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. Warren,J. Douglas Freeman,Thomas Zeng,Gina Choe,Sarah A. Munro,Richard D. Moore,John R. Webb,Robert A. Holt +7 more
TLDR
It is shown that the sensitivity of sequence-based repertoire profiling is limited by both sequencing depth and sequencing accuracy, and a new, directly measured, lower limit on individual T-cell repertoire size is established.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 naive (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.read more
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Patent
Clonotypes as biometric specimen tags
Malek Faham,Thomas D. Willis +1 more
TL;DR: In this article, a method for identifying or distinguishing biological specimens, such as patient specimens, as being from the same or different individuals by analysis of specimen clonotypes is presented.
Patent
Rare clonotypes and uses thereof
TL;DR: In this paper, a method of selecting disease-correlated clonotypes that have a reduced likelihood of producing a false positive signal of relapse when, used to monitor minimal residual disease.
Journal ArticleDOI
Applications of next-generation sequencing to blood and marrow transplantation.
TL;DR: The ability to perform comprehensive tumor sequencing provides a systematic approach to the discovery of genetic alterations that can encode peptides with restricted tumor expression, and hence serve as potential target antigens of graft-versus-leukemia responses.
Journal ArticleDOI
Quantitative analysis of T cell receptor diversity in clinical samples of human peripheral blood
TL;DR: It is demonstrated that one hundred thousand T cells are sufficient to obtain a robust, highly reproducible measure of the global TCR Vβ repertoire diversity among twenty Vβ families in human peripheral blood and it is shown that use of lower cell number results in a dwindling of observed diversity.
Journal ArticleDOI
Multi-loci diagnosis of acute lymphoblastic leukaemia with high-throughput sequencing and bioinformatics analysis.
Yann Ferret,Aurélie Caillault,Shéhérazade Sebda,Marc Duez,Marc Duez,Nathalie Grardel,Nicolas Duployez,Céline Villenet,Martin Figeac,Claude Preudhomme,Mikaël Salson,Mikaël Salson,Mathieu Giraud,Mathieu Giraud +13 more
TL;DR: This study emphasizes the progress that HTS with adapted bioinformatics tools can bring to the diagnosis of leukaemia patients, and identifies 125 leukaemic clones with recombinations on multiple loci, including Dd2/Dd3 and Intron/KDE rearrangements.
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