S100A9-RAGE Axis Accelerates Formation of Macrophage-Mediated Extracellular Vesicle Microcalcification in Diabetes Mellitus-Reference-Cited by-同舟云学术

S100A9-RAGE Axis Accelerates Formation of Macrophage-Mediated Extracellular Vesicle Microcalcification in Diabetes Mellitus

Published:2020-08 Issue:8 Volume:40 Page:1838-1853
ISSN:1079-5642
Container-title:Arteriosclerosis, Thrombosis, and Vascular Biology
language:en
Short-container-title:ATVB

Author:

Kawakami Ryo¹,Katsuki Shunsuke¹,Travers Richard¹,Romero Dayanna Carolina¹,Becker-Greene Dakota¹,Passos Livia Silva Araujo¹,Higashi Hideyuki²,Blaser Mark C.²,Sukhova Galina K.¹,Buttigieg Josef³,Kopriva David⁴,Schmidt Ann Marie⁵,Anderson Daniel G.⁶,Singh Sasha A.²,Cardoso Luis⁷,Weinbaum Sheldon⁷,Libby Peter¹,Aikawa Masanori¹²,Croce Kevin¹,Aikawa Elena¹²⁸^ORCID

Affiliation:

1. From the Center for Excellence in Vascular Biology (R.K., S.K., R.T., D.C.R., D.B.-G., L.S.A.P., G.K.S., P.L., M.A., K.C., E.A.), Brigham and Women’s Hospital, Harvard Medical School, Boston, MA

2. Center for Interdisciplinary Cardiovascular Sciences (H.H., M.C.B., S.A.S., M.A., E.A.), Brigham and Women’s Hospital, Harvard Medical School, Boston, MA

3. Department of Biology, University of Regina, Saskatchewan, Canada (J.B.)

4. Regina Qu’Appelle Health Region, University of Saskatchewan, Regina, Canada (D.K.)

5. Diabetes Research Program, Division of Endocrinology, Diabetes and Metabolism, Department of Medicine, New York University (A.M.S.)

6. Institutes for Medical Engineering and Science, Massachusetts Institute of Technology, Cambridge (D.G.A.)

7. Department of Biomedical Engineering, The City College of New York (L.C., S.W.)

8. Department of Human Pathology, Sechenov First Moscow State Medical University, Russia (E.A.).

Abstract

Objective: Vascular calcification is a cardiovascular risk factor and accelerated in diabetes mellitus. Previous work has established a role for calcification-prone extracellular vesicles in promoting vascular calcification. However, the mechanisms by which diabetes mellitus provokes cardiovascular events remain incompletely understood. Our goal was to identify that increased S100A9 promotes the release of calcification-prone extracellular vesicles from human macrophages in diabetes mellitus. Approach and Results: Human primary macrophages exposed to high glucose (25 mmol/L) increased S100A9 secretion and the expression of receptor for advanced glycation end products (RAGE) protein. Recombinant S100A9 induced the expression of proinflammatory and osteogenic factors, as well as the number of extracellular vesicles with high calcific potential (alkaline phosphatase activity, P <0.001) in macrophages. Treatment with a RAGE antagonist or silencing with S100A9 siRNA in macrophages abolished these responses, suggesting that stimulation of the S100A9-RAGE axis by hyperglycemia favors a procalcific environment. We further showed that an imbalance between Nrf-2 (nuclear factor 2 erythroid related factor 2) and NF-κB (nuclear factor-κB) pathways contributes to macrophage activation and promotes a procalcific environment. In addition, streptozotocin-induced diabetic Apoe −/− S100a9 −/− mice and mice treated with S100a9 siRNA encapsulated in macrophage-targeted lipid nanoparticles showed decreased inflammation and microcalcification in atherosclerotic plaques, as gauged by molecular imaging and comprehensive histological analysis. In human carotid plaques, comparative proteomics in patients with diabetes mellitus and histological analysis showed that the S100A9-RAGE axis associates with osteogenic activity and the formation of microcalcification. Conclusions: Under hyperglycemic conditions, macrophages release calcific extracellular vesicles through mechanisms involving the S100A9-RAGE axis, thus contributing to the formation of microcalcification within atherosclerotic plaques.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

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