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胎盘蛋白14对T细胞活化的负调控是由酪氨酸磷酸酶受体CD45介导的。

Negative regulation of T cell activation by placental protein 14 is mediated by the tyrosine phosphatase receptor CD45.

作者信息

Rachmilewitz Jacob, Borovsky Zipora, Riely Gregory J, Miller Robin, Tykocinski Mark L

机构信息

Goldyne Savad Institute of Gene Therapy, Hadassah University Hospital, Jerusalem 91120, Israel.

出版信息

J Biol Chem. 2003 Apr 18;278(16):14059-65. doi: 10.1074/jbc.M211716200. Epub 2003 Jan 29.

DOI:10.1074/jbc.M211716200
PMID:12556471
Abstract

CD45 is the major protein tyrosine phosphatase receptor on T cell surfaces that functions as both a positive and a negative regulator of T cell receptor (TCR) signaling. Although CD45 is required for the activation of TCR-associated Src family kinases, it also dephosphorylates phosphoproteins involved in the TCR-signaling cascade. This study links CD45 to the inhibitory activity of placental protein 14 (PP14), a major soluble protein of pregnancy that is now known to be a direct modulator of T cells and to function by desensitizing TCR signaling. PP14 and CD45 co-capped with each other, pointing to a physical linkage between the two. Interestingly, however, the binding of PP14 to T cell surfaces was not restricted to CD45 alone, with evidence showing that PP14 binds to other surface molecules in a carbohydrate-dependent fashion. Notwithstanding the broader molecular binding potential of PP14, its interaction with CD45 appeared to have special functional significance. Using transfected derivatives of the HPB. ALL mutant T cell line that differ in CD45 expression, we established that the inhibitory effects of PP14 are dependent upon the expression of intact CD45 on T cell surfaces. Based upon these findings, we propose a new immunoregulatory model for PP14, wherein one of its surface molecular targets, CD45, mediates its T cell inhibitory activity, accounting for the intriguing capacity of PP14 to elevate TCR activation thresholds and thereby down-regulate T cell activation.

摘要

CD45是T细胞表面主要的蛋白酪氨酸磷酸酶受体,它作为T细胞受体(TCR)信号传导的正向和负向调节因子发挥作用。虽然TCR相关Src家族激酶的激活需要CD45,但它也能使参与TCR信号级联反应的磷酸化蛋白去磷酸化。本研究将CD45与胎盘蛋白14(PP14)的抑制活性联系起来,PP14是妊娠期间的一种主要可溶性蛋白,现在已知它是T细胞的直接调节剂,通过使TCR信号脱敏发挥作用。PP14和CD45相互共帽,表明两者之间存在物理联系。然而,有趣的是,PP14与T细胞表面的结合并不局限于单独的CD45,有证据表明PP14以碳水化合物依赖的方式与其他表面分子结合。尽管PP14具有更广泛的分子结合潜力,但其与CD45的相互作用似乎具有特殊的功能意义。使用HPB.ALL突变T细胞系的转染衍生物,这些衍生物在CD45表达上存在差异,我们确定PP14的抑制作用取决于T细胞表面完整CD45的表达。基于这些发现,我们提出了一种新的PP14免疫调节模型,其中其表面分子靶点之一CD45介导其T细胞抑制活性,这解释了PP14提高TCR激活阈值从而下调T细胞激活的有趣能力。

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