MicroRNA-210通过靶向线粒体生物能和mtROS通量介导缺氧诱导的肺动脉高压。

IF 5.6 2区 医学 Q1 PHYSIOLOGY
Abu Shufian Ishtiaq Ahmed, Arlin B. Blood, Lubo Zhang
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引用次数: 0

摘要

目的:慢性缺氧是肺动脉高压(PH)的常见原因。我们检验了微RNA-210(miR-210)通过靶向线粒体代谢和增加肺部活性氧(mtROS)产生来介导缺氧诱导的肺动脉高压的假说:成年野生型(WT)或 miR-210 基因敲除(KO)小鼠暴露于低氧(10.5% O2)或常氧环境 4 周。我们测量了 miR-210 水平、右心室收缩压(RVSP)以及心肺组织的组织学变化。在分离的肺线粒体中评估了线粒体生物能和mtROS的产生:结果:缺氧会增加 WT 小鼠的右心室壁厚度和肺血管壁肌肉化,但不会增加 miR-210 KO 小鼠的右心室壁厚度和肺血管壁肌肉化。没有观察到性别差异。在雄性小鼠中,缺氧会增加肺部和 RVSP 中的 miR-210 水平,而 miR-210 缺乏则会使这种情况消失。缺氧会上调线粒体耗氧率和mtROS通量,而在miR-210 KO小鼠中这一作用被抵消。此外,慢性缺氧会增加 WT 小鼠肺中巨噬细胞的积累,而 miR-210 KO 小鼠则不会。此外,miR-210 在 WT 动物肺中的过表达再现了缺氧的影响,并增加了线粒体耗氧率、mtROS 通量、右心室壁厚度、肺血管壁肌肉化和 RVSP。MitoQ抑制了miR-210对肺线粒体生物能、右心室和肺血管重塑以及RVSP的影响:我们采用功能缺失和功能增益方法的研究结果提供了明确的证据,证明 miR-210 在小鼠模型中通过上调线粒体生物能和 mtROS 的产生来介导缺氧诱导的 PH,揭示了治疗 PH 的机制和治疗靶点的新见解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
MicroRNA-210 mediates hypoxia-induced pulmonary hypertension by targeting mitochondrial bioenergetics and mtROS flux

Aim

Chronic hypoxia is a common cause of pulmonary hypertension (PH). We test the hypothesis that microRNA-210 (miR-210) mediates hypoxia-induced PH by targeting mitochondrial metabolism and increasing reactive oxygen species (mtROS) production in the lungs.

Methods

Adult wildtype (WT) or miR-210 knockout (KO) mice were exposed to hypoxia (10.5% O2) or normoxia for 4 weeks. We measured miR-210 levels, right ventricular systolic pressure (RVSP), and histological changes in heart and lung tissues. Mitochondrial bioenergetics and mtROS production were assessed in isolated lung mitochondria.

Results

Hypoxia increased right ventricular wall thickness and pulmonary vessel wall muscularization in WT, but not miR-210 KO mice. No sex differences were observed. In male mice, hypoxia increased miR-210 levels in the lung and RVSP, which were abrogated by miR-210 deficiency. Hypoxia upregulated mitochondrial oxygen consumption rate and mtROS flux, which were negated in miR-210 KO animals. In addition, chronic hypoxia increased macrophage accumulation in lungs of WT, but not miR-210 KO mice. Moreover, miR-210 overexpression in lungs of WT animals recapitulated the effects of hypoxia and increased mitochondrial oxygen consumption rate, mtROS flux, right ventricular wall thickness, pulmonary vessel wall muscularization and RVSP. MitoQ revoked the effects of miR-210 on lung mitochondrial bioenergetics, right ventricular and pulmonary vessel remodeling and RVSP.

Conclusion

Our findings with loss-of-function and gain-of-function approaches provide explicit evidence that miR-210 mediates hypoxia-induced PH by upregulating mitochondrial bioenergetics and mtROS production in a murine model, revealing new insights into the mechanisms and therapeutic targets for treatment of PH.

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来源期刊
Acta Physiologica
Acta Physiologica 医学-生理学
CiteScore
11.80
自引率
15.90%
发文量
182
审稿时长
4-8 weeks
期刊介绍: Acta Physiologica is an important forum for the publication of high quality original research in physiology and related areas by authors from all over the world. Acta Physiologica is a leading journal in human/translational physiology while promoting all aspects of the science of physiology. The journal publishes full length original articles on important new observations as well as reviews and commentaries.
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