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On the viability of unsupervised T-cell receptor sequence clustering for epitope preference

Journal Contribution - Journal Article

Motivation The T-cell receptor (TCR) is responsible for recognizing epitopes presented on cell surfaces. Linking TCR sequences to their ability to target specific epitopes is currently an unsolved problem, yet one of great interest. Indeed, it is currently unknown how dissimilar TCR sequences can be before they no longer bind the same epitope. This question is confounded by the fact that there are many ways to define the similarity between two TCR sequences. Here we investigate both issues in the context of TCR sequence unsupervised clustering. Results We provide an overview of the performance of various distance metrics on two large independent data sets with 412 and 2835 TCR sequences respectively. Our results confirm the presence of structural distinct TCR groups that target identical epitopes. In addition, we put forward several recommendations to perform unsupervised T-cell receptor sequence clustering.

Journal: Bioinformatics

ISSN: 1367-4803

Volume: 35

Pages: 1461 - 1468

Publication year:2019

Keywords:A1 Journal article

WoS Id: 000469491000004
DOI: https://doi.org/10.1093/bioinformatics/bty821
Handle: https://hdl.handle.net/10067/1533860151162165141

BOF-keylabel:yes

BOF-publication weight:10

CSS-citation score:2

Authors from:Higher Education

Accessibility:Open

See also: On the viability of unsupervised T-cell receptor sequence clustering for epitope preference

Publication

On the viability of unsupervised T-cell receptor sequence clustering for epitope preference

Journal Contribution - Journal Article

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