What question did this study set out to answer?

To investigate how monocyte interactions and oxidative stress contribute to atherosclerosis in HIV.

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March 15, 2026Open Access

Monocytes Defined by Platelet Interactions and Oxidative Stress Signaling Underlie HIV‐Associated Atherosclerosis

Key Points

To investigate how monocyte interactions and oxidative stress contribute to atherosclerosis in HIV.
Identified two monocyte clusters in people living with HIV.
Analyzed the role of platelet-monocyte complexes in vascular dysfunction.
Evaluated oxidative stress responses in CD14+ monocytes.
Platelet-monocyte-derived macrophages promote endothelial dysfunction.
CD14+ monocytes exhibit increased oxidative signaling and stress responses.
These mechanisms contribute to accelerated atherosclerosis in HIV.

Abstract

Two monocyte clusters contribute independently to vascular immune dysregulation in people living with HIV. Platelet-monocyte complex-derived macrophages promote endothelial dysfunction while adopting a profibrotic cytokine profile. CD14+ monocytes show heightened oxidative signaling and stress responses, consistent with vascular activation. Together, these mechanisms may accelerate atherosclerosis development in HIV, even in the absence of traditional cardiovascular risk factors.

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Cite This Study

Wang et al. (Fri,) studied this question.

synapsesocial.com/papers/69b5ff4f83145bc643d1b822 https://doi.org/https://doi.org/10.1161/jaha.125.046482

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