HLA-DR polymorphism in SARS-CoV-2 infection and susceptibility to symptomatic COVID-19

Stuart Astbury; Catherine J. Reynolds; David K. Butler; Diana C. Muñoz-Sandoval; Kai Min Lin; Franziska P. Pieper; Ashley Otter; Afroditi Kouraki; Lola Cusin; Jessica Nightingale; Amrita Vijay; Simon Craxford; Guruprasad P. Aithal; Patrick J. Tighe; Joseph M. Gibbons; Corinna Pade; George Joy; Mala Maini; Benny Chain; Amanda Semper; Timothy Brooks; Benjamin J. Ollivere; Áine McKnight; Mahdad Noursadeghi; Thomas A. Treibel; Charlotte Manisty; James C. Moon; Ana M. Valdes; Rosemary J. Boyton; Daniel M. Altmann; Hakam Abbass; Aderonke Abiodun; Mashael Alfarih; Zoe Alldis; Daniel M. Altmann; Oliver E. Amin; Mervyn Andiapen; Jessica Artico; João B. Augusto; Georgiana L. Baca; Sasha N.L. Bailey; Anish N. Bhuva; Alex Boulter; Ruth Bowles; Rosemary J. Boyton; Olivia V. Bracken; Ben O’Brien; Tim Brooks; Natalie Bullock; Jonathan Ball

doi:10.1111/imm.13450

HLA-DR polymorphism in SARS-CoV-2 infection and susceptibility to symptomatic COVID-19

Stuart Astbury, Catherine J. Reynolds, David K. Butler, Diana C. Muñoz-Sandoval, Kai Min Lin, Franziska P. Pieper, Ashley Otter, Afroditi Kouraki, Lola Cusin, Jessica Nightingale, Amrita Vijay, Simon Craxford, Guruprasad P. Aithal, Patrick J. Tighe, Joseph M. Gibbons, Corinna Pade, George Joy, Mala Maini, Benny Chain, Amanda SemperTimothy Brooks, Benjamin J. Ollivere, Áine McKnight, Mahdad Noursadeghi, Thomas A. Treibel, Charlotte Manisty, James C. Moon, Ana M. Valdes, Rosemary J. Boyton, Daniel M. Altmann, Hakam Abbass, Aderonke Abiodun, Mashael Alfarih, Zoe Alldis, Daniel M. Altmann, Oliver E. Amin, Mervyn Andiapen, Jessica Artico, João B. Augusto, Georgiana L. Baca, Sasha N.L. Bailey, Anish N. Bhuva, Alex Boulter, Ruth Bowles, Rosemary J. Boyton, Olivia V. Bracken, Ben O’Brien, Tim Brooks, Natalie Bullock, Jonathan Ball

Liverpool School of Tropical Medicine

Research output: Contribution to journal › Article › peer-review

28 Citations (Scopus)

Abstract

SARS-CoV-2 infection results in different outcomes ranging from asymptomatic infection to mild or severe disease and death. Reasons for this diversity of outcome include differences in challenge dose, age, gender, comorbidity and host genomic variation. Human leukocyte antigen (HLA) polymorphisms may influence immune response and disease outcome. We investigated the association of HLAII alleles with case definition symptomatic COVID-19, virus-specific antibody and T-cell immunity. A total of 1364 UK healthcare workers (HCWs) were recruited during the first UK SARS-CoV-2 wave and analysed longitudinally, encompassing regular PCR screening for infection, symptom reporting, imputation of HLAII genotype and analysis for antibody and T-cell responses to nucleoprotein (N) and spike (S). Of 272 (20%) HCW who seroconverted, the presence of HLA-DRB1*13:02 was associated with a 6·7-fold increased risk of case definition symptomatic COVID-19. In terms of immune responsiveness, HLA-DRB1*15:02 was associated with lower nucleocapsid T-cell responses. There was no association between DRB1 alleles and anti-spike antibody titres after two COVID vaccine doses. However, HLA DRB1*15:01 was associated with increased spike T-cell responses following both first and second dose vaccination. Trial registration: NCT04318314 and ISRCTN15677965.

Original language	English
Pages (from-to)	68-77
Number of pages	10
Journal	Immunology
Volume	166
Issue number	1
DOIs	https://doi.org/10.1111/imm.13450
Publication status	Published - 1 May 2022

Keywords

COVID-19
HLA
immunogenetics
SARS-CoV-2
T-cell immunity
vaccine

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1111/imm.13450Licence: CC BY

Cite this

Astbury, S., Reynolds, C. J., Butler, D. K., Muñoz-Sandoval, D. C., Lin, K. M., Pieper, F. P., Otter, A., Kouraki, A., Cusin, L., Nightingale, J., Vijay, A., Craxford, S., Aithal, G. P., Tighe, P. J., Gibbons, J. M., Pade, C., Joy, G., Maini, M., Chain, B., ... Ball, J. (2022). HLA-DR polymorphism in SARS-CoV-2 infection and susceptibility to symptomatic COVID-19. Immunology, 166(1), 68-77. https://doi.org/10.1111/imm.13450

@article{85bbc230af184cf3b024dcb5d1ec6e1a,

title = "HLA-DR polymorphism in SARS-CoV-2 infection and susceptibility to symptomatic COVID-19",

abstract = "SARS-CoV-2 infection results in different outcomes ranging from asymptomatic infection to mild or severe disease and death. Reasons for this diversity of outcome include differences in challenge dose, age, gender, comorbidity and host genomic variation. Human leukocyte antigen (HLA) polymorphisms may influence immune response and disease outcome. We investigated the association of HLAII alleles with case definition symptomatic COVID-19, virus-specific antibody and T-cell immunity. A total of 1364 UK healthcare workers (HCWs) were recruited during the first UK SARS-CoV-2 wave and analysed longitudinally, encompassing regular PCR screening for infection, symptom reporting, imputation of HLAII genotype and analysis for antibody and T-cell responses to nucleoprotein (N) and spike (S). Of 272 (20\%) HCW who seroconverted, the presence of HLA-DRB1*13:02 was associated with a 6·7-fold increased risk of case definition symptomatic COVID-19. In terms of immune responsiveness, HLA-DRB1*15:02 was associated with lower nucleocapsid T-cell responses. There was no association between DRB1 alleles and anti-spike antibody titres after two COVID vaccine doses. However, HLA DRB1*15:01 was associated with increased spike T-cell responses following both first and second dose vaccination. Trial registration: NCT04318314 and ISRCTN15677965.",

keywords = "COVID-19, HLA, immunogenetics, SARS-CoV-2, T-cell immunity, vaccine",

author = "Stuart Astbury and Reynolds, \{Catherine J.\} and Butler, \{David K.\} and Mu{\~n}oz-Sandoval, \{Diana C.\} and Lin, \{Kai Min\} and Pieper, \{Franziska P.\} and Ashley Otter and Afroditi Kouraki and Lola Cusin and Jessica Nightingale and Amrita Vijay and Simon Craxford and Aithal, \{Guruprasad P.\} and Tighe, \{Patrick J.\} and Gibbons, \{Joseph M.\} and Corinna Pade and George Joy and Mala Maini and Benny Chain and Amanda Semper and Timothy Brooks and Ollivere, \{Benjamin J.\} and {\'A}ine McKnight and Mahdad Noursadeghi and Treibel, \{Thomas A.\} and Charlotte Manisty and Moon, \{James C.\} and Valdes, \{Ana M.\} and Boyton, \{Rosemary J.\} and Altmann, \{Daniel M.\} and Hakam Abbass and Aderonke Abiodun and Mashael Alfarih and Zoe Alldis and Altmann, \{Daniel M.\} and Amin, \{Oliver E.\} and Mervyn Andiapen and Jessica Artico and Augusto, \{Jo{\~a}o B.\} and Baca, \{Georgiana L.\} and Bailey, \{Sasha N.L.\} and Bhuva, \{Anish N.\} and Alex Boulter and Ruth Bowles and Boyton, \{Rosemary J.\} and Bracken, \{Olivia V.\} and Ben O{\textquoteright}Brien and Tim Brooks and Natalie Bullock and Jonathan Ball",

year = "2022",

month = may,

day = "1",

doi = "10.1111/imm.13450",

language = "English",

volume = "166",

pages = "68--77",

journal = "Immunology",

issn = "0019-2805",

publisher = "Wiley-Blackwell Publishing Ltd",

number = "1",

}

Astbury, S, Reynolds, CJ, Butler, DK, Muñoz-Sandoval, DC, Lin, KM, Pieper, FP, Otter, A, Kouraki, A, Cusin, L, Nightingale, J, Vijay, A, Craxford, S, Aithal, GP, Tighe, PJ, Gibbons, JM, Pade, C, Joy, G, Maini, M, Chain, B, Semper, A, Brooks, T, Ollivere, BJ, McKnight, Á, Noursadeghi, M, Treibel, TA, Manisty, C, Moon, JC, Valdes, AM, Boyton, RJ, Altmann, DM, Abbass, H, Abiodun, A, Alfarih, M, Alldis, Z, Altmann, DM, Amin, OE, Andiapen, M, Artico, J, Augusto, JB, Baca, GL, Bailey, SNL, Bhuva, AN, Boulter, A, Bowles, R, Boyton, RJ, Bracken, OV, O’Brien, B, Brooks, T, Bullock, N & Ball, J 2022, 'HLA-DR polymorphism in SARS-CoV-2 infection and susceptibility to symptomatic COVID-19', Immunology, vol. 166, no. 1, pp. 68-77. https://doi.org/10.1111/imm.13450

TY - JOUR

T1 - HLA-DR polymorphism in SARS-CoV-2 infection and susceptibility to symptomatic COVID-19

AU - Astbury, Stuart

AU - Reynolds, Catherine J.

AU - Butler, David K.

AU - Muñoz-Sandoval, Diana C.

AU - Lin, Kai Min

AU - Pieper, Franziska P.

AU - Otter, Ashley

AU - Kouraki, Afroditi

AU - Cusin, Lola

AU - Nightingale, Jessica

AU - Vijay, Amrita

AU - Craxford, Simon

AU - Aithal, Guruprasad P.

AU - Tighe, Patrick J.

AU - Gibbons, Joseph M.

AU - Pade, Corinna

AU - Joy, George

AU - Maini, Mala

AU - Chain, Benny

AU - Semper, Amanda

AU - Brooks, Timothy

AU - Ollivere, Benjamin J.

AU - McKnight, Áine

AU - Noursadeghi, Mahdad

AU - Treibel, Thomas A.

AU - Manisty, Charlotte

AU - Moon, James C.

AU - Valdes, Ana M.

AU - Boyton, Rosemary J.

AU - Altmann, Daniel M.

AU - Abbass, Hakam

AU - Abiodun, Aderonke

AU - Alfarih, Mashael

AU - Alldis, Zoe

AU - Altmann, Daniel M.

AU - Amin, Oliver E.

AU - Andiapen, Mervyn

AU - Artico, Jessica

AU - Augusto, João B.

AU - Baca, Georgiana L.

AU - Bailey, Sasha N.L.

AU - Bhuva, Anish N.

AU - Boulter, Alex

AU - Bowles, Ruth

AU - Boyton, Rosemary J.

AU - Bracken, Olivia V.

AU - O’Brien, Ben

AU - Brooks, Tim

AU - Bullock, Natalie

AU - Ball, Jonathan

PY - 2022/5/1

Y1 - 2022/5/1

N2 - SARS-CoV-2 infection results in different outcomes ranging from asymptomatic infection to mild or severe disease and death. Reasons for this diversity of outcome include differences in challenge dose, age, gender, comorbidity and host genomic variation. Human leukocyte antigen (HLA) polymorphisms may influence immune response and disease outcome. We investigated the association of HLAII alleles with case definition symptomatic COVID-19, virus-specific antibody and T-cell immunity. A total of 1364 UK healthcare workers (HCWs) were recruited during the first UK SARS-CoV-2 wave and analysed longitudinally, encompassing regular PCR screening for infection, symptom reporting, imputation of HLAII genotype and analysis for antibody and T-cell responses to nucleoprotein (N) and spike (S). Of 272 (20%) HCW who seroconverted, the presence of HLA-DRB1*13:02 was associated with a 6·7-fold increased risk of case definition symptomatic COVID-19. In terms of immune responsiveness, HLA-DRB1*15:02 was associated with lower nucleocapsid T-cell responses. There was no association between DRB1 alleles and anti-spike antibody titres after two COVID vaccine doses. However, HLA DRB1*15:01 was associated with increased spike T-cell responses following both first and second dose vaccination. Trial registration: NCT04318314 and ISRCTN15677965.

AB - SARS-CoV-2 infection results in different outcomes ranging from asymptomatic infection to mild or severe disease and death. Reasons for this diversity of outcome include differences in challenge dose, age, gender, comorbidity and host genomic variation. Human leukocyte antigen (HLA) polymorphisms may influence immune response and disease outcome. We investigated the association of HLAII alleles with case definition symptomatic COVID-19, virus-specific antibody and T-cell immunity. A total of 1364 UK healthcare workers (HCWs) were recruited during the first UK SARS-CoV-2 wave and analysed longitudinally, encompassing regular PCR screening for infection, symptom reporting, imputation of HLAII genotype and analysis for antibody and T-cell responses to nucleoprotein (N) and spike (S). Of 272 (20%) HCW who seroconverted, the presence of HLA-DRB1*13:02 was associated with a 6·7-fold increased risk of case definition symptomatic COVID-19. In terms of immune responsiveness, HLA-DRB1*15:02 was associated with lower nucleocapsid T-cell responses. There was no association between DRB1 alleles and anti-spike antibody titres after two COVID vaccine doses. However, HLA DRB1*15:01 was associated with increased spike T-cell responses following both first and second dose vaccination. Trial registration: NCT04318314 and ISRCTN15677965.

KW - COVID-19

KW - HLA

KW - immunogenetics

KW - SARS-CoV-2

KW - T-cell immunity

KW - vaccine

U2 - 10.1111/imm.13450

DO - 10.1111/imm.13450

M3 - Article

SN - 0019-2805

VL - 166

SP - 68

EP - 77

JO - Immunology

JF - Immunology

IS - 1

ER -

HLA-DR polymorphism in SARS-CoV-2 infection and susceptibility to symptomatic COVID-19

Abstract

Keywords

UN SDGs

Access to Document

Fingerprint

Cite this