Depletion of Gsdma1/2/3 alleviates PMA-induced epidermal hyperplasia by inhibiting the EGFR-Stat3/Akt pathway.

IF 5.3 2区 生物学 Q2 CELL BIOLOGY
Qiyao Liu, Manyun Li, Minli Sun, Ruyue Xin, Yushu Wang, Qin Chen, Xiang Gao, Zhaoyu Lin
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Abstract

Homeostasis of the skin barrier is essential for maintaining normal skin function. Gasdermin A (GSDMA) is highly expressed in the skin and associated with many skin diseases, such as melanoma and psoriasis. In mice, GSDMA is encoded by three gene homologues, namely Gsdma1, Gsdma2, and Gsdma3. Although Gsdma3 gain-of-function mutations cause hair loss and skin inflammation, Gsdma3-deficient mice do not show any visible phenotypes in skin and hair structures. To explore the physiological function of GSDMA, we generated conventional Gsdma1/2/3 knockout (KO) mice. These mice showed significantly alleviated epidermal hyperplasia and inflammation induced by phorbol 12-myristate 13-acetate (PMA). Furthermore, the alleviation of epidermal hyperplasia depended on the expression of Gsdma1/2/3 specifically in keratinocytes. Mechanistically, Gsdma1/2/3 depletion downregulated epidermal growth factor receptor (EGFR) ligands, leading to the decreased EGFR-Stat3/Akt signalling. These results demonstrate that depletion of Gsdma1/2/3 alleviates PMA-induced epidermal hyperplasia partially by inhibiting the EGFR-Stat3/Akt pathway.

通过抑制表皮生长因子受体-Stat3/Akt通路,消耗Gsdma1/2/3可减轻PMA诱导的表皮增生。
皮肤屏障的平衡对维持皮肤的正常功能至关重要。Gasdermin A(GSDMA)在皮肤中高度表达,与许多皮肤病有关,如黑色素瘤和银屑病。在小鼠体内,GSDMA 由三个同源基因编码,即 Gsdma1、Gsdma2 和 Gsdma3。虽然 Gsdma3 功能增益突变会导致脱毛和皮肤炎症,但 Gsdma3 缺失的小鼠在皮肤或毛发结构上没有表现出任何表型。为了探索 GSDMA 的生理功能,我们产生了传统的 Gsdma1/2/3 基因敲除(KO)小鼠。我们发现,Gsdma1/2/3 KO 小鼠的表皮增生和光甘油 12-肉豆蔻酸 13-乙酸酯(PMA)诱导的炎症明显减少。此外,我们还发现表皮增生的缓解取决于特异性表达于角质形成细胞中的 Gsdma1/2/3。从机制上讲,Gsdma1/2/3 的消耗会下调表皮生长因子受体(EGFR)配体,从而导致 EGFR-Stat3/Akt 信号的减少。这些结果表明,通过抑制表皮生长因子受体-Stat3/Akt通路,消耗Gsdma1/2/3可部分缓解PMA诱导的表皮增生。
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来源期刊
CiteScore
9.60
自引率
1.80%
发文量
1383
期刊介绍: The Journal of Molecular Cell Biology ( JMCB ) is a full open access, peer-reviewed online journal interested in inter-disciplinary studies at the cross-sections between molecular and cell biology as well as other disciplines of life sciences. The broad scope of JMCB reflects the merging of these life science disciplines such as stem cell research, signaling, genetics, epigenetics, genomics, development, immunology, cancer biology, molecular pathogenesis, neuroscience, and systems biology. The journal will publish primary research papers with findings of unusual significance and broad scientific interest. Review articles, letters and commentary on timely issues are also welcome. JMCB features an outstanding Editorial Board, which will serve as scientific advisors to the journal and provide strategic guidance for the development of the journal. By selecting only the best papers for publication, JMCB will provide a first rate publishing forum for scientists all over the world.
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