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真皮白色脂肪组织(dWAT)在皮肤伤口愈合的早期阶段受 Foxn1 和 Hif-1α 的调控。

Dermal White Adipose Tissue (dWAT) Is Regulated by Foxn1 and Hif-1α during the Early Phase of Skin Wound Healing.

机构信息

Institute of Animal Reproduction and Food Research, Polish Academy of Sciences, 10-748 Olsztyn, Poland.

Virus Vector Core, Turku Centre for Biotechnology BioCity, 20520 Turku, Finland.

出版信息

Int J Mol Sci. 2021 Dec 27;23(1):257. doi: 10.3390/ijms23010257.

DOI:10.3390/ijms23010257
PMID:35008683
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8745105/
Abstract

Dermal white adipose tissue (dWAT) is involved in the maintenance of skin homeostasis. However, the studies concerning its molecular regulation are limited. In the present paper, we ask whether the introduction of two transcription factors, Foxn1 and Hif-1α, into the post-wounded skin of Foxn1 mice regulates dWAT during wound healing (days 3 and 6). We have chosen lentivirus vectors (LVs) as a tool to deliver Foxn1 and Hif-1α into the post-wounded skin. We documented that combinations of both transgenes reduces the number, size and diameter of dermal adipocytes at the wound bed area. The qRT-PCR analysis of pro-adipogenic genes, revealed that LV-Hif-1α alone, or combined with LV-Foxn1, increases the mRNA expression of , and at post-wounding day 6. However, the most spectacular stimulatory effect of Foxn1 and/or Hif-1α was observed for Igf2, the growth factor participating in adipogenic signal transduction. Our data also shows that Foxn1/Hif-1α, at post-wounding day 3, reduces levels of and mRNA expression and the percentage of CD68 positive cells in the wound site. In conclusion, the present data are the first to document that Foxn1 and Hif-1α cooperatively (1) regulate dWAT during the proliferative phase of skin wound healing through the Igf2 signaling pathway, and (2) reduce the macrophages content in the wound site.

摘要

真皮白色脂肪组织(dWAT)参与维持皮肤稳态。然而,其分子调节的研究有限。在本文中,我们询问在 Foxn1 小鼠受伤后的皮肤中引入两个转录因子 Foxn1 和 Hif-1α 是否会在伤口愈合期间(第 3 天和第 6 天)调节 dWAT。我们选择慢病毒载体(LVs)作为将 Foxn1 和 Hif-1α 递送至受伤后皮肤的工具。我们记录到,两种转基因的组合减少了伤口床区域真皮脂肪细胞的数量、大小和直径。对前脂肪生成基因的 qRT-PCR 分析显示,LV-Hif-1α 单独或与 LV-Foxn1 联合使用,在受伤后第 6 天增加了 、 和 的 mRNA 表达。然而,Foxn1 和/或 Hif-1α 对 Igf2 的最显著刺激作用最大,Igf2 是参与脂肪生成信号转导的生长因子。我们的数据还表明,Foxn1/Hif-1α 在受伤后第 3 天减少了 和 mRNA 表达水平以及伤口部位 CD68 阳性细胞的百分比。总之,本研究数据首次记录到 Foxn1 和 Hif-1α 通过 Igf2 信号通路在皮肤伤口愈合的增殖期协同(1)调节 dWAT,(2)减少伤口部位的巨噬细胞含量。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f808/8745105/e657139cd194/ijms-23-00257-g008.jpg
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