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首页> 外文期刊>Immunology: An Official Journal of the British Society for Immunology >Understanding the mechanisms that facilitate specificity, not redundancy, of chemokine-mediated leukocyte recruitment
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Understanding the mechanisms that facilitate specificity, not redundancy, of chemokine-mediated leukocyte recruitment

机译:了解促进特异性,而不是冗余,趋化因子介导的白细胞募集的机制

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摘要

Chemokines (chemotactic cytokines) and their receptors are critical to recruitment and positioning of cells during development and the immune response. The chemokine system has long been described as redundant for a number of reasons, where multiple chemokine ligands can bind to multiple receptors and vice versa. This apparent redundancy has been thought to be a major reason for the failure of drugs targeting chemokines during inflammatory disease. We are now beginning to understand that chemokine biology is in fact based around a high degree of specificity, where each chemokine and receptor plays a particular role in the immune response. This specificity hypothesis is supported by a number of recent studies designed to address this problem. This review will detail these studies and the mechanisms that produce this specificity of function with an emphasis on the emerging role of chemokine-glycosaminoglycan interactions.
机译:趋化因子(趋化性细胞因子)及其受体对于在发育过程中招募和定位细胞和免疫反应至关重要。 由于多种原因,趋化因子系统长期被描述为多余的,其中多个趋化因子配体可以与多个受体结合,反之亦然。 这种明显的冗余被认为是煽动性疾病靶向趋化因子的药物失败的主要原因。 我们现在开始了解,趋化因素生物学实际上基于高度的特异性,其中每个趋化因子和受体在免疫应答中起着特定作用。 该特异性假设是由最近旨在解决这一问题的最近研究的支持。 本综述将详述这些研究和产生这种功能特异性的机制,重点是趋化因子 - 糖胺聚糖相互作用的新兴作用。

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