脱敏(药物)
支持细胞
过度活跃
受体
调解人
去甲肾上腺素
封锁
细胞生物学
信号转导
内分泌学
分泌物
生物
内科学
普萘洛尔
细胞
细胞信号
同源性脱敏
生殖系统
睾酮(贴片)
旁观者效应
交感神经系统
激素
神经递质
作者
Lingyu Zhang,Shanfeng Gao,Xiaofan Xiong,Xin Liu,Rufeng Li,Xia Wang,Lin Han,Xuan Xiao,Xiaofei Wang,Wen Li,Yongxia Chang,Yuefeng Du,Juan Yang
标识
DOI:10.1002/advs.202504817
摘要
Abstract Psychological stress poses a significant threat to male reproduction; however, the underlying molecular mechanisms remain poorly understood. Stress‐induced hyperactivation of the sympathetic nervous system triggers the secretion of norepinephrine (NE), a key mediator implicated in various pathophysiological processes. Although NE is linked to male reproductive dysfunction, the precise mechanism remains unclear. Here, it is demonstrated that psychological stress can induce Sertoli cell ferroptosis through NE, which is characterized by iron overload, lipid peroxidation, and altered expression of ferroptosis‐related proteins. Blockade of β‐adrenergic receptors (β‐ARs) with propranolol alleviated stress‐induced damage, inhibiting ferroptosis and promoting spermatogenesis. In vitro, selective β 1 ‐ and β 2 ‐AR antagonists reversed NE‐induced Sertoli cell ferroptosis. Mechanistically, NE activated β‐arrestin1, driving β‐ARs desensitization and internalization, which subsequently stimulated inhibitory G proteins (Gi), suppressed CREB1‐dependent GPX4 transcription, and promoted ferroptosis. The findings reveal NE‐induced β‐ARs desensitization as a mechanistic driver of Sertoli cell ferroptosis. β‐ARs signaling modulation is proposed as a potential therapeutic approach for alleviating stress‐associated male reproductive impairment.
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