首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Interplay between TCR affinity and necessity of coreceptor ligation: high-affinity peptide-MHC/TCR interaction overcomes lack of CD8 engagement.
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Interplay between TCR affinity and necessity of coreceptor ligation: high-affinity peptide-MHC/TCR interaction overcomes lack of CD8 engagement.

机译:TCR亲和力与共受体连接的必要性之间的相互作用:高亲和力肽-MHC / TCR相互作用克服了CD8参与的缺乏。

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摘要

CD8 engagement is believed to be a critical event in the activation of naive T cells. In this communication, we address the effects of peptide-MHC (pMHC)/TCR affinity on the necessity of CD8 engagement in T cell activation of primary naive cells. Using two peptides with different measured avidities for the same pMHC-TCR complex, we compared biochemical affinity of pMHC/TCR and the cell surface binding avidity of pMHC/TCR with and without CD8 engagement. We compared early signaling events and later functional activity of naive T cells in the same manner. Although early signaling events are altered, we find that high-affinity pMHC/TCR interactions can overcome the need for CD8 engagement for proliferation and CTL function. An integrated signal over time allows T cell activation with a high-affinity ligand in the absence of CD8 engagement.
机译:CD8的参与被认为是幼稚T细胞活化中的关键事件。在本通讯中,我们探讨了肽-MHC(pMHC)/ TCR亲和力对原代幼稚细胞T细胞活化中CD8参与的必要性的影响。对于相同的pMHC-TCR复合物,使用两种具有不同测量亲和力的肽,我们比较了有和没有CD8参与的pMHC / TCR的生化亲和力和pMHC / TCR的细胞表面结合亲和力。我们以相同的方式比较了幼稚T细胞的早期信号传导事件和后来的功能活性。尽管早期的信号事件发生了变化,但我们发现高亲和力的pMHC / TCR相互作用可以克服CD8参与增殖和CTL功能的需要。随着时间的推移,整合的信号允许T细胞在没有CD8参与的情况下以高亲和力的配体活化。

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