2. Academic Validation
  3. Chemerin-9, a potent agonist of chemerin receptor (ChemR23), prevents atherogenesis

Chemerin-9, a potent agonist of chemerin receptor (ChemR23), prevents atherogenesis

  • Clin Sci (Lond). 2019 Aug 20;133(16):1779-1796. doi: 10.1042/CS20190336.
Kengo Sato 1 Hayami Yoshizawa 2 Tomomi Seki 2 3 Remina Shirai 2 Tomoyuki Yamashita 2 Taisuke Okano 2 Koichiro Shibata 2 Miyu J Wakamatsu 2 Yusaku Mori 4 Toshisuke Morita 3 Taka-Aki Matsuyama 5 6 Hatsue Ishibashi-Ueda 6 Tsutomu Hirano 4 Takuya Watanabe 2
Affiliations

Affiliations

  • 1 Laboratory of Cardiovascular Medicine, Tokyo University of Pharmacy and Life Sciences, Tokyo, Japan [email protected].
  • 2 Laboratory of Cardiovascular Medicine, Tokyo University of Pharmacy and Life Sciences, Tokyo, Japan.
  • 3 Department of Laboratory Medicine, Toho University Faculty of Medicine, Tokyo, Japan.
  • 4 Division of Diabetes, Metabolism, and Endocrinology, Department of Medicine, Showa University School of Medicine, Tokyo, Japan.
  • 5 Department of Legal Medicine, Showa University School of Medicine, Tokyo, Japan.
  • 6 Department of Pathology, National Cerebral and Cardiovascular Center, Osaka, Japan.
PMID: 31399499 DOI: 10.1042/CS20190336
Abstract

Plasma levels of chemerin, an adipocytokine produced from the adipose tissues and liver, are associated with metabolic syndrome and coronary artery disease (CAD). Chemerin and its analog, chemerin-9, are known to bind to their receptor, ChemR23. However, whether chemerin and chemerin-9 affect atherogenesis remains to be elucidated. We investigated the expression of chemerin and ChemR23 in human coronary arteries and cultured human vascular cells. The effects of chemerin and chemerin-9 on atheroprone phenomena were assessed in human THP1 monocytes, human umbilical vein endothelial cells (HUVECs), and human aortic smooth muscle cells (HASMCs) and aortic lesions in Apoe-/- mice. In patients with CAD, a small amount of ChemR23, but not chemerin, was expressed within atheromatous plaques in coronary arteries. Chemerin and ChemR23 were expressed at high levels in THP1 monocytes, THP1-derived macrophages, and HUVECs; however, their expression in HASMCs was weak. Chemerin and chemerin-9 significantly suppressed the tumor necrosis factor-α (TNF-α)-induced mRNA expression of adhesion and pro-inflammatory molecules in HUVECs. Chemerin and chemerin-9 significantly attenuated the TNF-α-induced adhesion of THP1 monocytes to HUVECs and macrophage inflammatory phenotype. Chemerin and chemerin-9 suppressed oxidized low-density lipoprotein (oxLDL)-induced macrophage foam cell formation associated with down-regulation of CD36 and up-regulation of ATP-binding cassette transporter A1 (ABCA1). In HASMCs, chemerin and chemerin-9 significantly suppressed migration and proliferation without inducing Apoptosis. In the Apoe-/- mice, a 4-week infusion of chemerin-9 significantly decreased the areas of aortic atherosclerotic lesions by reducing intraplaque macrophage and SMC contents. Our results indicate that chemerin-9 prevents atherosclerosis. Therefore, the development of chemerin analogs/ChemR23 agonists may serve as a novel therapeutic target for atherosclerotic diseases.

Keywords

atherosclerosis; chemerin; endothelial cell; macrophage; vascular smooth muscle cell.

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