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细胞外基质的氧化还原相关方面及其通过整合素的细胞接触。

Redox-relevant aspects of the extracellular matrix and its cellular contacts via integrins.

作者信息

Eble Johannes A, de Rezende Flávia Figueiredo

机构信息

1 Institute for Physiological Chemistry and Pathobiochemistry, University of Münster , Münster, Germany .

出版信息

Antioxid Redox Signal. 2014 May 1;20(13):1977-93. doi: 10.1089/ars.2013.5294. Epub 2014 Jan 8.

Abstract

SIGNIFICANCE

The extracellular matrix (ECM) fulfills essential functions in multicellular organisms. It provides the mechanical scaffold and environmental cues to cells. Upon cell attachment, the ECM signals into the cells. In this process, reactive oxygen species (ROS) are physiologically used as signalizing molecules.

RECENT ADVANCES

ECM attachment influences the ROS-production of cells. In turn, ROS affect the production, assembly and turnover of the ECM during wound healing and matrix remodeling. Pathological changes of ROS levels lead to excess ECM production and increased tissue contraction in fibrotic disorders and desmoplastic tumors. Integrins are cell adhesion molecules which mediate cell adhesion and force transmission between cells and the ECM. They have been identified as a target of redox-regulation by ROS. Cysteine-based redox-modifications, together with structural data, highlighted particular regions within integrin heterodimers that may be subject to redox-dependent conformational changes along with an alteration of integrin binding activity.

CRITICAL ISSUES

In a molecular model, a long-range disulfide-bridge within the integrin β-subunit and disulfide bridges within the genu and calf-2 domains of the integrin α-subunit may control the transition between the bent/inactive and upright/active conformation of the integrin ectodomain. These thiol-based intramolecular cross-linkages occur in the stalk domain of both integrin subunits, whereas the ligand-binding integrin headpiece is apparently unaffected by redox-regulation.

FUTURE DIRECTIONS

Redox-regulation of the integrin activation state may explain the effect of ROS in physiological processes. A deeper understanding of the underlying mechanism may open new prospects for the treatment of fibrotic disorders.

摘要

意义

细胞外基质(ECM)在多细胞生物中发挥着重要功能。它为细胞提供机械支架和环境线索。细胞附着于ECM时,ECM会向细胞发出信号。在此过程中,活性氧(ROS)在生理上被用作信号分子。

最新进展

ECM附着会影响细胞的ROS生成。反过来,ROS在伤口愈合和基质重塑过程中会影响ECM的产生、组装和周转。ROS水平的病理变化会导致纤维化疾病和促结缔组织增生性肿瘤中ECM产生过多和组织收缩增加。整合素是介导细胞与ECM之间的细胞黏附和力传递的细胞黏附分子。它们已被确定为ROS氧化还原调节的靶点。基于半胱氨酸的氧化还原修饰以及结构数据突出显示了整合素异二聚体内的特定区域,这些区域可能会随着整合素结合活性的改变而发生氧化还原依赖性构象变化。

关键问题

在一个分子模型中,整合素β亚基内的远距离二硫键以及整合素α亚基的膝部和小腿-2结构域内的二硫键可能控制整合素胞外域从弯曲/无活性构象到直立/活性构象的转变。这些基于硫醇的分子内交联发生在两个整合素亚基的柄部结构域,而与配体结合的整合素头部显然不受氧化还原调节的影响。

未来方向

整合素激活状态的氧化还原调节可能解释了ROS在生理过程中的作用。对潜在机制的更深入理解可能为纤维化疾病的治疗开辟新前景。

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