| Literature DB >> 35347234 |
Yang Zheng1,2, Feng Jiang1,3,4, Chao Wang1,3,4, Mengjie Dong1,3,4, Chundi Wang1,5, Enshi Yan6, Yi Wang1,3,4, Zaiou Zhu1,3,4, Xianbin Xiong1,3,4, Xu Ding1,3,4, Jinhai Ye1,3,4, Yue He2, Hongchuang Zhang7, Junbo Zhou8, Wei Zhang9,10, Yunong Wu11,12,13, Xiaomeng Song14,15,16.
Abstract
Semaphorin 3A (Sema3A) has been recognized as a crucial regulator of morphogenesis and homeostasis over a wide range of organ systems. However, its function in cutaneous wound healing is poorly understood. In our study, we demonstrated that Sema3A adenovirus plasmids transfection limited keratinocyte proliferation and decreased migrative capacity as assessed by in vitro wound healing assay. Sema3A transduction inhibited TGF-β1-mediated keratinocyte migration and EMT process. Besides, we applied mice with K14-Cre-mediated deletion of Sema3A and found that Sema3A depletion postponed wound closure with decreased re-epithelialization and matrix growth. Contrary to the results obtained with full-length Sema3A plasmids transfection, increased keratinocyte migration with recombinant Sema3A proteins resulted in quicker closure of the wounding area after a scratch. Further, exogenously applied recombinant Sema3A worked with EGF to maintain the activation of EGFR by interacting with NRP1 and thereby regulated the internalization of the EGFR-NRP1 complex. Taken together, these results indicated a paradoxical role of autonomous and non-autonomous Sema3A expression during wound healing. Combined administration of recombinant EGF and Sema3A proteins could accelerate the process of wound repair, thus providing promising treatment prospects in the future.Entities:
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Year: 2022 PMID: 35347234 PMCID: PMC9525670 DOI: 10.1038/s41418-022-00981-6
Source DB: PubMed Journal: Cell Death Differ ISSN: 1350-9047 Impact factor: 12.067