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体外重建的人体皮肤暴露于紫外线A会诱导真皮成纤维细胞凋亡:随后的结缔组织修复及其在光老化中的影响。

UVA exposure of human skin reconstructed in vitro induces apoptosis of dermal fibroblasts: subsequent connective tissue repair and implications in photoaging.

作者信息

Bernerd F, Asselineau D

机构信息

L'Oréal, Life Sciences Research, C. Zviak Centre, 90 rue du général Roguet, 92583 Clichy, France.

出版信息

Cell Death Differ. 1998 Sep;5(9):792-802. doi: 10.1038/sj.cdd.4400413.

Abstract

The skin reconstructed in vitro has been previously shown to be a useful model to investigate the effects of UVB exposure (Bernerd and Asselineau, 1997). The present study describes the response to UVA irradiation. Major alterations were observed within the dermal compartment. Apoptosis of fibroblasts located in the superficial area of the dermal equivalent was observed as soon as 6 h after irradiation, leading to their disappearance after 48 h. This effect was obtained without major alterations of epidermal keratinocytes suggesting a differential cell type sensitivity to UVA radiations. In addition, collagenase I was secreted by dermal fibroblasts. The UVA dermal effects could be observed even after removal of the epidermis during the post irradiation period, demonstrating that they were independent of the keratinocyte response. The analysis of the tissue regeneration during the following 2 weeks revealed a connective tissue repair via fibroblasts proliferation, migration and active synthesis of extracellular matrix proteins such as fibronectin and procollagen I. This cellular recolonization of the superficial part of the dermal equivalent was due to activation of surviving fibroblasts located deeply in the dermal equivalent. The direct damage in the dermis and the subsequent connective tissue repair may contribute to the formation of UVA-induced dermal alterations.

摘要

先前已证明体外重建皮肤是研究紫外线B(UVB)照射影响的有用模型(Bernerd和Asselineau,1997年)。本研究描述了对紫外线A(UVA)照射的反应。在真皮层观察到主要变化。照射后6小时,即在真皮替代物浅层区域的成纤维细胞就出现凋亡,48小时后这些细胞消失。这种效应出现时,表皮角质形成细胞没有发生重大变化,表明不同细胞类型对UVA辐射的敏感性不同。此外,真皮成纤维细胞分泌了胶原酶I。即使在照射后时期去除表皮,仍可观察到UVA对真皮的影响,这表明这些影响与角质形成细胞的反应无关。对接下来2周内组织再生的分析显示,通过成纤维细胞增殖、迁移以及细胞外基质蛋白(如纤连蛋白和I型前胶原)的活跃合成实现了结缔组织修复。真皮替代物浅层部分的这种细胞重新定植是由于真皮替代物深处存活的成纤维细胞被激活。真皮的直接损伤以及随后的结缔组织修复可能导致UVA诱导的真皮改变的形成。

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