LDL and IL-6 induce TGF-β1 release and mast cell migration toward intimal macrophages
Heng Yu, Radhika R. Josi, Ankur Khanna, Damir B. Khismatullin

TL;DR
The study shows that LDL and IL-6 cause macrophages to release TGF-β1, which attracts mast cells to the artery wall, potentially contributing to inflammation.
Contribution
The novel finding is that LDL and IL-6 induce macrophage repolarization, leading to TGF-β1 release and mast cell migration.
Findings
LDL and IL-6 treatment caused M1 macrophages to release TGF-β1 at levels similar to M2 macrophages.
M2-like macrophages retained inflammatory properties and attracted mast cells via TGF-β1.
LUVA cells migrated toward TGF-β1 or conditioned medium from M2-like macrophages.
Abstract
This study tests the hypothesis that mast cells migration to the artery’s intimal layer occurs due to release of TGF-β1 from macrophages exposed to LDL and IL-6. Human monocytic cells (THP-1), human mast cells (LUVA), and human umbilical vein endothelial cells (HUVEC). THP-1 cells were differentiated into M0, M1, and M2 macrophages, which were then treated with LDL, oxidized LDL (oxLDL), IL-6, or a combination of LDL and IL-6. LUVA cells and HUVEC were exposed to conditioned media from untreated and treated macrophages. LUVA cells were also exposed to TGF-β1. The concentration of TNF-α and TGF-β1 released from macrophages was measured by ELISA. The migration of LUVA cells in a microfluidic channel was assessed for 12 h. THP-1 cell adhesion to HUVEC was investigated under static conditions. Inflammatory (M1) macrophages exposed to LDL + IL-6 or oxLDL released TGF-β1 at the level…
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Taxonomy
TopicsMast cells and histamine · Atherosclerosis and Cardiovascular Diseases · Cell Adhesion Molecules Research
