Sex-specific role of RNA-binding protein, pAUF1, on prolonged hypersensitivity after repetitive ischemia with reperfusion injury.

IF 5.9 1区 医学 Q1 ANESTHESIOLOGY
Meranda M Quijas, Luis F Queme, Samantha T Woodke, Alex A Weyler, Dana Buesing, Ally Butterfield, Diya P Joshi, Irati Mitxelena-Balerdi, Yvonne M Ulrich-Lai, Michael P Jankowski
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Abstract

Abstract: Repetitive ischemia with reperfusion (I/R) injury is a common cause of myalgia. Ischemia with reperfusion injuries occur in many conditions that differentially affect males and females including complex regional pain syndrome and fibromyalgia. Our preclinical studies have indicated that primary afferent sensitization and behavioral hypersensitivity caused by I/R injury may be due to sex-specific gene expression in the dorsal root ganglia (DRG) and distinct upregulation of growth factors and cytokines in the affected muscles. To determine how these unique gene expression programs may be established in a sex-dependent manner in a model that more closely mimics clinical scenarios, we used a developed prolonged ischemic myalgia model in mice whereby animals experience repeated I/R injuries and compared behavioral results with unbiased and targeted screening strategies in male and female DRG. Several distinct proteins were found to be differentially expressed in male and female DRG, including phosphorylated AU-rich element RNA-binding protein (pAUF1), which is known to regulate gene expression. Nerve-specific siRNA-mediated knockdown of AUF1 inhibited prolonged hypersensitivity in females only, whereas overexpression of AUF1 in male DRG neurons increased pain-like responses. AUF1 knockdown was able to specifically inhibit repeated I/R-induced gene expression in females potentially downstream of prolactin receptor signaling. Data suggest RNA-binding proteins such as pAUF1 may underlie the sex-specific effects on DRG gene expression that modulates behavioral hypersensitivity after repeated I/R injury through prolactin signaling. This study may aid in finding distinct receptor differences related to the evolution of acute to chronic ischemic muscle pain development between sexes.

RNA结合蛋白pAUF1对重复性缺血再灌注损伤后长期超敏反应的作用具有性别特异性
摘要:反复缺血再灌注(I/R)损伤是引起肌痛的常见原因。缺血再灌注损伤发生在许多对男性和女性有不同影响的疾病中,包括复杂性区域疼痛综合征和纤维肌痛。我们的临床前研究表明,I/R 损伤引起的原发性传入敏感和行为超敏可能是由于背根神经节(DRG)中的性别特异性基因表达以及受影响肌肉中生长因子和细胞因子的不同上调所致。为了确定这些独特的基因表达程序是如何以性别依赖的方式在一个更接近临床情景的模型中建立起来的,我们使用了一种已开发的小鼠长期缺血性肌痛模型,该模型中的动物会经历反复的 I/R 损伤,并将行为结果与雌雄 DRG 的无偏见和靶向筛选策略进行了比较。研究发现,雌雄DRG中有几种不同的蛋白质表达不同,其中包括磷酸化富含AU元素RNA结合蛋白(pAUF1),该蛋白已知可调控基因表达。神经特异性 siRNA 介导的 AUF1 敲除仅抑制了女性的长期超敏反应,而在男性 DRG 神经元中过表达 AUF1 则会增加疼痛样反应。AUF1 基因敲除能特异性地抑制反复 I/R 诱导的雌性基因表达,这可能是催乳素受体信号转导的下游作用。数据表明,RNA结合蛋白(如pAUF1)可能是DRG基因表达的性别特异性效应的基础,这种效应通过催乳素信号调节反复I/R损伤后的行为超敏性。这项研究可能有助于发现与急性到慢性缺血性肌肉疼痛发展演变有关的性别间独特的受体差异。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
PAIN®
PAIN® 医学-临床神经学
CiteScore
12.50
自引率
8.10%
发文量
242
审稿时长
9 months
期刊介绍: PAIN® is the official publication of the International Association for the Study of Pain and publishes original research on the nature,mechanisms and treatment of pain.PAIN® provides a forum for the dissemination of research in the basic and clinical sciences of multidisciplinary interest.
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