Abstract
Paradoxical tuberculosis-associated immune reconstitution inflammatory syndrome (TB-IRIS) is an aberrant inflammatory response occurring in a subset of TB-HIV co-infected patients initiating anti-retroviral therapy (ART). Here, we examined monocyte activation by prospectively quantitating pro-inflammatory plasma markers and monocyte subsets in TB-HIV co-infected patients from a South Indian cohort at baseline and following ART initiation at the time of IRIS, or at equivalent time points in non-IRIS controls. Pro-inflammatory biomarkers of innate and myeloid cell activation were increased in plasma of IRIS patients pre-ART and at the time of IRIS; this association was confirmed in a second cohort in South Africa. Increased expression of these markers correlated with elevated antigen load as measured by higher sputum culture grade and shorter duration of anti-TB therapy. Phenotypic analysis revealed the frequency of CD14++CD16− monocytes was an independent predictor of TB-IRIS, and was closely associated with plasma levels of CRP, TNF, IL-6 and tissue factor during IRIS. In addition, production of inflammatory cytokines by monocytes was higher in IRIS patients compared to controls pre-ART. These data point to a major role of mycobacterial antigen load and myeloid cell hyperactivation in the pathogenesis of TB-IRIS, and implicate monocytes and monocyte-derived cytokines as potential targets for TB-IRIS prevention or treatment.
Highlights
Implementation of antiretroviral therapy (ART) in patients coinfected with HIV and tuberculosis (TB) has greatly improved life expectancy [1,2,3,4,5]
tuberculosis-associated immune reconstitution inflammatory syndrome (TB-IRIS) has been clearly shown to be associated with elevated plasma concentrations of several pro-inflammatory and anti-inflammatory cytokines [20], some of them known to be strongly linked to monocyte stimulation
Our findings revealed distinct differences in monocyte subsets between individuals who developed paradoxical TB-IRIS compared to those who did not, which were strongly linked to the profound inflammatory milieu of IRIS
Summary
Implementation of antiretroviral therapy (ART) in patients coinfected with HIV and tuberculosis (TB) has greatly improved life expectancy [1,2,3,4,5]. Anti-retroviral therapy reconstitutes the number and function of CD4+ T-cells and most patients manifest clinical improvement of signs and symptoms of opportunistic co-infections including tuberculosis (TB). Some patients experience a paradoxical worsening of TB during the first 3 months of ART, a phenomenon known as immune reconstitution inflammatory syndrome or IRIS [6,7,8]. The clinical manifestations can range from fever and lymph node enlargement to sepsis-like syndrome and neurological deterioration [7].
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