2013
DOI: 10.1101/gr.154815.113
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Network properties derived from deep sequencing of human B-cell receptor repertoires delineate B-cell populations

Abstract: The adaptive immune response selectively expands B-and T-cell clones following antigen recognition by B-and T-cell receptors (BCR and TCR), respectively. Next-generation sequencing is a powerful tool for dissecting the BCR and TCR populations at high resolution, but robust computational analyses are required to interpret such sequencing. Here, we develop a novel computational approach for BCR repertoire analysis using established next-generation sequencing methods coupled with network construction and populati… Show more

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Cited by 135 publications
(203 citation statements)
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“…Previous efforts to characterize the TCR repertoire in T1D subjects have been limited to tissues obtained from few or even a mere single organ donor (12,13) or were restricted to peripheral blood samples (14,37). Furthermore, BCR sequencing data in human samples is limited, particularly in subjects with T1D (15,16). Thus, to our knowledge, this report contains the most comprehensive TCR and BCR data set from human pLN, spleen, and islet tissues from T1D donors available to date.…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…Previous efforts to characterize the TCR repertoire in T1D subjects have been limited to tissues obtained from few or even a mere single organ donor (12,13) or were restricted to peripheral blood samples (14,37). Furthermore, BCR sequencing data in human samples is limited, particularly in subjects with T1D (15,16). Thus, to our knowledge, this report contains the most comprehensive TCR and BCR data set from human pLN, spleen, and islet tissues from T1D donors available to date.…”
Section: Discussionmentioning
confidence: 99%
“…Moreover, TCR overlap among pathogenic CD4 + effector T cells and protective Treg have yet to be investigated in human T1D. Likewise, B cell receptor (BCR) sequencing efforts have been limited overall (15,16) and, in particular, in patients with T1D (17), despite a known role for B cells in contributing to T1D through their capacity to present antigens (18).…”
Section: Molecules Technological Advances Including the Applicationmentioning
confidence: 99%
“…Metastatic cancer can now be monitored through deep sequencing of circulating tumor DNA [13], and the potential for poor DNA quality combined with deep sequencing requirements make PCR duplicates an important concern, especially if the results impact clinical decisions. Further, methods to study highly diverse mixtures like the immune repertoire [26][27][28] or viral heterogeneity [29] rely on accurate read depths to infer population dynamics. Our approach can also be applied to applications that require high accuracy of rare variant calls, such as in pooled populations or cancer, where SMTs have been used to group duplicate reads together in order to cancel out sequencing errors and obtain highly accurate variant calls [22].…”
Section: Discussionmentioning
confidence: 99%
“…The output consists (1) Fasta files: containing the CDRH3 sequences for each read and clonotype, as well as the sequence for each consensus lineage with a unique identifier. metrics include normalized clonal and lineages frequencies, global entropy measurements such as Shannon-Weaver index 18 and Gini coefficient 19,20 ( Fig. 1 and Fig.…”
Section: Outputmentioning
confidence: 99%