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Arginase-2 enhances monocyte-endothelial interaction through regulation of integrin and membrane receptor expression: role in atherogenesis.

Created on 14 Jul 2026

Authors

Guillaume Ajalbert, Yuejun Yao, Sophie Rohrer, Matteo Caretti, Santhoshkumar Sundaramoorthy, Anastasia Rigkou, Michael Stumpe, Xiu-Fen Ming, Duilio M Potenza, Zhihong Yang

Published in

Journal of biomedical science. Volume 33. Issue 1. Jul 13, 2026. Epub Jul 13, 2026.

Abstract

Circulating monocyte trans-endothelial migration is critical for vascular diseases. The monocyte surface proteins, i.e., integrins and membrane receptors are central in this process. Previous studies demonstrate that ablation of the mitochondrial arginase-2 (ARG2) reduces monocyte/macrophage infiltration in cardiovascular disease. We further investigate whether ARG2 regulates integrin and surface receptor levels in monocytes and facilitates trans-endothelial migration, contributing to atherogenesis.
For this purpose, human THP1 cells deficient in ARG2 gene (THP1ARG2-/-) were generated by CRISPR-U-mediated genome engineering. Atherosclerotic Apoe-/-Arg2+/+ mice and Apoe-/-Arg2-/- mouse models are used. Proteomic profiling, cellular/molecular biology methods, and confocal microscopy were utilized for gene or protein expression analysis.
As compared to the control THP1WT cells, the THP1ARG2-/- cells reveal decreased adhesion and trans-endothelial migratory activities towards chemoattractants in a transwell co-culture system, accompanied by lower levels of αL and α4 integrins, CD99 and PECAM1 (CD31) (surface molecules for trans-endothelial activity) and CCR2 (the chemoattractant receptor). The monocyte adhesion to endothelial cells is reduced by blocking LFA-1 (αLβ2) or VLA-4 (α4β1) integrin. Pro-inflammatory polarization of the THP1 cells with LPS does not affect the integrin and surface receptor levels, however, enhances release of several pro-inflammatory cytokines, which is reduced in THP1ARG2-/- cells due to reduced TLR4-ERK-NF-κB signaling. Conditioned medium from the LPS-primed THP1WT reveals higher capacity to enhance endothelial VCAM-1 and ICAM-1 levels than the THP1ARG2-/- cells, that is partly mediated by IL-1β. Moreover, ARG2-dependent TGF-β signaling was found to selectively regulate αL expression in monocytes. Finally, as compared to Apoe-/-Arg2+/+ mice, the ApoE-/-Arg2-/- mice show significantly decreased macrophage integrin, chemoattractant receptor levels, and atherosclerosis.
Our study identifies ARG2 as a key regulator of monocyte-mediated vascular inflammation and atherogenesis by controlling integrin, chemoattractant receptor expression, and pro-inflammatory cytokine release through TLR4-ERK-NFκB signaling, highlighting ARG2 as a potential therapeutic target for vascular and chronic inflammatory diseases.

PMID:
42443923
Bibliographic data and abstract were imported from PubMed on 14 Jul 2026.

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