疗如促性腺激素治疗或 GnRH 补充/替代治疗有反应。当选择使用促性腺激素时,常规治疗包括人绒毛膜促性腺激素(hCG)和不同的 FSH 制剂:人绝经期促性腺激素(hMG)、高纯度尿促卵泡激素制剂(hpFSH)(如尿促卵泡素)或重组 FSH(rFSH)。FSH 和 hCG 的联合治疗显示与单一化合物相比具有更好的结果,而在男性个体中使用不同的 FSH 制剂也获得了相似的结果;这两种制剂在刺激精子发生并最终诱导生理妊娠方面均有效果。促性腺激素可皮下或肌肉内给药。发现 hCG 和 FSH 的联合治疗 12-24 个月可促进几乎所有患者的睾丸生长、约 80%的精子发生和 50%的妊娠率。促性腺激素治疗最常见的副作用是男性乳房发育,这是由于 hCG 刺激芳香化酶导致雌二醇分泌增加所致。青春期后 HH、以前未下降的睾丸、基线睾丸体积较高、接受多次治疗周期和基线抑制素 B 血清浓度较高的患者治疗成功率较高。多达 10%的患者可能会出现低促性腺激素血症逆转,但其病理生理机制尚未阐明。总之,促性腺激素治疗可有效促进青春期和支持下丘脑或垂体病变的 HH 患者精子发生的启动和维持。

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