| Literature DB >> 29605672 |
Jianyun Shi1, Xianghui Ma1, Yang Su1, Yongli Song1, Yuhua Tian1, Shukai Yuan2, Xiuqing Zhang3, Dong Yang3, Hao Zhang4, Jianwei Shuai5, Wei Cui6, Fazheng Ren4, Maksim V Plikus7, Yaoxing Chen8, Jie Luo9, Zhengquan Yu10.
Abstract
Wound healing is essential for skin repair after injury, and it consists of hemostasis, inflammation, re-epithelialization, and remodeling phases. Successful re-epithelialization, which relies on proliferation and migration of epidermal keratinocytes, requires a reduction in tissue inflammation. Therefore, understanding the molecular mechanism underlying the transition from inflammation to re-epithelialization will help to better understand the principles of wound healing. Currently, the in vivo functions of specific microRNAs in wound healing are not fully understood. We observed that miR-31 expression is strongly induced in wound edge keratinocytes, and is directly regulated by the activity of NF-κB and signal transducer and activator of transcription 3 signaling pathways during the inflammation phase. We used miR-31 loss-of-function mouse models to demonstrate that miR-31 promotes keratinocyte proliferation and migration. Mechanistically, miR-31 activates the Ras/mitogen-activated protein kinase signaling by directly targeting Rasa1, Spred1, Spred2, and Spry4, which are negative regulators of the Ras/mitogen-activated protein kinase pathway. Knockdown of these miR-31 targets at least partially rescues the delayed scratch wound re-epithelialization phenotype observed in vitro in miR-31 knockdown keratinocytes. Taken together, these findings identify miR-31 as an important cell-autonomous mediator during the transition from inflammation to re-epithelialization phases of wound healing, suggesting a therapeutic potential for miR-31 in skin injury repair.Entities:
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Year: 2018 PMID: 29605672 PMCID: PMC6153075 DOI: 10.1016/j.jid.2018.03.1521
Source DB: PubMed Journal: J Invest Dermatol ISSN: 0022-202X Impact factor: 8.551