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miR-30b 在白细胞介素-21 受体介导的实验性外周动脉疾病中的血管生成中既是必需的又是充分的。

MicroRNA-30b Is Both Necessary and Sufficient for Interleukin-21 Receptor-Mediated Angiogenesis in Experimental Peripheral Arterial Disease.

机构信息

State Key Laboratory of Respiratory Diseases, Guangzhou Institute of Respiratory Health, Guangzhou Medical University, Guangzhou 510120, China.

Robert M Berne Cardiovascular Research Center, University of Virginia, Charlottesville, VA 22908, USA.

出版信息

Int J Mol Sci. 2021 Dec 27;23(1):271. doi: 10.3390/ijms23010271.

DOI:10.3390/ijms23010271
PMID:35008699
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8745227/
Abstract

The interleukin-21 receptor (IL-21R) can be upregulated in endothelial cells (EC) from ischemic muscles in mice following hind-limb ischemia (HLI), an experimental peripheral arterial disease (PAD) model, blocking this ligand-receptor pathway-impaired STAT3 activation, angiogenesis, and perfusion recovery. We sought to identify mRNA and microRNA transcripts that were differentially regulated following HLI, based on the ischemic muscle having intact, or reduced, IL-21/IL21R signaling. In this comparison, 200 mRNAs were differentially expressed but only six microRNA (miR)/miR clusters (and among these only miR-30b) were upregulated in EC isolated from ischemic muscle. Next, myoglobin-overexpressing transgenic (MgTG) C57BL/6 mice examined following HLI and IL-21 overexpression displayed greater angiogenesis, better perfusion recovery, and less tissue necrosis, with increased miR-30b expression. In EC cultured under hypoxia serum starvation, knock-down of miR-30b reduced, while overexpression of miR-30b increased IL-21-mediated EC survival and angiogenesis. In Il21r mice following HLI, miR-30b overexpression vs. control improved perfusion recovery, with a reduction of suppressor of cytokine signaling 3, a miR-30b target and negative regulator of STAT3. Together, miR-30b appears both necessary and sufficient for IL21/IL-21R-mediated angiogenesis and may present a new therapeutic option to treat PAD if the IL21R is not available for activation.

摘要

白细胞介素 21 受体 (IL-21R) 在小鼠后肢缺血 (HLI) 后缺血肌肉中的内皮细胞 (EC) 中上调,HLI 是一种实验性外周动脉疾病 (PAD) 模型,阻断该配体-受体途径可损害 STAT3 激活、血管生成和灌注恢复。我们试图根据缺血肌肉中是否存在完整或减少的 IL-21/IL21R 信号,确定 HLI 后差异调节的 mRNA 和 microRNA 转录本。在这种比较中,200 个 mRNAs 表达差异,但仅在从缺血肌肉中分离的 EC 中上调了 6 个 microRNA (miR)/miR 簇(其中只有 miR-30b)。接下来,在 HLI 和 IL-21 过表达后检查过表达肌红蛋白的转基因 (MgTG) C57BL/6 小鼠,显示出更多的血管生成、更好的灌注恢复和更少的组织坏死,同时 miR-30b 表达增加。在缺氧血清饥饿培养的 EC 中,miR-30b 的敲低降低了,而 miR-30b 的过表达增加了 IL-21 介导的 EC 存活和血管生成。在 HLI 后的 Il21r 小鼠中,与对照相比,miR-30b 的过表达改善了灌注恢复,同时降低了细胞因子信号转导抑制因子 3 的表达,miR-30b 的一个靶标和 STAT3 的负调节剂。总之,miR-30b 似乎是 IL21/IL-21R 介导的血管生成所必需和充分的,如果 IL21R 无法激活,则可能为治疗 PAD 提供一种新的治疗选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dca7/8745227/4dfcd49187fc/ijms-23-00271-g007.jpg
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