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重建鼠表皮模型的开发及其对促炎细胞因子反应的特征。

Development of a new model of reconstituted mouse epidermis and characterization of its response to proinflammatory cytokines.

机构信息

Laboratoire Inflammation, Tissus Epithéliaux et Cytokines (LITEC), EA 4331, Université de Poitiers, France.

Laboratorio de Inmunología Básica, Facultad de Bioquímica y Ciencias Biológicas, Universidad Nacional del Litoral, Santa Fe, Argentina.

出版信息

J Tissue Eng Regen Med. 2018 Feb;12(2):e1098-e1107. doi: 10.1002/term.2442. Epub 2017 Jun 26.

Abstract

The development of three-dimensional models of reconstituted mouse epidermis (RME) has been hampered by the difficulty to maintain murine primary keratinocyte cultures and to achieve a complete epidermal stratification. In this study, a new protocol is proposed for the rapid and convenient generation of RME, which reproduces accurately the architecture of a normal mouse epidermis. During RME morphogenesis, the expression of differentiation markers such as keratins, loricrin, filaggrin, E-cadherin and connexins was followed, showing that RME structure at day 5 was similar to those of a normal mouse epidermis, with the acquisition of the natural barrier function. It was also demonstrated that RME responded to skin-relevant proinflammatory cytokines by increasing the expression of antimicrobial peptides and chemokines, and inhibiting epidermal differentiation markers, as in the human system. This new model of RME is therefore suitable to investigate mouse epidermis physiology further and opens new perspectives to generate reconstituted epidermis from transgenic mice.

摘要

重建的小鼠表皮(RME)三维模型的发展受到维持小鼠原代角质形成细胞培养和实现完全表皮分层的困难的阻碍。在这项研究中,提出了一种新的快速简便的 RME 生成方案,可准确再现正常小鼠表皮的结构。在 RME 形态发生过程中,观察到分化标志物(如角蛋白、兜甲蛋白、丝聚合蛋白、E-钙黏蛋白和连接蛋白)的表达,表明第 5 天的 RME 结构类似于正常小鼠表皮,具有天然的屏障功能。还证明 RME 对皮肤相关促炎细胞因子的反应是通过增加抗菌肽和趋化因子的表达以及抑制表皮分化标志物的表达来实现的,这与人类系统相似。因此,这种新的 RME 模型适合进一步研究小鼠表皮生理学,并为从转基因小鼠中生成重建的表皮开辟了新的前景。

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