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皮肤伤口修复中炎症相关微小RNA的鉴定与功能分析

Identification and functional analysis of inflammation-related miRNAs in skin wound repair.

作者信息

Mori Ryoichi, Tanaka Katsuya, Shimokawa Isao

机构信息

Department of Pathology, Nagasaki University School of Medicine and Graduate School of Biomedical Sciences, Nagasaki, Japan.

Department of Plastic and Reconstructive Surgery, Ehime Prefectural Center Hospital, Matsuyama, Japan.

出版信息

Dev Growth Differ. 2018 Aug;60(6):306-315. doi: 10.1111/dgd.12542. Epub 2018 Jun 5.

DOI:10.1111/dgd.12542
PMID:29873073
Abstract

Inflammation at a wound site is essential for preventing infection. However, misregulated inflammation leads to pathologies of the healing process, including chronic non-healing wounds and scarring. MicroRNAs (miRNAs) are key regulators of the inflammatory response and tissue repair, acting by translational processing of target mRNAs. In the final step of miRNA processing, Argonaute 2 (Ago2)-bound mature miRNA complexes bind to target mRNAs and inhibit their translation. A variety of wound healing-related miRNAs have been identified and their misregulation likely contributes to wound pathologies, including scarring and chronic healing. Recently, we have developed an Ago2-bound mature miRNA purification system that uses Ago2 antibody to analyze the expression of miRNAs from wound tissues by microarray and next generation sequencing. We have identified several wound inflammation-related miRNAs via Ago2-target immunoprecipitation assays and next generation sequencing of wound tissues from wild-type and PU.1 knockout mice, which exhibit no inflammatory response because of a lack of immune cell lineages. We demonstrated that miR-142, an identified inflammation-related miRNA, is essential role for neutrophilic chemotaxis via inhibition of small GTPase translation; its misregulation leads to susceptibility to infection against Staphylococcus aureus at skin wound sites. In this review, we summarize recent advances of miRNA studies in skin wound healing, introduce our miRNA purification system using an immunoprecipitation assay method, and discuss the function of miR-142 in skin wound healing.

摘要

伤口部位的炎症对于预防感染至关重要。然而,炎症调节失调会导致愈合过程出现病理状况,包括慢性不愈合伤口和瘢痕形成。微小RNA(miRNA)是炎症反应和组织修复的关键调节因子,通过对靶mRNA进行翻译加工发挥作用。在miRNA加工的最后一步,与AGO2结合的成熟miRNA复合物与靶mRNA结合并抑制其翻译。已经鉴定出多种与伤口愈合相关的miRNA,其调节失调可能导致伤口病理状况,包括瘢痕形成和慢性愈合。最近,我们开发了一种与AGO2结合的成熟miRNA纯化系统,该系统使用AGO2抗体通过微阵列和下一代测序分析伤口组织中miRNA的表达。我们通过AGO2靶标免疫沉淀试验和对野生型和PU.1基因敲除小鼠伤口组织的下一代测序,鉴定出了几种与伤口炎症相关的miRNA,由于缺乏免疫细胞谱系,PU.1基因敲除小鼠不表现出炎症反应。我们证明,已鉴定出的与炎症相关的miRNA miR-142通过抑制小GTP酶的翻译对中性粒细胞趋化性起关键作用;其调节失调会导致皮肤伤口部位对金黄色葡萄球菌感染易感。在本综述中,我们总结了miRNA在皮肤伤口愈合研究中的最新进展,介绍了我们使用免疫沉淀测定法的miRNA纯化系统,并讨论了miR-142在皮肤伤口愈合中的功能。

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