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活性氧簇在 2 型糖尿病大鼠模型中 IGF1 抵抗和伤口愈合受损的发展中构成一个汇聚枢纽。

ROS constitute a convergence nexus in the development of IGF1 resistance and impaired wound healing in a rat model of type 2 diabetes.

机构信息

Department of Pharmacology and Toxicology, School of Medicine, PO Box 24923, Safat 13110, Kuwait.

出版信息

Dis Model Mech. 2012 May;5(3):375-88. doi: 10.1242/dmm.007872. Epub 2012 Feb 23.

DOI:10.1242/dmm.007872

PMID:22362362

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3339831/

Abstract

An indolent non-healing wound and insulin and/or insulin-like growth factor (IGF1) resistance are cardinal features of diabetes, inflammation and hypercortisolemia. Little is known about why these phenomena occur in so many contexts. Do the various triggers that induce insulin and/or IGF1 resistance and retard wound healing act through a common mechanism? Cultured dermal fibroblasts from rats and full-thickness excisional wounds were used as models to test the premise that reactive oxygen species (ROS) play a causal role in the development of IGF1 resistance and impaired wound healing under different but pathophysiologically relevant clinical settings, including diabetes, dexamethasone-induced hypercortisolemia and TNFα-induced inflammation. In normal fibroblasts, IGF1 initiated a strong degree of phosphorylation of insulin receptor substrate 1 (IRS1) (Tyr612) and Akt (Ser473), concomitantly with increased PI3K activity. This phenomenon seemed to be attenuated in fibroblasts that had phenotypic features of diabetes, inflammation or hypercortisolemia. Notably, these cells also exhibited an increase in the activity of the ROS-phospho-JNK (p-JNK)-p-IRS1 (Ser307) axis. The above-mentioned defects were reflected functionally by attenuation in IGF1-dependent stimulation of key fibroblast functions, including collagen synthesis and cell proliferation, migration and contraction. The effects of IGF1 on glucose disposal and cutaneous wound healing were also impaired in diabetic or hypercortisolemic rats. The ROS suppressors EUK-134 and α-lipoic acid, or small interfering RNA (siRNA)-mediated silencing of JNK expression, restored IGF1 sensitivity both in vitro and in vivo, and also ameliorated the impairment in IGF1-mediated wound responses during diabetes, inflammation and hypercortisolemia. Our data advance the notion that ROS constitute a convergence nexus for the development of IGF1 resistance and impaired wound healing under different but pathophysiologically relevant clinical settings, with a proof of concept for the beneficial effect of ROS suppressors.

摘要

慢性不愈合伤口以及胰岛素和/或胰岛素样生长因子 1（IGF1）抵抗是糖尿病、炎症和皮质醇过多的主要特征。目前尚不清楚为什么这些现象会在如此多的情况下发生。那么，各种导致胰岛素和/或 IGF1 抵抗以及延迟伤口愈合的诱因是否通过共同的机制起作用？我们使用大鼠真皮成纤维细胞和全层切除伤口作为模型，来验证以下前提：在不同但与病理生理学相关的临床环境下，包括糖尿病、地塞米松诱导的皮质醇过多和 TNFα 诱导的炎症，活性氧（ROS）在 IGF1 抵抗和伤口愈合受损的发展中起因果作用。在正常成纤维细胞中，IGF1 引发胰岛素受体底物 1（IRS1）（Tyr612）和 Akt（Ser473）强烈程度的磷酸化，同时伴随着 PI3K 活性增加。这种现象在具有糖尿病、炎症或皮质醇过多表型特征的成纤维细胞中似乎减弱。值得注意的是，这些细胞还表现出 ROS-磷酸化-JNK（p-JNK）-p-IRS1（Ser307）轴的活性增加。上述缺陷在 IGF1 依赖性刺激关键成纤维细胞功能方面表现为功能减弱，包括胶原合成和细胞增殖、迁移和收缩。IGF1 对葡萄糖摄取和皮肤伤口愈合的影响也在糖尿病或皮质醇过多的大鼠中受损。ROS 抑制剂 EUK-134 和 α-硫辛酸，或 JNK 表达的小干扰 RNA（siRNA）介导的沉默，在体外和体内恢复了 IGF1 的敏感性，并且还改善了糖尿病、炎症和皮质醇过多期间 IGF1 介导的伤口反应受损。我们的数据进一步证实，ROS 构成了在不同但与病理生理学相关的临床环境下发生 IGF1 抵抗和伤口愈合受损的汇聚枢纽，为 ROS 抑制剂的有益作用提供了概念验证。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8117/3339831/a88ae2ee3af9/DMM007872F1.jpg

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活性氧簇在 2 型糖尿病大鼠模型中 IGF1 抵抗和伤口愈合受损的发展中构成一个汇聚枢纽。

ROS constitute a convergence nexus in the development of IGF1 resistance and impaired wound healing in a rat model of type 2 diabetes.

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