Gut-derived bacterial toxins impair memory CD4+ T cell mitochondrial function in HIV-1 infection
Brian Ferrari, … , Rafick-Pierre Sekaly, Souheil-Antoine Younes
Brian Ferrari, … , Rafick-Pierre Sekaly, Souheil-Antoine Younes
Published March 22, 2022
Citation Information: J Clin Invest. 2022;132(9):e149571. https://doi.org/10.1172/JCI149571.
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Research Article AIDS/HIV Infectious disease

Gut-derived bacterial toxins impair memory CD4+ T cell mitochondrial function in HIV-1 infection

Abstract

People living with HIV (PLWH) who are immune nonresponders (INRs) are at greater risk of comorbidity and mortality than are immune responders (IRs) who restore their CD4+ T cell count after antiretroviral therapy (ART). INRs have low CD4+ T cell counts (<350 c/μL), heightened systemic inflammation, and increased CD4+ T cell cycling (Ki67+). Here, we report the findings that memory CD4+ T cells and plasma samples of INRs from several cohorts are enriched in gut-derived bacterial solutes p-cresol sulfate (PCS) and indoxyl sulfate (IS) that both negatively correlated with CD4+ T cell counts. In vitro PCS or IS blocked CD4+ T cell proliferation, induced apoptosis, and diminished the expression of mitochondrial proteins. Electron microscopy imaging revealed perturbations of mitochondrial networks similar to those found in INRs following incubation of healthy memory CD4+ T cells with PCS. Using bacterial 16S rDNA, INR stool samples were found enriched in proteolytic bacterial genera that metabolize tyrosine and phenylalanine to produce PCS. We propose that toxic solutes from the gut bacterial flora may impair CD4+ T cell recovery during ART and may contribute to CD4+ T cell lymphopenia characteristic of INRs.

Authors

Brian Ferrari, Amanda Cabral Da Silva, Ken H. Liu, Evgeniya V. Saidakova, Larisa B. Korolevskaya, Konstantin V. Shmagel, Carey Shive, Gabriela Pacheco Sanchez, Mauricio Retuerto, Ashish Arunkumar Sharma, Khader Ghneim, Laura Noel-Romas, Benigno Rodriguez, Mahmoud A. Ghannoum, Peter P. Hunt, Steven G. Deeks, Adam D. Burgener, Dean P. Jones, Mirela A. Dobre, Vincent C. Marconi, Rafick-Pierre Sekaly, Souheil-Antoine Younes

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Figure 1

Enrichment of PCS and IS in INR samples.

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Enrichment of PCS and IS in INR samples. Untargeted metabolic UPLC-MS/MS...
Untargeted metabolic UPLC-MS/MS measurements showing levels of PCS (A) in 1 × 106 to 2 × 106 sorted memory CD4+ T cells of IRs (n = 15), INRs (n = 14), and HCs (n = 7). Concentration of PCS (B) and IS (C) in the plasma of the IR and INR groups in the CLIF (red dots) and SCOPE (green dots) cohorts. Median and interquartile range (solid lines) are displayed in the dot plots. P values were generated by Kruskal-Wallis with Dunn’s multiple-comparison test. Spearman’s correlation of plasma concentrations of PCS (D) and IS (E) with CD4+ T cell count. Blue dots are INR patient data.