Identification of human progenitors of exhausted CD8+ T cells associated with elevated IFN-γ response in early phase of viral infection

Curtis Cai; Jerome Samir; Mehdi R. Pirozyan; Thiruni N. Adikari; Money Gupta; Preston Leung; Brendan Hughes; Willem Van der Byl; Simone Rizzetto; Auda Elthala; Elizabeth Keoshkerian; Jean Louis Palgen; Timothy Peters; Thi H.O. Nguyen; Raymond Louie; Katherine Kedzierska; Silvana Gaudieri; Rowena A. Bull; Andrew R. Lloyd; Fabio Luciani

doi:10.1038/s41467-022-35281-7

Identification of human progenitors of exhausted CD8⁺ T cells associated with elevated IFN-γ response in early phase of viral infection

Curtis Cai, Jerome Samir, Mehdi R. Pirozyan, Thiruni N. Adikari, Money Gupta, Preston Leung, Brendan Hughes, Willem Van der Byl, Simone Rizzetto, Auda Elthala, Elizabeth Keoshkerian, Jean Louis Palgen, Timothy Peters, Thi H.O. Nguyen, Raymond Louie, Katherine Kedzierska, Silvana Gaudieri, Rowena A. Bull, Andrew R. Lloyd, Fabio Luciani

School of Human Sciences

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

10 Citations (Scopus)

Abstract

T cell exhaustion is a hallmark of hepatitis C virus (HCV) infection and limits protective immunity in chronic viral infections and cancer. Limited knowledge exists of the initial viral and immune dynamics that characterise exhaustion in humans. We studied longitudinal blood samples from a unique cohort of individuals with primary infection using single-cell multi-omics to identify the functions and phenotypes of HCV-specific CD8⁺ T cells. Early elevated IFN-γ response against the transmitted virus is associated with the rate of immune escape, larger clonal expansion, and early onset of exhaustion. Irrespective of disease outcome, we find heterogeneous subsets of progenitors of exhaustion, based on the level of PD-1 expression and loss of AP-1 transcription factors. Intra-clonal analysis shows distinct trajectories with multiple fates and evolutionary plasticity of precursor cells. These findings challenge the current paradigm on the contribution of CD8⁺ T cells to HCV disease outcome and provide data for future studies on T cell differentiation in human infections.

Original language	English
Article number	7543
Journal	Nature Communications
Volume	13
Issue number	1
DOIs	https://doi.org/10.1038/s41467-022-35281-7
Publication status	Published - Dec 2022

UN SDGs

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

Access to Document

10.1038/s41467-022-35281-7Licence: CC BY

Cite this

Cai, C., Samir, J., Pirozyan, M. R., Adikari, T. N., Gupta, M., Leung, P., Hughes, B., Van der Byl, W., Rizzetto, S., Elthala, A., Keoshkerian, E., Palgen, J. L., Peters, T., Nguyen, T. H. O., Louie, R., Kedzierska, K., Gaudieri, S., Bull, R. A., Lloyd, A. R., & Luciani, F. (2022). Identification of human progenitors of exhausted CD8⁺ T cells associated with elevated IFN-γ response in early phase of viral infection. Nature Communications, 13(1), Article 7543. https://doi.org/10.1038/s41467-022-35281-7

@article{be8f2ce952444bec970a43e1d917f287,

title = "Identification of human progenitors of exhausted CD8+ T cells associated with elevated IFN-γ response in early phase of viral infection",

abstract = "T cell exhaustion is a hallmark of hepatitis C virus (HCV) infection and limits protective immunity in chronic viral infections and cancer. Limited knowledge exists of the initial viral and immune dynamics that characterise exhaustion in humans. We studied longitudinal blood samples from a unique cohort of individuals with primary infection using single-cell multi-omics to identify the functions and phenotypes of HCV-specific CD8+ T cells. Early elevated IFN-γ response against the transmitted virus is associated with the rate of immune escape, larger clonal expansion, and early onset of exhaustion. Irrespective of disease outcome, we find heterogeneous subsets of progenitors of exhaustion, based on the level of PD-1 expression and loss of AP-1 transcription factors. Intra-clonal analysis shows distinct trajectories with multiple fates and evolutionary plasticity of precursor cells. These findings challenge the current paradigm on the contribution of CD8+ T cells to HCV disease outcome and provide data for future studies on T cell differentiation in human infections.",

author = "Curtis Cai and Jerome Samir and Pirozyan, {Mehdi R.} and Adikari, {Thiruni N.} and Money Gupta and Preston Leung and Brendan Hughes and {Van der Byl}, Willem and Simone Rizzetto and Auda Elthala and Elizabeth Keoshkerian and Palgen, {Jean Louis} and Timothy Peters and Nguyen, {Thi H.O.} and Raymond Louie and Katherine Kedzierska and Silvana Gaudieri and Bull, {Rowena A.} and Lloyd, {Andrew R.} and Fabio Luciani",

note = "Funding Information: The HITS-p and HITS-c investigators include Andrew Lloyd, Lisa Maher, Kate Dolan, Paul Haber, William Rawlinson, Carla Treloar and Greg Dore. Flow cytometry and sequencing were supported by staff at the UNSW Flow Cytometry and Ramaciotti Centre core facilities. This research was supported from National Health and Medical Research Council of Australia (NHMRC) - Project Nos. APP1121643, 1027551, 1060199, Partnership No. 1016351, and Programme Nos. 510488 and 1053206. The HITS-c cohort was supported by the UNSW Hepatitis C Vaccine Initiative and NHMRC Project Grant No. 630483. F.L., A.R.L. and R.A.B. are supported by NHMRC Research Fellowships (Numbers: 1128416, 1041897 and 1084706). M.R.P., P.L., and C.C. were supported by an Australian Government Research Training Programme (RTP) Scholarship. S.G. was supported by the NHMRC grant APP1148284. K.K. is supported by the NHMRC grant APP1148284. Leadership Investigator Grant (#1173871), T.H.O.N. is supported by NHMRC Emerging Leadership Level 1 Investigator Grant (#1194036). Publisher Copyright: {\textcopyright} 2022, The Author(s).",

year = "2022",

month = dec,

doi = "10.1038/s41467-022-35281-7",

language = "English",

volume = "13",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Publishing Group - Macmillan Publishers",

number = "1",

}

Cai, C, Samir, J, Pirozyan, MR, Adikari, TN, Gupta, M, Leung, P, Hughes, B, Van der Byl, W, Rizzetto, S, Elthala, A, Keoshkerian, E, Palgen, JL, Peters, T, Nguyen, THO, Louie, R, Kedzierska, K, Gaudieri, S, Bull, RA, Lloyd, AR & Luciani, F 2022, 'Identification of human progenitors of exhausted CD8⁺ T cells associated with elevated IFN-γ response in early phase of viral infection', Nature Communications, vol. 13, no. 1, 7543. https://doi.org/10.1038/s41467-022-35281-7

TY - JOUR

T1 - Identification of human progenitors of exhausted CD8+ T cells associated with elevated IFN-γ response in early phase of viral infection

AU - Cai, Curtis

AU - Samir, Jerome

AU - Pirozyan, Mehdi R.

AU - Adikari, Thiruni N.

AU - Gupta, Money

AU - Leung, Preston

AU - Hughes, Brendan

AU - Van der Byl, Willem

AU - Rizzetto, Simone

AU - Elthala, Auda

AU - Keoshkerian, Elizabeth

AU - Palgen, Jean Louis

AU - Peters, Timothy

AU - Nguyen, Thi H.O.

AU - Louie, Raymond

AU - Kedzierska, Katherine

AU - Gaudieri, Silvana

AU - Bull, Rowena A.

AU - Lloyd, Andrew R.

AU - Luciani, Fabio

N1 - Funding Information: The HITS-p and HITS-c investigators include Andrew Lloyd, Lisa Maher, Kate Dolan, Paul Haber, William Rawlinson, Carla Treloar and Greg Dore. Flow cytometry and sequencing were supported by staff at the UNSW Flow Cytometry and Ramaciotti Centre core facilities. This research was supported from National Health and Medical Research Council of Australia (NHMRC) - Project Nos. APP1121643, 1027551, 1060199, Partnership No. 1016351, and Programme Nos. 510488 and 1053206. The HITS-c cohort was supported by the UNSW Hepatitis C Vaccine Initiative and NHMRC Project Grant No. 630483. F.L., A.R.L. and R.A.B. are supported by NHMRC Research Fellowships (Numbers: 1128416, 1041897 and 1084706). M.R.P., P.L., and C.C. were supported by an Australian Government Research Training Programme (RTP) Scholarship. S.G. was supported by the NHMRC grant APP1148284. K.K. is supported by the NHMRC grant APP1148284. Leadership Investigator Grant (#1173871), T.H.O.N. is supported by NHMRC Emerging Leadership Level 1 Investigator Grant (#1194036). Publisher Copyright: © 2022, The Author(s).

PY - 2022/12

Y1 - 2022/12

N2 - T cell exhaustion is a hallmark of hepatitis C virus (HCV) infection and limits protective immunity in chronic viral infections and cancer. Limited knowledge exists of the initial viral and immune dynamics that characterise exhaustion in humans. We studied longitudinal blood samples from a unique cohort of individuals with primary infection using single-cell multi-omics to identify the functions and phenotypes of HCV-specific CD8+ T cells. Early elevated IFN-γ response against the transmitted virus is associated with the rate of immune escape, larger clonal expansion, and early onset of exhaustion. Irrespective of disease outcome, we find heterogeneous subsets of progenitors of exhaustion, based on the level of PD-1 expression and loss of AP-1 transcription factors. Intra-clonal analysis shows distinct trajectories with multiple fates and evolutionary plasticity of precursor cells. These findings challenge the current paradigm on the contribution of CD8+ T cells to HCV disease outcome and provide data for future studies on T cell differentiation in human infections.

AB - T cell exhaustion is a hallmark of hepatitis C virus (HCV) infection and limits protective immunity in chronic viral infections and cancer. Limited knowledge exists of the initial viral and immune dynamics that characterise exhaustion in humans. We studied longitudinal blood samples from a unique cohort of individuals with primary infection using single-cell multi-omics to identify the functions and phenotypes of HCV-specific CD8+ T cells. Early elevated IFN-γ response against the transmitted virus is associated with the rate of immune escape, larger clonal expansion, and early onset of exhaustion. Irrespective of disease outcome, we find heterogeneous subsets of progenitors of exhaustion, based on the level of PD-1 expression and loss of AP-1 transcription factors. Intra-clonal analysis shows distinct trajectories with multiple fates and evolutionary plasticity of precursor cells. These findings challenge the current paradigm on the contribution of CD8+ T cells to HCV disease outcome and provide data for future studies on T cell differentiation in human infections.

UR - http://www.scopus.com/inward/record.url?scp=85143509881&partnerID=8YFLogxK

U2 - 10.1038/s41467-022-35281-7

DO - 10.1038/s41467-022-35281-7

M3 - Article

C2 - 36477661

AN - SCOPUS:85143509881

SN - 2041-1723

VL - 13

JO - Nature Communications

JF - Nature Communications

IS - 1

M1 - 7543

ER -

Identification of human progenitors of exhausted CD8⁺ T cells associated with elevated IFN-γ response in early phase of viral infection

Abstract

UN SDGs

Access to Document

Other files and links

Fingerprint

Understanding pathogen effects on human T cell receptor diversity and function

Cite this

Identification of human progenitors of exhausted CD8+ T cells associated with elevated IFN-γ response in early phase of viral infection

Abstract

UN SDGs

Access to Document

Other files and links

Fingerprint

Projects

Understanding pathogen effects on human T cell receptor diversity and function

Cite this

Identification of human progenitors of exhausted CD8⁺ T cells associated with elevated IFN-γ response in early phase of viral infection