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Expression of a novel integrin beta 1 chain epitope and anti-beta 1 antibody-mediated enhancement of fibronectin binding are dependent on the stage of T cell differentiation.

表位 胸腺细胞 整合素 分子生物学 纤维连接蛋白 生物 BETA(编程语言) 层粘连蛋白 T细胞 细胞生物学 CD8型 CD3型 CD44细胞 T细胞受体 阿尔法(金融) 整合素αM T淋巴细胞 抗原 受体 细胞 细胞外基质 免疫学 生物化学 免疫系统 流式细胞术 护理部 程序设计语言 患者满意度 医学 结构效度 计算机科学
作者
Scott Wadsworth,Andrew C. Chang,Meng Hong,Mark J. Halvorson,Sigrid A. Otto,J E Coligan
出处
期刊:Journal of Immunology [American Association of Immunologists]
卷期号:154 (5): 2125-2133 被引量:1
标识
DOI:10.4049/jimmunol.154.5.2125
摘要

Beta 1 integrins are a family of alpha beta heterodimers that serve as cell surface receptors for extracellular matrix proteins. We demonstrate that the anti-mouse integrin beta 1 chain mAb KMI6 selectively recognizes a beta 1 epitope that is constitutively expressed by certain immature thymocytes and is induced only slightly on mature thymocytes and peripheral T cells by activation with Con A. Because virtually all cells examined expressed beta 1 integrins on their surface, expression of the KMI6 epitope is T cell differentiation stage specific. Most CD3-4-8- thymocytes were KMI6+, with the lowest level of staining observed on the earliest CD44+IL-2R- cells within this subset. Expression was down-regulated during the CD3-4-8- to CD3-4-8+ transition, and lost by the CD4+8+ stage. Mature single positive thymocytes and resting peripheral T cells were also KMI6-. In contrast with the loss of the epitope before TCR expression by other thymocytes, most CD3+4-8- and certain CD8+ gamma delta TCR+ thymocytes were KMI6+ Addition of KMI6 to cell adhesion assays enhanced CD4-8- thymocyte, but not activated mature thymocyte or peripheral T cell, binding to fibronectin (via alpha 4 beta 1 and alpha 5 beta 1), whereas laminin binding (via alpha 6 beta 1) was unaffected. These properties distinguish the KMI6 epitope from other epitopes involved in beta 1 integrin activation in mice and other species. The unique selectivity of KMI6 recognition of beta 1 integrins, and its selective enhancement of ligand binding suggest that beta 1 integrin structure and factors that regulate beta 1 integrin binding are correlated with the stage of T cell differentiation.

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