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A New Era of Testosterone and Prostate Cancer: From Physiology to Clinical Implications

机译:睾丸激素和前列腺癌的新时代:从生理学到临床意义

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Context Decades-old beliefs regarding androgens and prostate cancer (PCa) have undergone dramatic shifts in light of modern evidence and new theoretical constructs, but considerable confusion remains on this topic, particularly with regard to the use of testosterone therapy in men with any history of PCa. Objective To review current literature regarding the relationship of serum testosterone on PCa and in particular the effect of testosterone therapy on PCa progression and recurrence. Evidence acquisition A Medline search was conducted to identify all original and review articles assessing the effect of androgens on the prostate and the use of testosterone in men with a history of treated and untreated PCa. Evidence synthesis Contrary to traditional teaching, high endogenous serum testosterone does not increase the risk of developing PCa, and low serum testosterone does not protect against PCa. Although limited in size and duration, current studies similarly fail to indicate any increased risk of PCa in men receiving testosterone therapy. These results indicate a finite ability of androgens to stimulate PCa growth (the saturation model). A majority of studies demonstrate an association between low serum testosterone and poor prognostic features of PCa, including high-grade disease, advanced pathologic stage, and increased risk of biochemical recurrence following radical prostatectomy. The prostate-specific antigen-to-testosterone ratio predicted PCa risk in several biopsy studies. Multiple reports of testosterone therapy in men after treatment for localized PCa have shown low or absent recurrence rates. Some men with untreated PCa have received testosterone therapy without evidence for PCa progression. Conclusions The long-held belief that PCa risk is related to high serum androgen concentrations can no longer be supported. Current evidence indicates that maximal androgen-stimulated PCa growth is achieved at relatively low serum testosterone concentrations. It may therefore be reasonable to consider testosterone therapy in selected men with PCa and symptomatic hypogonadism.
机译:背景根据现代证据和新的理论构建,关于雄激素和前列腺癌(PCa)的几十年的观念已经发生了巨大的变化,但是在这个话题上仍然存在相当多的困惑,特别是在男性睾丸激素治疗史上, PCa。目的回顾有关血清睾丸激素与PCa的关系,特别是睾丸激素治疗对PCa进展和复发的影响的文献。证据采集进行了Medline搜索,以鉴定所有具有PCa治疗和未治疗史的男性,评估雄激素对前列腺的作用以及睾丸激素的使用。证据合成与传统教学相反,高内源性血清睾丸激素不会增加患PCa的风险,而低血清睾丸激素不能预防PCa。尽管其大小和持续时间受到限制,但目前的研究同样未能表明接受睾丸激素治疗的男性PCa风险增加。这些结果表明雄激素刺激PCa生长的能力有限(饱和模型)。大多数研究表明,血清睾丸激素水平低与PCa的不良预后特征之间存在关联,包括高级别疾病,晚期病理分期以及根治性前列腺切除术后生化复发的风险增加。在一些活检研究中,前列腺特异性抗原与睾丸激素的比例预测了PCa的风险。关于局部PCa治疗后男性睾丸激素治疗的多份报告显示,复发率较低或没有。一些未经治疗的PCa男性接受了睾丸激素治疗,但无PCa进展的证据。结论长期以来一直认为PCa风险与血清雄激素水平高有关的信念不再得到支持。当前证据表明,在相对较低的血清睾丸激素浓度下,可以获得最大的雄激素刺激的PCa生长。因此,在某些患有PCa和有症状的性腺功能减退的男性中考虑睾丸激素治疗可能是合理的。

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