Distinctive TCR repertoire in PIMS-TS/MIS-C patients: possible thymus involvement

Diana C. Yanez 1
Jasmine Rowell 1
Maximillian Woodall 1
Stuart Adams 2
Lauran O’Neill 2
Konstantinos Mengrelis 1
Ching-In Lau 1
Susan Ross 1
Sarah Benkenstein 2
Kate Plant 2
Claire M. Smith 1
Benny Chain 3
Mark J. Peters 1, 2
Tessa Crompton 1
1
 
UCL Great Ormond Street Institute of Child Health, 30 Guilford Street , London ,
2
 
Great Ormond Street Hospital , London ,
Publication typeJournal Article
Publication date2025-05-04
scimago Q1
wos Q2
SJR1.308
CiteScore7.5
Impact factor3.8
ISSN00099104, 13652249
Abstract

During the COVID-19 pandemic a rare new paediatric inflammatory condition (paediatric inflammatory multisystem syndrome temporally associated with COVID-19 (PIMS-TS)/MIS-C) was identified which correlated with previous or recent SARS-CoV-2 infection. PIMS-TS led to severe multi-organ inflammation, suggestive of disruption of central tolerance and thymus function. Here we investigated the possible role of the thymus in paediatric PIMS-TS. We confirmed that human thymus explants can be infected with SARS-CoV-2 in vitro. Comparison of T-cell populations in blood from PIMS-TS patients and age-matched healthy control children showed that although the overall proportions of CD4 and CD8 T-cell populations were decreased in PIMS-TS patients, the proportion of naïve cells in the CD4 population was higher in the PIMS-TS group. In PIMS-TS patients, the number of TREC in PBMC correlated strongly with the proportion of naive CD4 and CD8 T-cells, whereas this correlation was not present in healthy children. Sequencing rearranged TCRα and TCRβ transcripts from FACS-sorted CD4+CD8-CD3+ and CD4-CD8+CD3+ from blood from PIMS-TS, healthy children, and additionally paediatric severe COVID-19 patients, showed that while all three groups showed similar diversity and distribution, the repertoire of the PIMS-TS and COVID-19 groups had distinctive patterns of TCR gene segment usage and VJ combinatorial usage compared to healthy controls (TRBV11-2xTRBJ2-7, TRBV11-2xTRBJ1-1, TRBV11-2xTRBJ2-5, TRBV11-2xTRBJ2-1; TRBV29-1xTRBJ2-7, TRBV29-1xTRBJ1-1 enriched in PIMS-TS; TRBV7-9xTRBJ1-2, TRAV9-2xTRAJ30 and TRAV26-1xTRAJ39 enriched in COVID-19). The non-productive TCR rearrangements in the PIMS-TS group were also enriched for TRBV11-2, and showed bias towards distal (5’TRAV to 3’TRAJ) TCR gene segment usage, suggesting involvement of the thymus in PIMS-TS.

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Yanez D. C. et al. Distinctive TCR repertoire in PIMS-TS/MIS-C patients: possible thymus involvement // Clinical and Experimental Immunology. 2025.
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Yanez D. C., Rowell J., Woodall M., Adams S., O’Neill L., Mengrelis K., Lau C., Ross S., Benkenstein S., Plant K., Smith C. M., Chain B., Peters M. J., Crompton T. Distinctive TCR repertoire in PIMS-TS/MIS-C patients: possible thymus involvement // Clinical and Experimental Immunology. 2025.
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TY - JOUR
DO - 10.1093/cei/uxaf027
UR - https://academic.oup.com/cei/advance-article/doi/10.1093/cei/uxaf027/8126240
TI - Distinctive TCR repertoire in PIMS-TS/MIS-C patients: possible thymus involvement
T2 - Clinical and Experimental Immunology
AU - Yanez, Diana C.
AU - Rowell, Jasmine
AU - Woodall, Maximillian
AU - Adams, Stuart
AU - O’Neill, Lauran
AU - Mengrelis, Konstantinos
AU - Lau, Ching-In
AU - Ross, Susan
AU - Benkenstein, Sarah
AU - Plant, Kate
AU - Smith, Claire M.
AU - Chain, Benny
AU - Peters, Mark J.
AU - Crompton, Tessa
PY - 2025
DA - 2025/05/04
PB - Oxford University Press
SN - 0009-9104
SN - 1365-2249
ER -
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@article{2025_Yanez,
author = {Diana C. Yanez and Jasmine Rowell and Maximillian Woodall and Stuart Adams and Lauran O’Neill and Konstantinos Mengrelis and Ching-In Lau and Susan Ross and Sarah Benkenstein and Kate Plant and Claire M. Smith and Benny Chain and Mark J. Peters and Tessa Crompton},
title = {Distinctive TCR repertoire in PIMS-TS/MIS-C patients: possible thymus involvement},
journal = {Clinical and Experimental Immunology},
year = {2025},
publisher = {Oxford University Press},
month = {may},
url = {https://academic.oup.com/cei/advance-article/doi/10.1093/cei/uxaf027/8126240},
doi = {10.1093/cei/uxaf027}
}