Opioids Cause Sex-Specific Vascular Changes via Cofilin-Extracellular Signal-Regulated Kinase Signaling: Female Mice Present Higher Risk of Developing Morphine-Induced Vascular Dysfunction than Male Mice.

IF 1.8 4区 医学 Q3 PERIPHERAL VASCULAR DISEASE
Journal of Vascular Research Pub Date : 2021-01-01 Epub Date: 2021-09-14 DOI:10.1159/000517555
Soyoung Cheon, Jeremy C Tomcho, Jonnelle M Edwards, Nicole R Bearss, Emily Waigi, Bina Joe, Cameron G McCarthy, Camilla F Wenceslau
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引用次数: 0

Abstract

Recent studies have shown that chronic use of prescription or illicit opioids leads to an increased risk of cardiovascular events and pulmonary arterial hypertension. Indices of vascular age and arterial stiffness are also shown to be increased in opioid-dependent patients, with the effects being more marked in women. There are currently no studies investigating sex-specific vascular dysfunction in opioid use, and the mechanisms leading to opioid-induced vascular damage remain unknown. We hypothesized that exposure to exogenous opioids causes sex-specific vascular remodeling that will be more pronounced in female. Acknowledging the emerging roles of cofilins and extracellular signal-regulated kinases (ERKs) in mediating actin dynamics, we investigated the effects of morphine on these molecules. Twenty-four hour exposure to morphine increased inactivated cofilin and activated ERKs in resistance arteries from female mice, which may promote stress fiber over-assembly. We also performed continuous intraluminal infusion of morphine in pressurized resistance arteries from male and female mice using culture pressure myographs. We observed that morphine reduced the vascular diameter in resistance arteries from female, but not male mice. These results have significant implications for the previously unexplored role of exogenous opioids as a modifiable cardiovascular risk factor, especially in women.

阿片类药物通过Cofilin-细胞外信号调节激酶信号传导导致血管发生性别特异性变化:与雄性小鼠相比,雌性小鼠出现吗啡诱导的血管功能障碍的风险更高。
最近的研究表明,长期使用处方或非法阿片类药物会导致心血管事件和肺动脉高压的风险增加。研究还显示,阿片类药物依赖患者的血管年龄和动脉僵化指数也会增加,女性受影响更为明显。目前还没有研究调查使用阿片类药物时血管功能障碍的性别特异性,导致阿片类药物诱发血管损伤的机制仍然未知。我们假设,暴露于外源性阿片类药物会导致性别特异性血管重塑,而这种重塑在女性中更为明显。鉴于共纤蛋白和细胞外信号调节激酶(ERKs)在介导肌动蛋白动力学中的新作用,我们研究了吗啡对这些分子的影响。在雌性小鼠的阻力动脉中,暴露于吗啡24小时会增加失活的cofilin和激活的ERKs,这可能会促进应力纤维的过度组装。我们还使用培养压力肌电图对雄性和雌性小鼠的加压阻力动脉进行了吗啡连续腔内输注。我们观察到吗啡降低了雌性小鼠阻力动脉的血管直径,而雄性小鼠则没有。这些结果对以前未曾探索过的外源性阿片类药物作为一种可调节的心血管风险因素具有重要意义,尤其是对女性而言。
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来源期刊
Journal of Vascular Research
Journal of Vascular Research 医学-生理学
CiteScore
3.40
自引率
0.00%
发文量
25
审稿时长
>12 weeks
期刊介绍: The ''Journal of Vascular Research'' publishes original articles and reviews of scientific excellence in vascular and microvascular biology, physiology and pathophysiology. The scope of the journal covers a broad spectrum of vascular and lymphatic research, including vascular structure, vascular function, haemodynamics, mechanics, cell signalling, intercellular communication, growth and differentiation. JVR''s ''Vascular Update'' series regularly presents state-of-the-art reviews on hot topics in vascular biology. Manuscript processing times are, consistent with stringent review, kept as short as possible due to electronic submission. All articles are published online first, ensuring rapid publication. The ''Journal of Vascular Research'' is the official journal of the European Society for Microcirculation. A biennial prize is awarded to the authors of the best paper published in the journal over the previous two years, thus encouraging young scientists working in the exciting field of vascular biology to publish their findings.
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