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The role of the androgen receptor in prostate development and benign prostatic hyperplasia: A review

机译:雄激素受体在前列腺发育和良性前列腺增生中的作用:综述

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Benign prostatic hyperplasia (BPH) is a benign enlargement of the prostate in which incidence increases linearly with age, beginning at about 50 years old. BPH is a significant source of morbidity in aging men by causing lower urinary tract symptoms and acute urinary retention. Unfortunately, the etiology of BPH incidence and progression is not clear. This review highlights the role of the androgen receptor (AR) in prostate development and the evidence for its involvement in BPH. The AR is essential for normal prostate development, and individuals with defective AR signaling, such as after castration, do not experience prostate enlargement with age. Furthermore, decreasing dihydrotestosterone availability through therapeutic targeting with 5α-reductase inhibitors diminishes AR activity and results in reduced prostate size and symptoms in some BPH patients. While there is some evidence that AR expression is elevated in certain cellular compartments, how exactly AR is involved in BPH progression has yet to be elucidated. It is possible that AR signaling within stromal cells alters intercellular signaling and a “reawakening” of the embryonic mesenchyme, loss of epithelial AR leads to changes in paracrine signaling interactions, and/or chronic inflammation aids in stromal or epithelial proliferation evident in BPH. Unfortunately, a subset of patients fails to respond to current medical approaches, forcing surgical treatment even though age or associated co-morbidities make surgery less attractive. Fundamentally, new therapeutic approaches to treat BPH are not currently forthcoming, so a more complete molecular understanding of BPH etiology is necessary to identify new treatment options.
机译:良性前列腺增生(BPH)是前列腺的良性增大,其中发病率随着年龄的年龄而线性增加,从大约50岁开始。 BPH是通过引起尿路症状和急性尿潴留的较低尿路症状和急性尿潴留的衰老患者的重要来源。不幸的是,BPH发病率和进展的病因尚不清楚。本综述突出了雄激素受体(AR)在前列腺发展中的作用以及其参与BPH的证据。 AR至关重要,对于正常的前列腺发育,并且具有缺陷的AR信号传导的个人,例如在阉割之后,不会随着年龄的增长体验前列腺增大。此外,通过用5α-还原酶抑制剂治疗靶向减少二氢酮酮可用性,减少AR活性并导致一些BPH患者的前列腺大小和症状降低。虽然存在一些证据,但在某些细胞室中升高AR表达,尚未阐明AR的涉及BPH进展的恰当。在基质细胞内的AR信号传递改变胚胎间能的细胞间信号传导和“Reawakening”,上皮AR的丧失导致旁节碱信号相互作用的变化,和/或慢性炎症助剂在BPH中明显明显明显。不幸的是,患者的子集未能应对目前的医学方法,迫使手术治疗,即使年龄或相关的共同生命性使手术不那么吸引人。从根本上,目前未来的新治疗方法的治疗BPH,因此对BPH病因的更完整的分子理解是必要的,以确定新的治疗方案。

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