Author
Listed:
- Roshni Roy Chowdhury
(Stanford University School of Medicine
Stanford University School of Medicine)
- Francesco Vallania
(Stanford University School of Medicine
Stanford University School of Medicine)
- Qianting Yang
(Shenzhen Third People’s Hospital)
- Cesar Joel Lopez Angel
(Stanford University School of Medicine
Stanford University School of Medicine)
- Fatoumatta Darboe
(University of Cape Town
University of Cape Town)
- Adam Penn-Nicholson
(University of Cape Town
University of Cape Town)
- Virginie Rozot
(University of Cape Town
University of Cape Town)
- Elisa Nemes
(University of Cape Town
University of Cape Town)
- Stephanus T. Malherbe
(Stellenbosch University)
- Katharina Ronacher
(Stellenbosch University
Stellenbosch University
The University of Queensland)
- Gerhard Walzl
(Stellenbosch University
Stellenbosch University)
- Willem Hanekom
(University of Cape Town
University of Cape Town)
- Mark M. Davis
(Stanford University School of Medicine
Stanford University School of Medicine
Stanford University School of Medicine
Stanford University School of Medicine)
- Jill Winter
(Catalysis Foundation for Health)
- Xinchun Chen
(Shenzhen University School of Medicine)
- Thomas J. Scriba
(University of Cape Town
University of Cape Town)
- Purvesh Khatri
(Stanford University School of Medicine
Stanford University School of Medicine
Stanford University School of Medicine)
- Yueh-hsiu Chien
(Stanford University School of Medicine
Stanford University School of Medicine)
Abstract
Most infections with Mycobacterium tuberculosis (Mtb) manifest as a clinically asymptomatic, contained state, known as latent tuberculosis infection, that affects approximately one-quarter of the global population1. Although fewer than one in ten individuals eventually progress to active disease2, tuberculosis is a leading cause of death from infectious disease worldwide3. Despite intense efforts, immune factors that influence the infection outcomes remain poorly defined. Here we used integrated analyses of multiple cohorts to identify stage-specific host responses to Mtb infection. First, using high-dimensional mass cytometry analyses and functional assays of a cohort of South African adolescents, we show that latent tuberculosis is associated with enhanced cytotoxic responses, which are mostly mediated by CD16 (also known as FcγRIIIa) and natural killer cells, and continuous inflammation coupled with immune deviations in both T and B cell compartments. Next, using cell-type deconvolution of transcriptomic data from several cohorts of different ages, genetic backgrounds, geographical locations and infection stages, we show that although deviations in peripheral B and T cell compartments generally start at latency, they are heterogeneous across cohorts. However, an increase in the abundance of circulating natural killer cells in tuberculosis latency, with a corresponding decrease during active disease and a return to baseline levels upon clinical cure are features that are common to all cohorts. Furthermore, by analysing three longitudinal cohorts, we find that changes in peripheral levels of natural killer cells can inform disease progression and treatment responses, and inversely correlate with the inflammatory state of the lungs of patients with active tuberculosis. Together, our findings offer crucial insights into the underlying pathophysiology of tuberculosis latency, and identify factors that may influence infection outcomes.
Suggested Citation
Roshni Roy Chowdhury & Francesco Vallania & Qianting Yang & Cesar Joel Lopez Angel & Fatoumatta Darboe & Adam Penn-Nicholson & Virginie Rozot & Elisa Nemes & Stephanus T. Malherbe & Katharina Ronacher, 2018.
"A multi-cohort study of the immune factors associated with M. tuberculosis infection outcomes,"
Nature, Nature, vol. 560(7720), pages 644-648, August.
Handle:
RePEc:nat:nature:v:560:y:2018:i:7720:d:10.1038_s41586-018-0439-x
DOI: 10.1038/s41586-018-0439-x
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