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TCR亲和力与共受体连接必要性之间的相互作用:高亲和力的肽-主要组织相容性复合体/TCR相互作用克服了CD8结合的缺乏。

Interplay between TCR affinity and necessity of coreceptor ligation: high-affinity peptide-MHC/TCR interaction overcomes lack of CD8 engagement.

作者信息

Kerry Samantha E, Buslepp Jennifer, Cramer Lorraine A, Maile Robert, Hensley Lucinda L, Nielsen Alma I, Kavathas Paula, Vilen Barbara J, Collins Edward J, Frelinger Jeffrey A

机构信息

Department of Microbiology and Immunology, University of North Carolina, Chapel Hill, NC 27599-7290, USA.

出版信息

J Immunol. 2003 Nov 1;171(9):4493-503. doi: 10.4049/jimmunol.171.9.4493.

Abstract

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.

摘要

CD8的结合被认为是初始T细胞激活过程中的关键事件。在本通讯中,我们探讨了肽-主要组织相容性复合体(pMHC)/T细胞受体(TCR)亲和力对CD8结合在原代初始细胞T细胞激活中的必要性的影响。我们使用了对同一pMHC-TCR复合体具有不同测量亲和力的两种肽,比较了有和没有CD8结合时pMHC/TCR的生化亲和力以及pMHC/TCR在细胞表面的结合亲和力。我们以同样的方式比较了初始T细胞的早期信号事件和后期功能活性。尽管早期信号事件发生了改变,但我们发现高亲和力的pMHC/TCR相互作用可以克服CD8结合对增殖和细胞毒性T淋巴细胞(CTL)功能的需求。随着时间的整合信号允许在没有CD8结合的情况下用高亲和力配体激活T细胞。

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