Immune correlates of early clearance ofMycobacterium tuberculosisamong tuberculosis household contacts in Indonesia

Author:

Setiabudiawan Todia P.ORCID,Apriani Lika,Verrall Ayesha J.,Utami Fitria,Schneider Marion,Indrati Agnes R.,Halim Pauline P.,Kaplonek Paulina,Malca Hadar,Lee Jessica Shih-Lu,Moorlag Simone J.C.F.M.,de Bree L. Charlotte J.,Mourits Vera P.,Joosten Leo A.B.,Netea Mihai G.,Alisjahbana Bachti,McNamara Ryan P.,Alter Galit,van Laarhoven Arjan,Ussher James E.,Sharples Katrina,Koeken Valerie A. C. M.,Hill Philip C.,van Crevel Reinout

Abstract

AbstractSome individuals, even when heavily exposed to an infectious tuberculosis patient, do not develop a specific T-cell response as measured by interferon-gamma release assay (IGRA). This could be explained by an IFN-γ-independent adaptive immune response, or an effective innate host response clearingMycobacterium tuberculosis (Mtb)without adaptive immunity. In heavily exposed Indonesian tuberculosis household contacts (n=1347), a persistently IGRA negative status was associated with presence of a BCG scar, and - especially among BCG-vaccinated individuals - with altered innate immune cells dynamics, higher heterologous (Escherichia coli-induced) proinflammatory cytokine production, and higher inflammatory proteins in the IGRA mitogen tube. Neither circulating concentrations ofMtb-specific antibodies nor functional antibody activity associated with IGRA status at baseline or follow-up. In a cohort of adults in a low tuberculosis incidence setting, BCG vaccination induced heterologous innate cytokine production, but only marginally affectedMtb-specific antibody profiles. Our findings suggest that a more efficient host innate immune response, rather than a humoral response, mediates early clearance ofMtb. The protective effect of BCG vaccination againstMtbinfection may be linked to innate immune priming, also termed ‘trained immunity’.

Publisher

Cold Spring Harbor Laboratory

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