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表达BV19的循环人类CD8 T细胞的CDR3克隆型和氨基酸基序多样性

CDR3 clonotype and amino acid motif diversity of BV19 expressing circulating human CD8 T cells.

作者信息

Yassai Maryam B, Demos Wendy, Janczak Teresa, Naumova Elena N, Gorski Jack

机构信息

Blood Research Institute, BloodCenter of Wisconsin, Milwaukee, WI, United States.

Initiative for the Forecasting and Modeling of Infectious Diseases, Tufts University, Medford, MA, United States.

出版信息

Hum Immunol. 2016 Jan;77(1):137-145. doi: 10.1016/j.humimm.2015.11.007. Epub 2015 Nov 24.

Abstract

Generating a detailed description of human T cell repertoire diversity is an important goal in the study of human immunology. The circulation is the source of most T cells used for studies in humans. Here we use high throughput sequencing of TCR BV19 transcripts from CD8 T cells derived from unmanipulated PBMC from an older HLA-A2 individual to provide a quantitative and qualitative description of the clonotypic CDR3 nucleotide and amino acid composition of the TCR β-chain from this subset of circulating CD8 T cells. Aggregated samples from six time points spanning ∼1.5 years were analyzed to smooth possible temporal fluctuation. BV19 encompasses the well studied RS-encoding clonotypes involved in recognition of the M1(58-66) epitope from influenza A in HLA-A2 individuals. The clonotype distribution was diverse, complex and self-similar. The amino acid composition was generally skewed in favor of glycines and there were specific amino acids observed at higher frequency at the NDN start position. The motif repertoire distribution was also diverse, complex and self-similar with respect to CDR3 length, NDN start and length.

摘要

生成人类T细胞受体库多样性的详细描述是人类免疫学研究的一个重要目标。循环系统是人类研究中使用的大多数T细胞的来源。在这里,我们对来自一名老年HLA - A2个体未经处理的外周血单核细胞(PBMC)的CD8 T细胞中的TCR BV19转录本进行高通量测序,以定量和定性地描述这群循环CD8 T细胞中TCR β链的克隆型CDR3核苷酸和氨基酸组成。分析了跨越约1.5年的六个时间点的聚合样本,以平滑可能的时间波动。BV19包含了在HLA - A2个体中参与识别甲型流感病毒M1(58 - 66)表位的、研究充分的编码RS的克隆型。克隆型分布多样、复杂且具有自相似性。氨基酸组成总体上偏向甘氨酸,并且在NDN起始位置观察到特定氨基酸的出现频率较高。基序库分布在CDR3长度、NDN起始和长度方面同样多样、复杂且具有自相似性。

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