Abstract
HIV-infected individuals are at high risk of tuberculosis disease and those with prior tuberculosis episodes are at even higher risk of disease recurrence. A non-sputum biomarker that identifies individuals at highest tuberculosis risk would allow targeted microbiological testing and appropriate treatment and also guide need for prolonged therapy. We determined the utility of a previously developed whole blood transcriptomic correlate of risk (COR) signature for (1) predicting incident recurrent tuberculosis, (2) tuberculosis diagnosis and (3) its potential utility for tuberculosis treatment monitoring in HIV-infected individuals. We retrieved cryopreserved blood specimens from three previously completed clinical studies and measured the COR signature by quantitative microfluidic real-time-PCR. The signature differentiated recurrent tuberculosis progressors from non-progressors within 3 months of diagnosis with an area under the Receiver-operating characteristic (ROC) curve (AUC) of 0.72 (95% confidence interval (CI), 0.58–0.85) amongst HIV-infected individuals on antiretroviral therapy (ART). Twenty-five of 43 progressors (58%) were asymptomatic at microbiological diagnosis and thus had subclinical disease. The signature showed excellent diagnostic discrimination between HIV-uninfected tuberculosis cases and controls (AUC 0.97; 95%CI 0.94–1). Performance was lower in HIV-infected individuals (AUC 0.83; 95%CI 0.81–0.96) and signature scores were directly associated with HIV viral loads. Tuberculosis treatment response in HIV-infected individuals on ART with a new recurrent tuberculosis diagnosis was also assessed. Signature scores decreased significantly during treatment. However, pre-treatment scores could not differentiate between those who became sputum negative before and after 2 months. Direct application of the unmodified blood transcriptomic COR signature detected subclinical and active tuberculosis by blind validation in HIV-infected individuals. However, prognostic performance for recurrent tuberculosis, and performance as diagnostic and as treatment monitoring tool in HIV-infected persons was inferior to published results from HIV-negative cohorts. Our results suggest that performance of transcriptomic signatures comprising interferon stimulated genes are negatively affected in HIV-infected individuals, especially in those with incompletely suppressed viral loads.
Highlights
Every year more than 10 million people develop tuberculosis (TB) disease, the leading infectious cause of death (World Health Organization [WHO], 2017b)
In this study we aimed to determine the prognostic value of this 11-gene COR signature for recurrent TB in people living with HIV who participated in the “TB Recurrence upon Treatment with HAART” (TRuTH) study conducted at the Centre for the Aids Programme of Research In South Africa (CAPRISA) in Durban, South Africa (Maharaj et al, 2017; Sivro et al, 2017)
Prognostic Cohort Among 520 participants in the longitudinal TRuTH study, 92 episodes of recurrent TB disease were recorded in 82 participants
Summary
Every year more than 10 million people develop tuberculosis (TB) disease, the leading infectious cause of death (World Health Organization [WHO], 2017b). Individuals who have had TB previously are at significantly increased risk of developing recurrent disease. Incidence of recurrence within the first year following completion of TB treatment is 2–8% (Friedrich et al, 2013; Gillespie et al, 2014; Merle et al, 2014), which is severalfold higher than the rate of incident TB disease in the same populations with no history of TB. Risk of recurrent TB disease was five times higher in HIV-infected South African gold miners relative to their HIV-uninfected colleagues (Mallory et al, 2000). And accurate identification of HIV-infected individuals who are at high risk of recurrent TB would allow targeted investigation for disease, facilitating earlier provision of antibiotic treatment
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