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Positive and Negative Regulation of FcɛRI-Mediated Signaling by the Adaptor Protein LAB/NTAL

机译:适配器蛋白LAB / NTAL对FcɛRI介导的信号的正向和负向调节

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摘要

Linker for activation of B cells (LAB, also called NTAL; a product of wbscr5 gene) is a newly identified transmembrane adaptor protein that is expressed in B cells, NK cells, and mast cells. Upon BCR activation, LAB is phosphorylated and interacts with Grb2. LAB is capable of rescuing thymocyte development in LAT-deficient mice. To study the in vivo function of LAB, LAB-deficient mice were generated. Although disruption of the Lab gene did not affect lymphocyte development, it caused mast cells to be hyperresponsive to stimulation via the FcɛRI, evidenced by enhanced Erk activation, calcium mobilization, degranulation, and cytokine production. These data suggested that LAB negatively regulates mast cell function. However, mast cells that lacked both linker for activation of T cells (LAT) and LAB proteins had a more severe block in FcɛRI-mediated signaling than LAT−/− mast cells, demonstrating that LAB also shares a redundant function with LAT to play a positive role in FcɛRI-mediated signaling.
机译:用于激活B细胞的连接子(LAB,也称为NTAL; wbscr5基因的产物)是一种新鉴定的跨膜衔接蛋白,在B细胞,NK细胞和肥大细胞中表达。在BCR激活后,LAB被磷酸化并与Grb2相互作用。 LAB能够挽救LAT缺陷小鼠的胸腺细胞发育。为了研究LAB的体内功能,产生了LAB缺陷的小鼠。尽管Lab基因的破坏不会影响淋巴细胞的发育,但它会导致肥大细胞对通过FcɛRI刺激产生高反应性,这通过增强的Erk活化,钙动员,脱粒和细胞因子生成来证明。这些数据表明LAB负调节肥大细胞功能。但是,缺乏激活T细胞(LAT)和LAB蛋白的接头的肥大细胞在FcɛRI介导的信号传导中比LAT -/-肥大细胞具有更严重的阻断作用,这表明LAB也共享一个具有LAT的冗余功能在FcɛRI介导的信号传导中发挥积极作用。

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