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信号蛋白SWAP-70是B细胞有效归巢至淋巴器官所必需的。

Signaling protein SWAP-70 is required for efficient B cell homing to lymphoid organs.

作者信息

Pearce Glen, Angeli Veronique, Randolph Gwendalyn J, Junt Tobias, von Andrian Ulrich, Schnittler Hans-Joachim, Jessberger Rolf

机构信息

Institute of Physiological Chemistry, Dresden University of Technology, 01307 Dresden, Germany.

出版信息

Nat Immunol. 2006 Aug;7(8):827-34. doi: 10.1038/ni1365. Epub 2006 Jul 16.

Abstract

The migration of B cells into secondary lymphoid organs is required for the generation of an effective immune response. Here we analyzed the involvement of SWAP-70, a Rac-interacting protein involved in actin rearrangement, in B cell entry into lymph nodes. We noted reduced migration of Swap70-/- B cells into lymph nodes in vivo. Swap70-/- B cells rolled and adhered, yet accumulated in lymph node high endothelial venules. This defect was not due to impaired integrin expression or chemotaxis. Instead, Swap70-/- B cells aberrantly regulated integrin-mediated adhesion. During attachment, Swap70-/- B cells showed defective polarization and did not form uropods or stabilize lamellipodia at a defined region. Thus, SWAP-70 selectively regulates processes essential for B cell entry into lymph nodes.

摘要

B细胞迁移至次级淋巴器官是产生有效免疫反应所必需的。在此,我们分析了SWAP-70(一种参与肌动蛋白重排的Rac相互作用蛋白)在B细胞进入淋巴结过程中的作用。我们注意到Swap70-/- B细胞在体内向淋巴结的迁移减少。Swap70-/- B细胞能够滚动和黏附,但在淋巴结高内皮微静脉中积累。此缺陷并非由于整合素表达受损或趋化性受损所致。相反,Swap70-/- B细胞异常调节整合素介导的黏附。在附着过程中,Swap70-/- B细胞表现出极化缺陷,并且在特定区域未形成尾足或稳定片状伪足。因此,SWAP-70选择性地调节B细胞进入淋巴结所必需的过程。

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