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首页> 外文期刊>The Journal of Experomental Medicine >An essential role for SKAP-55 in LFA-1 clustering on T cells that cannot be substituted by SKAP-55R
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An essential role for SKAP-55 in LFA-1 clustering on T cells that cannot be substituted by SKAP-55R

机译:SKAP-55在无法被SKAP-55R取代的T细胞LFA-1簇中的重要作用

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Lymphocyte function-associated antigen (LFA)-1 clustering, which is needed for high avidity binding to intercellular adhesion molecule (ICAM)-1 and -2, regulates T cell motility and T cell–antigen-presenting cell (APC) conjugation. In this study, down-regulation of SKAP-55 by small interfering RNAs (siRNAs) identified an essential role for this adaptor molecule in the T cell receptor (TCR)–mediated ”inside-out signaling” that is needed for LFA-1 clustering and T cell–APC conjugation. In contrast, down-regulation of SKAP-55 had no effect on TCR–CD3 clustering. Furthermore, the expression of the related protein SKAP-55R failed to compensate for the loss of SKAP-55 in LFA-1 clustering, indicating that SKAP-55 has a unique function that cannot be replaced by this closely related protein. Our findings therefore indicate that SKAP-55, unlike SKAP-55R, is specifically tailored as an essential component of the inside-out signaling events that couple the TCR to LFA-1 clustering and T cell–APC conjugation.
机译:淋巴细胞功能相关抗原(LFA)-1簇是细胞与细胞间粘附分子(ICAM)-1和-2的高亲和力结合所必需的,它调节T细胞运动性和T细胞-抗原呈递细胞(APC)的结合。在这项研究中,小干扰RNA(siRNA)对SKAP-55的下调确定了该衔接子分子在T细胞受体(TCR)介导的“由内而外的信号传导”中的重要作用,这是LFA-1聚类所必需的和T细胞与APC的结合。相反,SKAP-55的下调对TCR-CD3簇没有影响。此外,相关蛋白SKAP-55R的表达未能补偿LFA-1簇中SKAP-55的损失,这表明SKAP-55具有无法被该紧密相关蛋白替代的独特功能。因此,我们的发现表明,与SKAP-55R不同,SKAP-55经过专门设计,是将TCR与LFA-1簇和T细胞与APC偶联的内向外信号事件的重要组成部分。

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