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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Extracellular ligation-dependent CD45RB enzymatic activity negatively regulates lipid raft signal transduction.
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Extracellular ligation-dependent CD45RB enzymatic activity negatively regulates lipid raft signal transduction.

机译:细胞外连接依赖CD45RB酶活性负调节脂质筏信号转导。

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摘要

CD45 is the most prominent membrane protein on lymphocytes. The function and regulation of this protein tyrosine phosphatase remain largely obscure, mainly because of the lack of a known ligand, and it still remains unknown whether such tyrosine phosphatases are subject to extracellular control at all. We report that an anti-CD45RB antibody (Ab) that prevents rejection and induces tolerance activates CD45RB tyrosine phosphatase enzymatic activity in T lymphocytes, allowing us to directly monitor the effects of increased CD45RB activity on signal transduction. Using both kinase substrate peptide arrays as well as conventional biochemistry, we also provide evidence of the various kinases involved in bringing about the inhibitory effect of this Ab on CD3-induced T-cell receptor signaling. Furthermore, we report that activated CD45RB translocates to lipid rafts and interferes with lipid raft localization and activation state of CD45 substrate Lck. Thus, these findings indeed prove that CD45 is subject to extracellular control and also define a novel mechanism by which receptor tyrosine phosphatases control lymphocyte biology and provide further insight into the intracellular signaling pathways effected by anti-CD45RB monoclonal Ab treatment.
机译:CD45是淋巴细胞上最突出的膜蛋白。该蛋白酪氨酸磷酸酶的功能和调节仍然很大程度上不清楚,这主要是由于缺乏已知的配体,并且仍然不清楚这种酪氨酸磷酸酶是否完全受到细胞外控制。我们报告说,一种抗CD45RB抗体(Ab)可以防止排斥并诱导耐受,从而激活T淋巴细胞中的CD45RB酪氨酸磷酸酶的酶促活性,从而使我们能够直接监测信号传导中CD45RB活性增加的影响。同时使用激酶底物肽阵列和常规生物化学,我们还提供了与这种Ab对CD3诱导的T细胞受体信号转导的抑制作用有关的各种激酶的证据。此外,我们报告说,活化的CD45RB易位到脂质筏并干扰脂质筏的定位和CD45底物Lck的激活状态。因此,这些发现确实证明了CD45受到细胞外控制,并且还定义了一种新的机制,受体酪氨酸磷酸酶通过该机制控制淋巴细胞生物学,并进一步揭示了抗CD45RB单克隆抗体治疗影响的细胞内信号传导途径。

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