Differential Immunodominance Hierarchy of CD8+ T-Cell Responses in HLA-B*27:05- and -B*27:02-Mediated Control of HIV-1 Infection

Emily Adland; Matilda Hill; Nora Lavandier; Anna Csala; Anne Edwards; Fabian Chen; Marek Radkowski; Justyna D Kowalska; Dimitrios Paraskevis; Angelos Hatzakis; Humberto Valenzuela-Ponce; Katja Pfafferott; Ian Williams; Pierre Pellegrino; Persephone Borrow; Masahiko Mori; Jürgen Rockstroh; Julia G Prado; Beatriz Mothe; Judith Dalmau; Javier Martinez-Picado; Gareth Tudor-Williams; John Frater; Anette Stryhn; Soren Buus; Gustavo Reyes Teran; Simon Mallal; Mina John; Susan Buchbinder; Gregory Kirk; Jeffrey Martin; Nelson Michael; Jacques Fellay; Steve Deeks; Bruce Walker; Santiago Avila-Rios; David Cole; Christian Brander; Mary Carrington; Philip Goulder

doi:10.1128/JVI.01685-17

Differential Immunodominance Hierarchy of CD8⁺ T-Cell Responses in HLA-B27:05- and -B27:02-Mediated Control of HIV-1 Infection

J Virol. 2018 Jan 30;92(4):e01685-17. doi: 10.1128/JVI.01685-17. Print 2018 Feb 15.

Authors

Emily Adland¹, Matilda Hill¹, Nora Lavandier¹, Anna Csala¹, Anne Edwards², Fabian Chen³, Marek Radkowski⁴, Justyna D Kowalska⁴, Dimitrios Paraskevis⁵, Angelos Hatzakis⁵, Humberto Valenzuela-Ponce⁶, Katja Pfafferott⁷, Ian Williams⁸, Pierre Pellegrino⁸, Persephone Borrow⁷, Masahiko Mori¹, Jürgen Rockstroh⁹, Julia G Prado¹⁰, Beatriz Mothe^{10

11}, Judith Dalmau¹⁰, Javier Martinez-Picado^{10

11

12}, Gareth Tudor-Williams¹³, John Frater^{7

14}, Anette Stryhn¹⁵, Soren Buus¹⁵, Gustavo Reyes Teran⁶, Simon Mallal¹⁶, Mina John¹⁷, Susan Buchbinder¹⁸, Gregory Kirk¹⁹, Jeffrey Martin²⁰, Nelson Michael²¹, Jacques Fellay²², Steve Deeks¹⁸, Bruce Walker²³, Santiago Avila-Rios⁶, David Cole^{24

25}, Christian Brander^{10

11

12}, Mary Carrington^{23

26}, Philip Goulder²⁷

Affiliations

¹ Department of Paediatrics, University of Oxford, United Kingdom.
² Department of GU Medicine, The Churchill Hospital, Oxford University NHS Foundation Trust, Oxford, United Kingdom.
³ Department of Sexual Health, Royal Berkshire Hospital, Reading, United Kingdom.
⁴ Department of Immunopathology of Infectious and Parasitic Diseases, Hospital for Infectious Diseases, Medical University of Warsaw, Warsaw, Poland.
⁵ Medical School, National and Kapodistrian University of Athens, Athens, Greece.
⁶ Centre for Research in Infectious Diseases, National Institute of Respiratory Diseases, Mexico City, Mexico.
⁷ Nuffield Department of Medicine, University of Oxford, Oxford, United Kingdom.
⁸ Centre for Sexual Health and HIV Research, Mortimer Market Centre, London, United Kingdom.
⁹ Department of Medicine I, University Hospital Bonn, Bonn, Germany.
¹⁰ AIDS Research Institute IrsiCaixa, Institut d'Investigació en Ciències de la Salut Germans Trias i Pujol (IGTP), Universitat Autònoma de Barcelona, Badalona, Spain.
¹¹ University of Vic-Central University of Catalonia (UVic-UCC), Vic, Barcelona, Spain.
¹² Institució Catalana de Recerca i Estudis Avançats (ICREA), Barcelona, Spain.
¹³ Department of Paediatrics, Imperial College, London, United Kingdom.
¹⁴ Oxford Martin School, University of Oxford, Oxford, United Kingdom.
¹⁵ Department of Immunology and Microbiology, University of Copenhagen, Copenhagen, Denmark.
¹⁶ Department of Medicine, Vanderbilt University Medical Center, Nashville, Tennessee, USA.
¹⁷ Institute of Immunology and Infectious Diseases, Murdoch University, Perth, Australia.
¹⁸ San Francisco Department of Public Health, HIV Research Section, San Francisco, California, USA.
¹⁹ Department of Epidemiology, Johns Hopkins University, Bloomberg School of Public Health, Baltimore, Maryland, USA.
²⁰ Department of Epidemiology and Biostatistics, University of California, San Francisco, California, USA.
²¹ U.S. Military HIV Research Program, Walter Reed Army Institute of Research, Silver Spring, Maryland, USA.
²² School of Life Sciences, EPFL, Lausanne, Switzerland.
²³ Ragon Institute of MGH, MIT and Harvard, Boston, Massachusetts, USA.
²⁴ Cardiff University School of Medicine, Heath Park, Cardiff, United Kingdom.
²⁵ Immunocore Limited, Abingdon, Oxfordshire, United Kingdom.
²⁶ Cancer and Inflammation Program, Leidos Biomedical Research, Frederick National Laboratory for Cancer Research, Maryland, USA.
²⁷ Department of Paediatrics, University of Oxford, United Kingdom philip.goulder@paediatrics.ox.ac.uk.

Abstract

The well-characterized association between HLA-B*27:05 and protection against HIV disease progression has been linked to immunodominant HLA-B*27:05-restricted CD8⁺ T-cell responses toward the conserved Gag KK10 (residues 263 to 272) and polymerase (Pol) KY9 (residues 901 to 909) epitopes. We studied the impact of the 3 amino acid differences between HLA-B*27:05 and the closely related HLA-B*27:02 on the HIV-specific CD8⁺ T-cell response hierarchy and on immune control of HIV. Genetic epidemiological data indicate that both HLA-B*27:02 and HLA-B*27:05 are associated with slower disease progression and lower viral loads. The effect of HLA-B*27:02 appeared to be consistently stronger than that of HLA-B*27:05. In contrast to HLA-B*27:05, the immunodominant HIV-specific HLA-B*27:02-restricted CD8⁺ T-cell response is to a Nef epitope (residues 142 to 150 [VW9]), with Pol KY9 subdominant and Gag KK10 further subdominant. This selection was driven by structural differences in the F pocket, mediated by a polymorphism between these two HLA alleles at position 81. Analysis of autologous virus sequences showed that in HLA-B*27:02-positive subjects, all three of these CD8⁺ T-cell responses impose selection pressure on the virus, whereas in HLA-B*27:05-positive subjects, there is no Nef VW9-mediated selection pressure. These studies demonstrate that HLA-B*27:02 mediates protection against HIV disease progression that is at least as strong as or stronger than that mediated by HLA-B*27:05. In combination with the protective Gag KK10 and Pol KY9 CD8⁺ T-cell responses that dominate HIV-specific CD8⁺ T-cell activity in HLA-B*27:05-positive subjects, a Nef VW9-specific response is additionally present and immunodominant in HLA-B*27:02-positive subjects, mediated through a polymorphism at residue 81 in the F pocket, that contributes to selection pressure against HIV.IMPORTANCE CD8⁺ T cells play a central role in successful control of HIV infection and have the potential also to mediate the eradication of viral reservoirs of infection. The principal means by which protective HLA class I molecules, such as HLA-B*27:05 and HLA-B*57:01, slow HIV disease progression is believed to be via the particular HIV-specific CD8⁺ T cell responses restricted by those alleles. We focus here on HLA-B*27:05, one of the best-characterized protective HLA molecules, and the closely related HLA-B*27:02, which differs by only 3 amino acids and which has not been well studied in relation to control of HIV infection. We show that HLA-B*27:02 is also protective against HIV disease progression, but the CD8⁺ T-cell immunodominance hierarchy of HLA-B*27:02 differs strikingly from that of HLA-B*27:05. These findings indicate that the immunodominant HLA-B*27:02-restricted Nef response adds to protection mediated by the Gag and Pol specificities that dominate anti-HIV CD8⁺ T-cell activity in HLA-B*27:05-positive subjects.

Keywords: CD8+ T cell; HIV Gag; HIV Nef; HLA; HLA-B*27; human immunodeficiency virus.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

CD8-Positive T-Lymphocytes / immunology*
Genes, MHC Class I
HIV Infections / immunology*
HIV Infections / virology
HIV-1
HLA-B27 Antigen / genetics*
Humans
Immunodominant Epitopes / immunology*
Viral Load
gag Gene Products, Human Immunodeficiency Virus / genetics*
nef Gene Products, Human Immunodeficiency Virus / genetics*

Substances

HLA-B*27:05 antigen
HLA-B27 Antigen
Immunodominant Epitopes
gag Gene Products, Human Immunodeficiency Virus
nef Gene Products, Human Immunodeficiency Virus

Abstract

Publication types

MeSH terms

Substances

Grants and funding