首页> 外文期刊>European Journal of Immunology >Ligand binding of leukocyte integrin very late antigen-4 involves exposure of sulfhydryl groups and is subject to redox modulation.
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Ligand binding of leukocyte integrin very late antigen-4 involves exposure of sulfhydryl groups and is subject to redox modulation.

机译:配体结合白细胞整合素很晚antigen-4涉及暴露巯基组和氧化还原调制。

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摘要

Activation of leukocyte integrins is important for selective recruitment of cells from the circulation to tissues. Our previous studies showed that the binding between the integrin very late antigen-4 (VLA-4) and vascular cell adhesion molecule-1 (VCAM-1) is modulated by reactive oxygen species. In this study, we investigated the molecular nature of redox modulation on the activation states of VLA-4 on human leukocytes. We found that ligand binding of VLA-4 induced exposure of sulfhydryl groups on the alpha4 peptide. Low concentrations (5-10 microM) of exogenous hydrogen peroxide in the presence or absence of added glutathione enhanced the ligand binding ability of VLA-4 to VCAM-1 and cell rolling on VCAM-1, while higher concentrations (>/=100 microM) of hydrogen peroxide inhibited the binding. Exogenous hydrogen peroxide and glutathione induced molecular modification of S-glutathionylation on the alpha4 peptide. The redox regulation of the VLA-4 binding activity required outside-in signaling and cytoskeleton rearrangement. Our results indicate that ligand binding of VLA-4 involves redox modulations which may play a pivotal role in regulating the activation states of VLA-4 in inflammatory tissues and hence direct leukocyte trafficking.
机译:激活白细胞整合蛋白是重要的选择招聘的细胞流通组织。表明,整合素之间的绑定晚antigen-4 (VLA-4)和血管细胞粘附molecule-1 (VCAM-1)是由无功调节氧物种。分子的氧化还原性质调制的对人类白细胞激活VLA-4状态。我们发现配体结合VLA-4诱导alpha4暴露巯基组肽。在存在或外源过氧化氢没有添加谷胱甘肽增强配体绑定VLA-4 VCAM-1和细胞的能力VCAM-1滚动,而更高的浓度(> / = 100 microM)过氧化氢的抑制绑定。谷胱甘肽诱导的分子修饰S-glutathionylation alpha4肽。氧化还原VLA-4绑定活动的监管需要由外向内信号传导和细胞骨架重排。绑定VLA-4涉及氧化还原调节的可能发挥关键作用,调节激活状态的VLA-4炎症组织,因此直接贩卖白细胞。

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