Literature DB >> 21349924

Exhaustive T-cell repertoire sequencing of human peripheral blood samples reveals signatures of antigen selection and a directly measured repertoire size of at least 1 million clonotypes.

René L Warren1, J Douglas Freeman, Thomas Zeng, Gina Choe, Sarah Munro, Richard Moore, John R Webb, Robert A Holt.   

Abstract

Massively parallel sequencing is a useful approach for characterizing T-cell receptor diversity. However, immune receptors are extraordinarily difficult sequencing targets because any given receptor variant may be present in very low abundance and may differ legitimately by only a single nucleotide. We show that the sensitivity of sequence-based repertoire profiling is limited by both sequencing depth and sequencing accuracy. At two timepoints, 1 wk apart, we isolated bulk PBMC plus naïve (CD45RA+/CD45RO-) and memory (CD45RA-/CD45RO+) T-cell subsets from a healthy donor. From T-cell receptor beta chain (TCRB) mRNA we constructed and sequenced multiple libraries to obtain a total of 1.7 billion paired sequence reads. The sequencing error rate was determined empirically and used to inform a high stringency data filtering procedure. The error filtered data yielded 1,061,522 distinct TCRB nucleotide sequences from this subject which establishes a new, directly measured, lower limit on individual T-cell repertoire size and provides a useful reference set of sequences for repertoire analysis. TCRB nucleotide sequences obtained from two additional donors were compared to those from the first donor and revealed limited sharing (up to 1.1%) of nucleotide sequences among donors, but substantially higher sharing (up to 14.2%) of inferred amino acid sequences. For each donor, shared amino acid sequences were encoded by a much larger diversity of nucleotide sequences than were unshared amino acid sequences. We also observed a highly statistically significant association between numbers of shared sequences and shared HLA class I alleles.

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Year:  2011        PMID: 21349924      PMCID: PMC3083096          DOI: 10.1101/gr.115428.110

Source DB:  PubMed          Journal:  Genome Res        ISSN: 1088-9051            Impact factor:   9.043


  24 in total

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3.  Profiling the T-cell receptor beta-chain repertoire by massively parallel sequencing.

Authors:  J Douglas Freeman; René L Warren; John R Webb; Brad H Nelson; Robert A Holt
Journal:  Genome Res       Date:  2009-06-18       Impact factor: 9.043

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Journal:  Bioinformatics       Date:  2007-09-10       Impact factor: 6.937

5.  Base-calling of automated sequencer traces using phred. II. Error probabilities.

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8.  Locus-specific amplification of HLA class I genes from genomic DNA: locus-specific sequences in the first and third introns of HLA-A, -B, and -C alleles.

Authors:  N Cereb; P Maye; S Lee; Y Kong; S Y Yang
Journal:  Tissue Antigens       Date:  1995-01

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  171 in total

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4.  IMonitor: A Robust Pipeline for TCR and BCR Repertoire Analysis.

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Authors:  Jonathan Desponds; Thierry Mora; Aleksandra M Walczak
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6.  Identifying specificity groups in the T cell receptor repertoire.

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Journal:  Nature       Date:  2017-06-21       Impact factor: 49.962

Review 7.  Biomarkers for glioma immunotherapy: the next generation.

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Review 8.  Systems immunology: just getting started.

Authors:  Mark M Davis; Cristina M Tato; David Furman
Journal:  Nat Immunol       Date:  2017-06-20       Impact factor: 25.606

9.  Diversity and clonal selection in the human T-cell repertoire.

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10.  MiTCR: software for T-cell receptor sequencing data analysis.

Authors:  Dmitriy A Bolotin; Mikhail Shugay; Ilgar Z Mamedov; Ekaterina V Putintseva; Maria A Turchaninova; Ivan V Zvyagin; Olga V Britanova; Dmitriy M Chudakov
Journal:  Nat Methods       Date:  2013-07-28       Impact factor: 28.547

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