Specific Host Signatures for the Detection of Tuberculosis Infection in Children in a Low TB Incidence Country

Overview

Journal Front Immunol

Specialty Allergy & Immunology

Date 2021 Apr 1

PMID 33790886

Citations 1

Authors

Alexandra Dreesman

Veronique Corbiere

Myriam Libin

Judith Racape

Philippe Collart

Mahavir Singh

Camille Locht

Francoise Mascart

Violette Dirix

Affiliations

Soon will be listed here.

Abstract

Diagnosis of tuberculosis (TB) in children remains challenging due to unspecific clinical presentation and low bacillary load. In low TB incidence countries, most cases are diagnosed by a contact screening strategy after exposure to an index TB case. Due to the severity of TB in young children, the priority is to determine whether a child is infected or not, whereas differential diagnosis between active TB (aTB) and latent TB constitutes a second step. In Belgium, a low TB incidence country, we prospectively included 47 children with a defined infection status (12 children with aTB, 18 with latent TB, and 17 uninfected) (exploratory cohort), and determined the optimal combinations of cytokines secreted by their peripheral blood mononuclear cells in response to a 5-days stimulation with four different mycobacterial antigens, in an attempt to classify the children according to their infectious status. Correct identification of all infected children was obtained by several combinations of two purified protein derivative (PPD)-induced cytokines (IFN-γ and either GM-CSF, MIP-1α, sCD40L or TNF-α), or by combining PPD-induced IFN-γ with culture-filtrate protein-10 (CFP-10)-induced TNF-α. Alternatively, combining CFP-10-induced TNF-α and IP-10 with heparin-binding haemagglutinin (HBHA)-induced-IFN-γ was more effective in testing recently BCG-vaccinated children or those suspected to be infected with non-tuberculous mycobacteria, providing a correct classification of 97% of the infected children. This combination also correctly classified 98% of the children from a validation cohort comprising 40 infected children and 20 non-infected children. Further differentiation between aTB and children with latent TB was more difficult. Combining ESAT-6-induced MIP1-α and IP-10, CFP-10-induced MIG, and HBHA-induced MIG provided a correct classification of 77% of the children from the exploratory cohort but only of 57.5% of those from the validation cohort. We conclude that combining the measurement of 2-4 cytokines induced by three different mycobacterial antigens allows an excellent identification of infected children, whereas differentiating children with aTB from those with latent TB remains far from perfect.

Citing Articles

HBHA induces IL-10 from CD4+ T cells in patients with active tuberculosis but IFN-γ and IL-17 from individuals with infection.

Izumida M, Jobe H, Coker E, Barry A, Rashid M, Manneh I Front Immunol. 2024; 15:1422700.

PMID: 39257584 PMC: 11384583. DOI: 10.3389/fimmu.2024.1422700.

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