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The role of hedgehog-interacting protein in maintaining cavernous nerve integrity and adult penile morphology.

机译:刺猬蛋白相互作用蛋白在维持海绵状神经完整性和成年阴茎形态中的作用。

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INTRODUCTION: Sonic hedgehog (SHH) is an essential regulator of smooth muscle apoptosis in the penis that has significant clinical potential as a therapy to suppress post-prostatectomy apoptosis, an underlying cause of erectile dysfunction (ED). Thus an understanding of how SHH signaling is regulated in the adult penis is essential to move the field of ED research forward and to develop new treatment strategies. We propose that hedgehog-interacting protein (HIP), which has been shown to bind SHH protein and to play a role in SHH regulation during embryogenesis of other organs, is a critical regulator of SHH signaling, penile morphology, and apoptosis induction. AIMS: We have examined HIP signaling in the penis and cavernous nerve (CN) during postnatal differentiation of the penis, in CN-injured, and a diabetic model of ED. METHODS: HIP localization/abundance and RNA abundance were examined by immunohistochemical (IHC) analysis and real-time reverse transcriptase-polymerase chain reaction (RT-PCR) in Sprague-Dawley rats between the ages of 7 and 92 days old, in CN-injured Sprague-Dawley rats and in BioBreeding/Worcester diabetic rats. HIP signaling was perturbed in the pelvic ganglia and in the penis and TUNEL assay was performed in the penis. CN tie, lidocaine, and anti-kinesin experiments were performed to examine HIP signaling in the CN and penis. RESULTS: In this study we are the first to demonstrate that HIP undergoes anterograde transport to the penis via the CN, that HIP perturbation in the pelvic ganglia or the penis induces apoptosis, and that HIP plays a role in maintaining CN integrity, penile morphology, and SHH abundance. CONCLUSIONS: These studies are significant because they show HIP involvement in cross-talk (signaling) between the pelvic ganglia and penis, which is integral for maintenance of penile morphology and they suggest a mechanism of how nerves may regulate target organ morphology and function.
机译:简介:刺猬(SHH)是阴茎中平滑肌细胞凋亡的重要调节剂,作为抑制前列腺切除术后细胞凋亡(一种勃起功能障碍(ED)的潜在原因)的疗法具有重要的临床潜力。因此,了解如何在成年阴茎中调节SHH信号对于推进ED研究领域并开发新的治疗策略至关重要。我们提出,已证明结合SHH蛋白并在其他器官的胚胎发生过程中在SHH调节中发挥作用的刺猬相互作用蛋白(HIP)是SHH信号,阴茎形态和凋亡诱导的关键调节剂。目的:我们研究了在阴茎产后分化,CN损伤和ED的糖尿病模型中,阴茎和海绵状神经(CN)中的HIP信号传导。方法:采用免疫组织化学(IHC)分析和实时逆转录酶-聚合酶链反应(RT-PCR)方法,对CN-中7至92天大的Sprague-Dawley大鼠进行了HIP定位/丰度和RNA丰度检测。受伤的Sprague-Dawley大鼠和BioBreeding / Worcester糖尿病大鼠。 HIP信号在骨盆神经节和阴茎中受到干扰,TUNEL分析在阴茎中进行。进行CN领带,利多卡因和抗驱动蛋白实验,以检查CN和阴茎中的HIP信号传导。结果:在这项研究中,我们是第一个证明HIP通过CN进行顺行转运到阴茎,HIP扰动骨盆神经节或阴茎引起细胞凋亡,并且HIP在维持CN完整性,阴茎形态,和SHH丰富。结论:这些研究具有重要意义,因为它们表明HIP参与了骨盆神经节和阴茎之间的串扰(信号传导),这对维持阴茎形态必不可少,并且它们提示了神经如何调节靶器官形态和功能的机制。

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