Mechanism of denervation muscle atrophy mediated by Ach/p38/MAPK pathway in rats with erectile dysfunction caused by nerve injury

IF 3.3 3区 生物学 Q3 CELL BIOLOGY Experimental cell research Pub Date : 2024-10-01 DOI:10.1016/j.yexcr.2024.114283
Huang wen Jie , Wang Jie , Ma Jianxiong , Zhang Xin , Xu Runnan , Fu Yijia , Lv Bodong , Huang jie
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Abstract

Background

Peripheral nerve injury can result in penile cavernosal denervation muscle atrophy, a primary factor in nerve injury erectile dysfunction (NED). While acetylcholine (Ach) is integral to erectile function, its role and mechanisms in NED need further exploration.

Objective

To investigate the inhibition of CCMSCs Apoptosis and Protein Degradation Pathway by Ach in NED rat model.

Methods

We investigated changes in Ach secretion and receptor expression in an NED rat model, followed by the evaluation of apoptosis and ubiquitin proteasome activation in hypoxic Cavernous smooth muscle cells (CCMSCs) and their co-cultures with Schwann cells (SWCs), under Ach influence. Further, key pathways in NED were identified via high-throughput sequencing, focusing on the p38/MAPK signaling pathway. We examined gene alterations related to this pathway using hypoxic cell models and employed p38 inhibitors to verify protein changes. Our findings in vitro were then confirmed in the NED rat model.

Results

Nerve injury led to reduced Ach receptors and associated gene expression. Experimentally, Ach was shown to counteract CCMSC apoptosis and muscle protein degradation via the p38/MAPK pathway. Inhibition of the Ach degradation pathway demonstrated a capacity to slow NED progression in vivo.

Discussion and conclusion

Activation of Ach receptors may decelerate denervation-induced cavernosal muscle atrophy, suggesting a potential therapeutic approach for NED. This study highlights the crucial role of the Ach/p38/MAPK axis in the pathophysiology of penis smooth muscle atrophy and its broader implications in managing NED and male erectile dysfunction.
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神经损伤导致勃起功能障碍的大鼠在 Ach/p38/MAPK 通路介导下发生神经支配肌肉萎缩的机制
背景周围神经损伤可导致阴茎海绵体神经支配肌肉萎缩,这是神经损伤性勃起功能障碍(NED)的主要因素。尽管乙酰胆碱(Ach)是勃起功能不可或缺的物质,但它在 NED 中的作用和机制仍需进一步探讨。目的研究 Ach 对 NED 大鼠模型中阴茎海绵体肌细胞凋亡和蛋白降解途径的抑制作用。方法我们研究了 NED 大鼠模型中 Ach 分泌和受体表达的变化,然后评估了缺氧海绵平滑肌细胞(CCMSCs)及其与许旺细胞(SWCs)共培养物在 Ach 影响下的凋亡和泛素蛋白酶体激活情况。此外,通过高通量测序确定了 NED 的关键通路,重点是 p38/MAPK 信号通路。我们利用缺氧细胞模型检查了与该通路相关的基因变化,并使用 p38 抑制剂来验证蛋白质变化。结果神经损伤导致 Ach 受体和相关基因表达减少。实验表明,Ach 可通过 p38/MAPK 通路抵消 CCMSC 的凋亡和肌肉蛋白降解。讨论与结论激活 Ach 受体可能会减缓神经支配诱导的海绵体肌萎缩,从而为 NED 提供了一种潜在的治疗方法。这项研究强调了 Ach/p38/MAPK 轴在阴茎平滑肌萎缩的病理生理学中的关键作用,以及它对治疗 NED 和男性勃起功能障碍的广泛影响。
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来源期刊
Experimental cell research
Experimental cell research 医学-细胞生物学
CiteScore
7.20
自引率
0.00%
发文量
295
审稿时长
30 days
期刊介绍: Our scope includes but is not limited to areas such as: Chromosome biology; Chromatin and epigenetics; DNA repair; Gene regulation; Nuclear import-export; RNA processing; Non-coding RNAs; Organelle biology; The cytoskeleton; Intracellular trafficking; Cell-cell and cell-matrix interactions; Cell motility and migration; Cell proliferation; Cellular differentiation; Signal transduction; Programmed cell death.
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