Classical complement and inflammasome activation converge in CD14highCD16- monocytes in HIV associated TB-immune reconstitution inflammatory syndrome.
Silvia Lucena LageChun-Shu WongEduardo Pinheiro AmaralDaniel SturdevantDenise C HsuAdam RupertEleanor M P WilsonS Sonia QasbaNuha Sultana NaqviElizabeth LaidlawAndrea LiscoMaura ManionIrini SeretiPublished in: PLoS pathogens (2021)
Inflammasome-derived cytokines, IL-1β and IL-18, and complement cascade have been independently implicated in the pathogenesis of tuberculosis (TB)-immune reconstitution inflammatory syndrome (TB-IRIS), a complication affecting HIV+ individuals starting antiretroviral therapy (ART). Although sublytic deposition of the membrane attack complex (MAC) has been shown to promote NLRP3 inflammasome activation, it is unknown whether these pathways may cooperatively contribute to TB-IRIS. To evaluate the activation of inflammasome, peripheral blood mononuclear cells (PBMCs) from HIV-TB co-infected patients prior to ART and at the IRIS or equivalent timepoint were incubated with a probe used to assess active caspase-1/4/5 followed by screening of ASC (apoptosis-associated speck-like protein containing a CARD domain) specks as a readout of inflammasome activation by imaging flow cytometry. We found higher numbers of monocytes showing spontaneous caspase-1/4/5+ASC-speck formation in TB-IRIS compared to TB non-IRIS patients. Moreover, numbers of caspase-1/4/5+ASC-speck+ monocytes positively correlated with IL-1β/IL-18 plasma levels. Besides increased systemic levels of C1q and C5a, TB-IRIS patients also showed elevated C1q and C3 deposition on monocyte cell surface, suggesting aberrant classical complement activation. A clustering tSNE analysis revealed TB-IRIS patients are enriched in a CD14highCD16- monocyte population that undergoes MAC deposition and caspase-1/4/5 activation compared to TB non-IRIS patients, suggesting complement-associated inflammasome activation during IRIS events. Accordingly, PBMCs from patients were more sensitive to ex-vivo complement-mediated IL-1β secretion than healthy control cells in a NLRP3-dependent manner. Therefore, our data suggest complement-associated inflammasome activation may fuel the dysregulated TB-IRIS systemic inflammatory cascade and targeting this pathway may represent a novel therapeutic approach for IRIS or related inflammatory syndromes.
Keyphrases
- mycobacterium tuberculosis
- antiretroviral therapy
- end stage renal disease
- ejection fraction
- chronic kidney disease
- newly diagnosed
- nlrp inflammasome
- hiv infected
- cell death
- prognostic factors
- human immunodeficiency virus
- oxidative stress
- hiv positive
- peritoneal dialysis
- dendritic cells
- cell proliferation
- cell cycle arrest
- patient reported outcomes
- drug delivery
- mass spectrometry
- deep learning
- hiv testing
- cell surface
- machine learning
- artificial intelligence
- electronic health record
- men who have sex with men
- single cell
- cancer therapy
- living cells