首页> 外文期刊>The journal of immunology >Characterization of CCR9 Expression and CCL25/Thymus-Expressed Chemokine Responsiveness During T Cell Development: CD3highCD69+ Thymocytes and γδTCR+ Thymocytes Preferentially Respond to CCL25
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Characterization of CCR9 Expression and CCL25/Thymus-Expressed Chemokine Responsiveness During T Cell Development: CD3highCD69+ Thymocytes and γδTCR+ Thymocytes Preferentially Respond to CCL25

机译:T细胞发育过程中CCR9表达和CCL25 /胸腺表达的趋化因子反应的表征:CD3highCD69 +胸腺细胞和γδTCR+胸腺细胞对CCL25有优先反应

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CCR9 mediates chemotaxis of thymocytes in response to CCL25/thymus-expressed chemokine, and its mRNA is selectively expressed in thymus and small intestine, the two known sites of T lymphopoiesis. To examine the expression of CCR9 during lymphocyte development, we generated polyclonal Ab that recognizes murine CCR9. CCR9 was expressed on the majority of immature CD4+CD8+ (double-positive) thymocytes, but not on immature CD4?CD8? (double-negative) thymocytes. CCR9 was down-regulated during the transition of double-positive thymocytes to the CD4+ or CD8+ (single-positive) stage, and only a minor subset of CD8+ lymph node T cells expressed CCR9. All CCR9+ thymocyte subsets migrated in response to CCL25; however, CD69+ thymocytes demonstrated enhanced CCL25-induced migration compared with CD69? thymocytes. Ab-mediated TCR stimulation also enhanced CCL25 responsiveness, indicating that CCL25-induced thymocyte migration is augmented by TCR signaling. Approximately one-half of all γδTCR+ thymocytes and peripheral γδTCR+ T cells expressed CCR9 on their surface, and these cells migrated in response to CCL25. These findings suggest that CCR9 may play an important role in the development and trafficking of both αβTCR+ and γδTCR+ T cells.
机译:CCR9响应CCL25 /胸腺表达的趋化因子介导胸腺细胞趋化性,其mRNA在T淋巴细胞生成的两个已知位点胸腺和小肠中选择性表达。为了检查淋巴细胞发育过程中CCR9的表达,我们产生了识别鼠CCR9的多克隆抗体。 CCR9在大多数未成熟的CD4 + CD8 +(双阳性)胸腺细胞中表达,但在未成熟的CD4?CD8?中表达。 (双阴性)胸腺细胞。在双阳性胸腺细胞过渡到CD4 +或CD8 +(单阳性)阶段期间,CCR9被下调,只有一小部分CD8 +淋巴结T细胞表达CCR9。所有CCR9 +胸腺细胞亚群均响应于CCL25而迁移。然而,与CD69相比,CD69 +胸腺细胞显示出增强的CCL25诱导的迁移。胸腺细胞。 Ab介导的TCR刺激也增强了CCL25的响应性,表明TCR信号传导增强了CCL25诱导的胸腺细胞迁移。所有γδTCR+胸腺细胞和外周γδTCR+ T细胞中约有一半在其表面表达CCR9,并且这些细胞响应于CCL25而迁移。这些发现表明CCR9可能在αβTCR+和γδTCR+ T细胞的发育和运输中起重要作用。

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