Postnatal Expansion, Maturation, and Functionality of MR1T Cells in Humans

Gwendolyn M. Swarbrick; Gwendolyn M. Swarbrick; Anele Gela; Meghan E. Cansler; Megan D. Null; Rowan B. Duncan; Elisa Nemes; Muki Shey; Muki Shey; Mary Nsereko; Harriet Mayanja-Kizza; Harriet Mayanja-Kizza; Sarah Kiguli; Sarah Kiguli; Jeffrey Koh; Willem A. Hanekom; Mark Hatherill; Christina Lancioni; David M. Lewinsohn; David M. Lewinsohn; Thomas J. Scriba; Deborah A. Lewinsohn

doi:10.3389/fimmu.2020.556695

Frontiers in Immunology (Sep 2020)

Postnatal Expansion, Maturation, and Functionality of MR1T Cells in Humans

Gwendolyn M. Swarbrick,
Gwendolyn M. Swarbrick,
Anele Gela,
Meghan E. Cansler,
Megan D. Null,
Rowan B. Duncan,
Elisa Nemes,
Muki Shey,
Muki Shey,
Mary Nsereko,
Harriet Mayanja-Kizza,
Harriet Mayanja-Kizza,
Sarah Kiguli,
Sarah Kiguli,
Jeffrey Koh,
Willem A. Hanekom,
Mark Hatherill,
Christina Lancioni,
David M. Lewinsohn,
David M. Lewinsohn,
Thomas J. Scriba,
Deborah A. Lewinsohn

Affiliations

Gwendolyn M. Swarbrick: Division of Infectious Diseases, Department of Pediatrics, Oregon Health & Science University, Portland, OR, United States
Gwendolyn M. Swarbrick: Portland Veterans Administration Healthcare System, Portland, OR, United States
Anele Gela: South African Tuberculosis Vaccine Initiative, Institute of Infectious Disease and Molecular Medicine and Division of Immunology, Department of Pathology, University of Cape Town, Cape Town, South Africa
Meghan E. Cansler: Division of Infectious Diseases, Department of Pediatrics, Oregon Health & Science University, Portland, OR, United States
Megan D. Null: Division of Infectious Diseases, Department of Pediatrics, Oregon Health & Science University, Portland, OR, United States
Rowan B. Duncan: Division of Infectious Diseases, Department of Pediatrics, Oregon Health & Science University, Portland, OR, United States
Elisa Nemes: South African Tuberculosis Vaccine Initiative, Institute of Infectious Disease and Molecular Medicine and Division of Immunology, Department of Pathology, University of Cape Town, Cape Town, South Africa
Muki Shey: South African Tuberculosis Vaccine Initiative, Institute of Infectious Disease and Molecular Medicine and Division of Immunology, Department of Pathology, University of Cape Town, Cape Town, South Africa
Muki Shey: Department of Medicine & Wellcome Centre for Infectious Disease Research in Africa (CIDRI-Africa), Institute of Infectious Disease and Molecular Medicine, University of Cape Town, Cape Town, South Africa
Mary Nsereko: Uganda-CWRU Research Collaboration, Kampala, Uganda
Harriet Mayanja-Kizza: Uganda-CWRU Research Collaboration, Kampala, Uganda
Harriet Mayanja-Kizza: Department of Medicine, Makerere University, Kampala, Uganda
Sarah Kiguli: Uganda-CWRU Research Collaboration, Kampala, Uganda
Sarah Kiguli: Department of Paediatrics, Makerere University, Kampala, Uganda
Jeffrey Koh: Department of Anesthesiology and Perioperative Medicine, Oregon Health & Science University, Portland, OR, United States
Willem A. Hanekom: South African Tuberculosis Vaccine Initiative, Institute of Infectious Disease and Molecular Medicine and Division of Immunology, Department of Pathology, University of Cape Town, Cape Town, South Africa
Mark Hatherill: South African Tuberculosis Vaccine Initiative, Institute of Infectious Disease and Molecular Medicine and Division of Immunology, Department of Pathology, University of Cape Town, Cape Town, South Africa
Christina Lancioni: Division of Infectious Diseases, Department of Pediatrics, Oregon Health & Science University, Portland, OR, United States
David M. Lewinsohn: Portland Veterans Administration Healthcare System, Portland, OR, United States
David M. Lewinsohn: Division of Pulmonary and Critical Care Medicine, Department of Medicine, Oregon Health & Science University, Portland, OR, United States
Thomas J. Scriba: South African Tuberculosis Vaccine Initiative, Institute of Infectious Disease and Molecular Medicine and Division of Immunology, Department of Pathology, University of Cape Town, Cape Town, South Africa
Deborah A. Lewinsohn: Division of Infectious Diseases, Department of Pediatrics, Oregon Health & Science University, Portland, OR, United States

DOI: https://doi.org/10.3389/fimmu.2020.556695
Journal volume & issue: Vol. 11

Abstract

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MR1-restricted T (MR1T) cells are defined by their recognition of metabolite antigens presented by the monomorphic MHC class 1-related molecule, MR1, the most highly conserved MHC class I related molecule in mammalian species. Mucosal-associated invariant T (MAIT) cells are the predominant subset of MR1T cells expressing an invariant TCR α-chain, TRAV1-2. These cells comprise a T cell subset that recognizes and mediates host immune responses to a broad array of microbial pathogens, including Mycobacterium tuberculosis. Here, we sought to characterize development of circulating human MR1T cells as defined by MR1-5-OP-RU tetramer labeling and of the TRAV1-2+ MAIT cells defined by expression of TRAV1-2 and high expression of CD26 and CD161 (TRAV1-2+CD161++CD26++ cells). We analyzed postnatal expansion, maturation, and functionality of peripheral blood MR1-5-OP-RU tetramer+ MR1T cells in cohorts from three different geographic settings with different tuberculosis (TB) vaccination practices, levels of exposure to and infection with M. tuberculosis. Early after birth, frequencies of MR1-5-OP-RU tetramer+ MR1T cells increased rapidly by several fold. This coincided with the transition from a predominantly CD4+ and TRAV1-2− population in neonates, to a predominantly TRAV1-2+CD161++CD26++ CD8+ population. We also observed that tetramer+ MR1T cells that expressed TNF upon mycobacterial stimulation were very low in neonates, but increased ~10-fold in the first year of life. These functional MR1T cells in all age groups were MR1-5-OP-RU tetramer+TRAV1-2+ and highly expressed CD161 and CD26, markers that appeared to signal phenotypic and functional maturation of this cell subset. This age-associated maturation was also marked by the loss of naïve T cell markers on tetramer+ TRAV1-2+ MR1T cells more rapidly than tetramer+TRAV1-2− MR1T cells and non-MR1T cells. These data suggest that neonates have infrequent populations of MR1T cells with diverse phenotypic attributes; and that exposure to the environment rapidly and preferentially expands the MR1-5-OP-RU tetramer+TRAV1-2+ population of MR1T cells, which becomes the predominant population of functional MR1T cells early during childhood.

Published in Frontiers in Immunology

ISSN: 1664-3224 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: http://journal.frontiersin.org/journal/immunology

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