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美伐他汀通过靶向窖蛋白-1来促进愈合,从而恢复 EGFR 信号。

Mevastatin promotes healing by targeting caveolin-1 to restore EGFR signaling.

机构信息

Wound Healing and Regenerative Medicine Research Program, Dr. Phillip Frost Department of Dermatology and Cutaneous Surgery, and.

Molecular and Cellular Pharmacology Graduate Program in Biomedical Sciences, University of Miami Miller School of Medicine, Miami, Florida, USA.

出版信息

JCI Insight. 2019 Dec 5;4(23):129320. doi: 10.1172/jci.insight.129320.

Abstract

Diabetic foot ulcers (DFUs) are a life-threatening disease that often results in lower limb amputations and a shortened life span. Current treatment options are limited and often not efficacious, raising the need for new therapies. To investigate the therapeutic potential of topical statins to restore healing in patients with DFUs, we performed next-generation sequencing on mevastatin-treated primary human keratinocytes. We found that mevastatin activated and modulated the EGF signaling to trigger an antiproliferative and promigratory phenotype, suggesting that statins may shift DFUs from a hyperproliferative phenotype to a promigratory phenotype in order to stimulate healing. Furthermore, mevastatin induced a migratory phenotype in primary human keratinocytes through EGF-mediated activation of Rac1, resulting in actin cytoskeletal reorganization and lamellipodia formation. Interestingly, the EGF receptor is downregulated in tissue biopsies from patients with DFUs. Mevastatin restored EGF signaling in DFUs through disruption of caveolae to promote keratinocyte migration, which was confirmed by caveolin-1 (Cav1) overexpression studies. We conclude that topical statins may have considerable therapeutic potential as a treatment option for patients with DFUs and offer an effective treatment for chronic wounds that can be rapidly translated to clinical use.

摘要

糖尿病足溃疡(DFUs)是一种危及生命的疾病,常导致下肢截肢和寿命缩短。目前的治疗选择有限,且往往效果不佳,这就需要新的治疗方法。为了研究局部应用他汀类药物治疗 DFUs 患者的愈合潜力,我们对经美伐他汀处理的原代人角质形成细胞进行了下一代测序。我们发现美伐他汀激活并调节了 EGF 信号,引发了一种抗增殖和促迁移表型,表明他汀类药物可能使 DFUs 从过度增殖表型转变为促迁移表型,以刺激愈合。此外,美伐他汀通过 EGF 介导的 Rac1 激活诱导原代人角质形成细胞发生迁移表型,导致细胞骨架的重组和片状伪足的形成。有趣的是,EGF 受体在 DFUs 患者的组织活检中下调。美伐他汀通过破坏质膜微囊泡来恢复 DFUs 中的 EGF 信号,从而促进角质形成细胞迁移,这一点通过 Cav1 过表达研究得到了证实。我们得出结论,局部应用他汀类药物可能具有相当大的治疗潜力,可作为 DFUs 患者的治疗选择,并为慢性伤口提供一种有效的治疗方法,可以迅速转化为临床应用。

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