BibTex format
@article{Rowntree:2025:10.1073/pnas.2503145122,
author = {Rowntree, LC and Allen, LF and Hagen, RR and McQuilten, HA and Quadeer, AA and Chaurasia, P and Kaewpreedee, P and Lee, KWK and Cohen, CA and Petersen, J and Littler, DR and Habel, JR and Zhang, W and Cheng, SMS and Chan, KKP and Kwok, JSY and Leung, KSM and Wu, JT and Lee, C-K and Davies, J and Pannaraj, PS and Kaity, Allen E and Thomas, PG and Tosif, S and Crawford, NW and Lappas, M and Thevarajan, I and Lewin, SR and Kent, SJ and Juno, JA and Bond, KA and Williamson, DA and Holmes, NE and Smibert, OC and Gordon, CL and Trubiano, JA and Kotsimbos, TC and Cheng, AC and Efstathiou, C and Turtle, L and Thwaites, RS and Brightling, CE and PHOSP-COVID, Collaborative Group and Rossjohn, J and McKay, MR and Tian, J and Liu, WJ and Gao, GF and Xu, J and Sonehara, K and Ishii, KJ and Namkoong, H and Okada, Y and Peiris, M and Hui, DSC and Poon, LLM and Doherty, PC and Nguyen, THO and Valkenburg, SA and Kedzierska, K},
doi = {10.1073/pnas.2503145122},
journal = {Proceedings of the National Academy of Sciences of USA},
title = {HLA-B*15:01-positive severe COVID-19 patients lack CD8+ T cell pools with highly expanded public clonotypes},
url = {http://dx.doi.org/10.1073/pnas.2503145122},
volume = {122},
year = {2025}
}
RIS format (EndNote, RefMan)
TY - JOUR
AB - Understanding host factors driving asymptomatic versus severe disease outcomes is of key importance if we are to control emerging and re-emerging viral infections. HLA-B15:01 has been associated with asymptomatic SARS-CoV-2 infection in nonhospitalized individuals of European ancestry, with protective immunity attributed to preexisting cross-reactive CD8+ T-cells directed against HLA-B15:01-restricted Spike-derived S919-927 peptide (B15/S919+CD8+ T-cells). However, fundamental questions remained on the abundance and clonotypic nature of CD8+ T-cell responses in HLA-B15:01-positive patients who succumbed to life-threatening COVID-19. Here, we analyzed B15/S919+CD8+ T-cell responses in COVID-19 patients from independent HLA-typed COVID-19 patient cohorts across three continents, Australia, Asia and Europe. We assessed B15/S919+CD8+ T-cells in COVID-19 patients across disease outcomes ranging from asymptomatic to hospitalized critical illness. We found that severe/critical COVID-19 patients mounted B15/S919+CD8+ T-cell responses lacking a highly expanded key public B15/S919+CD8+ T-cell receptor (TCR; TRAV9-2/TRBV7-2) which recurred across multiple individuals in COVID-19 patients with a mild disease. Instead, B15/S919+CD8+ T-cell responses in life-threatening disease had a prevalence of an alternate TCR clonotypic motif (TRAV38-2/DV8/TRBV20-1), potentially contributing, at least in part, to why B15/S919+CD8+ T-cells in severe COVID-19 patients were less protective. Interestingly, the frequency, memory phenotype, and activation profiles of circulating B15/S919+CD8+ T-cells did not differ across disease severity. Moreover, B15/S919+CD8+ T-cells were better maintained into convalescence compared to other SARS-CoV-2-specificities. Our study thus provides evidence on the differential nature of the TCR clonal repertoire in 22.37% of HLA-B15:01-positive COVID-19 patients who developed severe or critical disease in our cohorts, comparing to HLA-B15:01-expressing individua
AU - Rowntree,LC
AU - Allen,LF
AU - Hagen,RR
AU - McQuilten,HA
AU - Quadeer,AA
AU - Chaurasia,P
AU - Kaewpreedee,P
AU - Lee,KWK
AU - Cohen,CA
AU - Petersen,J
AU - Littler,DR
AU - Habel,JR
AU - Zhang,W
AU - Cheng,SMS
AU - Chan,KKP
AU - Kwok,JSY
AU - Leung,KSM
AU - Wu,JT
AU - Lee,C-K
AU - Davies,J
AU - Pannaraj,PS
AU - Kaity,Allen E
AU - Thomas,PG
AU - Tosif,S
AU - Crawford,NW
AU - Lappas,M
AU - Thevarajan,I
AU - Lewin,SR
AU - Kent,SJ
AU - Juno,JA
AU - Bond,KA
AU - Williamson,DA
AU - Holmes,NE
AU - Smibert,OC
AU - Gordon,CL
AU - Trubiano,JA
AU - Kotsimbos,TC
AU - Cheng,AC
AU - Efstathiou,C
AU - Turtle,L
AU - Thwaites,RS
AU - Brightling,CE
AU - PHOSP-COVID,Collaborative Group
AU - Rossjohn,J
AU - McKay,MR
AU - Tian,J
AU - Liu,WJ
AU - Gao,GF
AU - Xu,J
AU - Sonehara,K
AU - Ishii,KJ
AU - Namkoong,H
AU - Okada,Y
AU - Peiris,M
AU - Hui,DSC
AU - Poon,LLM
AU - Doherty,PC
AU - Nguyen,THO
AU - Valkenburg,SA
AU - Kedzierska,K
DO - 10.1073/pnas.2503145122
PY - 2025///
SN - 0027-8424
TI - HLA-B15:01-positive severe COVID-19 patients lack CD8+ T cell pools with highly expanded public clonotypes
T2 - Proceedings of the National Academy of Sciences of USA
UR - http://dx.doi.org/10.1073/pnas.2503145122
UR - https://www.ncbi.nlm.nih.gov/pubmed/40892914
UR - https://www.pnas.org/doi/10.1073/pnas.2503145122
VL - 122
ER -
