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The ecto-enzyme CD38 modulates CD4 T cell immunometabolic responses and participates in HIV pathogenesis.

Díaz-Basilio, Fernando; Vergara-Mendoza, Moisés; Romero-Rodríguez, Jessica; Hernández-Rizo, Sharik; Escobedo-Calvario, Alejandro; Fuentes-Romero, Luis-León; Pérez-Patrigeon, Santiago; Murakami-Ogasawara, Akio; Gomez-Palacio, María; Reyes-Terán, Gustavo; Jiang, Wei; Vázquez-Pérez, Joel-Armando; Marín-Hernández, Álvaro; Romero-Rodríguez, Dámaris-Priscila; Gutiérrez-Ruiz, María-Concepción; Viveros-Rogel, Mónica; Espinosa, Enrique.

J Leukoc Biol ; 2024 Mar 11.

Article in English | MEDLINE | ID: mdl-38466822

ABSTRACT

Despite abundant evidence correlating T cell CD38 expression and HIV infection pathogenesis, its role as a CD4 T cell immunometabolic regulator remains unclear. We find that CD38's extracellular glycohydrolase activity restricts metabolic reprogramming after TCR-engaging stimulation in Jurkat T CD4 cells, together with functional responses, while reducing intracellular NAD and NMN concentrations. Selective elimination of CD38's ectoenzyme function licenses them to decrease the OCR/ECAR ratio upon TCR signaling and to increase cycling, proliferation, survival, and CD40L induction. Pharmacological inhibition of ectoCD38 catalytic activity in memory CD4 T cells from chronic HIV-infected patients rescued TCR-triggered responses, including differentiation and effector functions, while reverting abnormally increased basal glycolysis, cycling, and spontaneous pro-inflammatory cytokine production. Additionally, ecto-CD38 blockage normalized basal and TCR-induced mitochondrial morpho-functionality, while increasing respiratory capacity in cells from HIV+ patients and healthy individuals. Ectoenzyme CD38's immunometabolic restriction of TCR-involving stimulation is relevant to CD4 T cell biology and to the deleterious effects of CD38 overexpression in HIV disease.

ABSTRACT

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