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Sonic hedgehog, the penis and erectile dysfunction: a review of sonic hedgehog signaling in the penis.

机译:声波刺猬,阴茎和勃起功能障碍:阴茎中的声波刺猬信号综述。

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摘要

The sinusoid anatomy of the penis is complex and requires complicated interaction between smooth muscle and endothelium in order to maintain homeostasis in the adult. The morphogen, Sonic hedgehog (Shh), is a crucial regulator of these processes, along with its down stream targets patched (Ptc), Hox, bone morphogenetic proteins (BMP's), vascular endothelial growth factor (VEGF) and nitric oxide synthase (NOS). Shh is critical for patterning and establishing tissue identity of the penis during embryonic development, is a crucial regulator of penile postnatal differentiation of the sinusoid morphology of the corpora cavernosa, and plays a fundamental role in maintaining sinusoidal structures pertinent to erectile function in the adult rat. Shh and its targets are active in human penes, and decreased in human diabetic penes in parallel with observations in the rat, thus lending clinical significance to the role of abnormal Shh signaling in erectile dysfunction (ED). Application of exogenous Shh protein to rat corpora cavernosa, induces VEGF and NOS proteins, suggesting a potential mechanism through which decreased Shh protein can cause ED. The studies outlined in this review provide in depth analysis of the Shh pathway and signal transduction, its role in penile development, how Shh signaling is altered in a rat model of ED and neuropathy, how abnormal Shh signaling can cause ED, and the clinical significance of the Shh pathway to human ED. These studies will provide valuable insight, at the molecular level, into understanding the mechanisms that under lie ED and lead to new treatment strategies for diabetic impotence.
机译:阴茎的正弦解剖结构很复杂,需要平滑肌和内皮之间复杂的相互作用才能维持成人的体内平衡。形态发生子Sonic刺猬(Shh)是这些过程的关键调节剂,其下游靶标有斑块(Ptc),Hox,骨形态发生蛋白(BMP),血管内皮生长因子(VEGF)和一氧化氮合酶(NOS) )。 Shh在胚胎发育过程中对阴茎的形态和建立阴茎的组织特性至关重要,是阴茎海绵体形态的阴茎产后分化的关键调节剂,并且在维持与成年大鼠勃起功能相关的正弦结构中起着基本作用。 Shh及其靶标在人的笔中活跃,在人的糖尿病人笔中减少,与在大鼠中观察到的结果平行,因此对异常的Shh信号在勃起功能障碍(ED)中的作用具有临床意义。外源性Shh蛋白应用于大鼠海绵体可诱导VEGF和NOS蛋白,提示减少的Shh蛋白可引起ED的潜在机制。这篇综述中概述的研究提供了Shh途径和信号转导的深入分析,其在阴茎发育中的作用,在ED和神经病大鼠模型中Shh信号如何改变,异常的Shh信号如何导致ED以及临床意义到人类ED的Shh途径。这些研究将在分子水平上提供宝贵的见识,以了解ED背后的机制并导致新的糖尿病性阳to治疗策略。

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