The Protein Crystallography Unit, Department of Biochemistry and Molecular Biology, Monash University, Clayton, Victoria 3800, Australia.
J Exp Med. 2010 Jul 5;207(7):1555-67. doi: 10.1084/jem.20100603. Epub 2010 Jun 21.
In comparison to human leukocyte antigen (HLA) polymorphism, the impact of allelic sequence variation within T cell receptor (TCR) loci is much less understood. Particular TCR loci have been associated with autoimmunity, but the molecular basis for this phenomenon is undefined. We examined the T cell response to an HLA-B3501-restricted epitope (HPVGEADYFEY) from Epstein-Barr virus (EBV), which is frequently dominated by a TRBV901(+) public TCR (TK3). However, the common allelic variant TRBV902, which differs by a single amino acid near the CDR2beta loop (Gln55-->His55), was never used in this response. The structure of the TK3 TCR, its allelic variant, and a nonnaturally occurring mutant (Gln55-->Ala55) in complex with HLA-B3501(HPVGEADYFEY) revealed that the Gln55-->His55 polymorphism affected the charge complementarity at the TCR-peptide-MHC interface, resulting in reduced functional recognition of the cognate and naturally occurring variants of this EBV peptide. Thus, polymorphism in the TCR loci may contribute toward variability in immune responses and the outcome of infection.
与人类白细胞抗原(HLA)多态性相比,T 细胞受体(TCR)基因座内等位基因序列变异的影响还不太清楚。某些 TCR 基因座与自身免疫有关,但这一现象的分子基础尚不清楚。我们研究了针对 Epstein-Barr 病毒(EBV)的 HLA-B3501 限制性表位(HPVGEADYFEY)的 T 细胞反应,该表位通常由 TRBV901(+)公共 TCR(TK3)主导。然而,在该反应中从未使用过常见的等位基因变体 TRBV902,其在 CDR2beta 环附近仅相差一个氨基酸(Gln55-->His55)。与 HLA-B3501(HPVGEADYFEY)结合的 TK3 TCR、其等位基因变体和非天然存在的突变体(Gln55-->Ala55)的结构表明,Gln55-->His55 多态性影响 TCR-肽-MHC 界面的电荷互补性,导致对该 EBV 肽的同源和天然变体的功能识别减少。因此,TCR 基因座的多态性可能导致免疫反应和感染结果的变异性。
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