Litcius/Paper detail

JAK/STAT signaling pathway affects CCR5 expression in human CD4 <sup>+</sup> T cells

Lingyun Wang, Yunus Yükselten, Julius Nuwagaba, Richard E. Sutton

2024Science Advances26 citationsDOIOpen Access PDF

Abstract

CCR5 serves as R5-tropic HIV co-receptor. Knocking out CCR5 in HIV patients, which has occurred &lt;10 times, is believed important for cure. JAK/STAT inhibitors tofacitinib and ruxolitinib inhibit CCR5 expression in HIV + viremic patients. We investigated the association of JAK/STAT signaling pathway with CCR5/CCR2 expression in human primary CD4 + T cells and confirmed its importance. Six of nine JAK/STAT inhibitors that reduced CCR5/CCR2 expression were identified. Inhibitor-treated CD4 + T cells were relatively resistant, specifically to R5-tropic HIV infection. Furthermore, single JAK2, STAT3, STAT5A, and STAT5B knockout and different combinations of JAK/STAT knockout significantly reduced CCR2/CCR5 expression of both RNA and protein levels, indicating that CCR5/CCR2 expression was positively regulated by JAK-STAT pathway in CD4 + T cells. Serum and glucocorticoid-regulated kinase 1 (SGK1) knockout affected CCR2/CCR5 gene expression, suggesting that SGK1 is involved in CCR2/CCR5 regulation. If cell surface CCR5 levels can be specifically and markedly down-regulated without adverse effects, that may have a major impact on the HIV cure agenda.

Topics & Concepts

RuxolitinibJAK-STAT signaling pathwaystatCCR5 receptor antagonistCCR2Chemokine receptor CCR5Janus kinaseTofacitinibSignal transductionChemokine receptorBiologyKnockout mouseTyrosine kinase 2Cancer researchCCR4STAT3ChemokineCell biologyReceptorImmunologyMyelofibrosisTyrosine kinaseInflammationGeneticsBone marrowGrowth factorPlatelet-derived growth factor receptorRheumatoid arthritisHIV Research and TreatmentImmune Cell Function and InteractionT-cell and B-cell Immunology