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The influence of the src-family kinases, Lck and Fyn, on T cell differentiation, survival and activation.

机译:src家族激酶Lck和Fyn对T细胞分化,存活和激活的影响。

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摘要

The src-family kinases p56lck (Lck) and p59fyn (Fyn) are expressed in T cells and are among the first signaling molecules to be activated downstream of the T cell receptor (TCR). Evidence is emerging that although closely related, these signaling molecules have discrete functions during development, maintenance and activation of peripheral T cells. For example, during thymopoiesis Lck is uniquely able to provide all the signals required for pre-TCRbeta selection, although Fyn can substitute for a subset of these. Positive selection of CD4 single-positive (SP) cells is also critically dependent on the expression of Lck but not Fyn, while differentiation of CD8 SP cells proceeds relatively efficiently in the absence of Lck. In naive peripheral T cells either Lck or Fyn can transmit TCR-mediated survival signals, and yet only Lck is able to trigger TCR-mediated expansion signals under conditions of lymphopenia. Stimulation of naive T cells by antigenic stimuli is also severely compromised in the absence of Lck, but more subtly impaired by the absence of Fyn. We discuss recent experiments addressing how these two src-kinase family members interface with downstream signaling pathways to regulate these diverse aspects of T cell behavior.
机译:src家族激酶p56lck(Lck)和p59fyn(Fyn)在T细胞中表达,并且是要在T细胞受体(TCR)下游激活的第一个信号分子。越来越多的证据表明,尽管这些信号分子密切相关,但它们在外周T细胞的发育,维持和激活过程中具有离散的功能。例如,在胸腺造血过程中,Lck独特地能够提供TCRbeta前选择所需的所有信号,尽管Fyn可以替代其中的一部分。 CD4单阳性(SP)细胞的阳性选择也关键取决于Lck的表达,而不取决于Fyn,而在没有Lck的情况下CD8 SP细胞的分化相对有效。在幼稚的外周血T细胞中,Lck或Fyn均可传递TCR介导的生存信号,但只有Lck能够在淋巴细胞减少症的条件下触发TCR介导的扩增信号。在缺乏Lck的情况下,抗原刺激对幼稚T细胞的刺激也受到严重损害,但在缺乏Fyn的情况下受到更微弱的损害。我们讨论了解决这两个src激酶家族成员如何与下游信号通路相互作用以调节T细胞行为的这些不同方面的最新实验。

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