Two-Stage Cooperative T Cell Receptor-Peptide Major Histocompatibility Complex-CD8 Trimolecular Interactions Amplify Antigen Discrimination

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• 作者：Ning Jiang¹ ; ³ ; ⁴ ; Jun Huang¹ ; ³ ; ⁵ ; Lindsay J. Edwards² ; Baoyu Liu¹ ; Yan Zhang¹ ; ⁶ ; Carrie D. Beal² ; ⁷ ; Brian D. Evavold² ; Cheng Zhu¹ ; ^{cheng.zhu@bme.gatech.edu}
• 刊名：Immunity
• 出版年：2011
• 出版时间：28 January 2011
• 年：2011
• 卷：34
• 期：1
• 页码：13-23
• 全文大小：1122 K

文摘

Summary

The T cell receptor (TCR) and CD8 bind peptide-major histocompatibility complex (pMHC) glycoproteins to initiate adaptive immune responses, yet the trimolecular binding kinetics at the T cell membrane is unknown. By using a micropipette adhesion frequency assay, we show that this kinetics has two stages. The first consists of TCR-dominant binding to agonist pMHC. This triggers a second stage consisting of a step increase in adhesion after a one second delay. The second-stage binding requires Src family kinase activity to initiate CD8 binding to the same pMHC engaged by the TCR. This induced trimeric-cooperative interaction enhances adhesion synergistically to favor potent ligands, which further amplifies discrimination. Our data reveal a TCR-CD8 positive-feedback loop involved in initial signaling steps that is sensitive to a single pMHC is rapid, reversible, synergistic, and peptide discriminative.