Deficiency of Circulating Monocytes Ameliorates the Progression of Myxomatous Valve Degeneration in Marfan Syndrome

Marfan syndrome; Fbn1 protein, mouse; C57BL mouse; Animals; Chemokine CCL2; Disease Models, Animal; Disease Progression; Dogs; Extracellular Matrix; Fibrillin-1; Heart Valve Diseases; Leukocyte Common Antigens; Macrophages; Mice; Mice, Inbred C57BL; Mitral Valve; Monocytes; Swine

Abstract :

[en] Background: Myxomatous valve degeneration (MVD) involves the progressive thickening and degeneration of the heart valves, leading to valve prolapse, regurgitant blood flow, and impaired cardiac function. Leukocytes composed primarily of macrophages have recently been detected in myxomatous valves, but the timing of the presence and the contributions of these cells in MVD progression are not known. Methods: We examined MVD progression, macrophages, and the valve microenvironment in the context of Marfan syndrome (MFS) using mitral valves from MFS mice (Fbn1C1039G/+), gene-edited MFS pigs (FBN1Glu433AsnfsX98/+), and patients with MFS. Additional histological and transcriptomic evaluation was performed by using nonsyndromic human and canine myxomatous valves, respectively. Macrophage ontogeny was determined using MFS mice transplanted with mTomato+ bone marrow or MFS mice harboring RFP (red fluorescent protein)-tagged C-C chemokine receptor type 2 (CCR2) monocytes. Mice deficient in recruited macrophages (Fbn1C1039G/+;Ccr2RFP/RFP) were generated to determine the requirements of recruited macrophages to MVD progression. Results: MFS mice recapitulated histopathological features of myxomatous valve disease by 2 months of age, including mitral valve thickening, increased leaflet cellularity, and extracellular matrix abnormalities characterized by proteoglycan accumulation and collagen fragmentation. Diseased mitral valves of MFS mice concurrently exhibited a marked increase of infiltrating (MHCII+, CCR2+) and resident macrophages (CD206+, CCR2-), along with increased chemokine activity and inflammatory extracellular matrix modification. Likewise, mitral valve specimens obtained from gene-edited MFS pigs and human patients with MFS exhibited increased monocytes and macrophages (CD14+, CD64+, CD68+, CD163+) detected by immunofluorescence. In addition, comparative transcriptomic evaluation of both genetic (MFS mice) and acquired forms of MVD (humans and dogs) unveiled a shared upregulated inflammatory response in diseased valves. Remarkably, the deficiency of monocytes was protective against MVD progression, resulting in a significant reduction of MHCII macrophages, minimal leaflet thickening, and preserved mitral valve integrity. Conclusions: All together, our results suggest sterile inflammation as a novel paradigm to disease progression, and we identify, for the first time, monocytes as a viable candidate for targeted therapy in MVD. © 2020 Lippincott Williams and Wilkins. All rights reserved.

Disciplines :

Cardiovascular & respiratory systems

Author, co-author :

Kim, A. J.; Heart Institute, Division of Molecular Cardiovascular Biology, Cincinnati Children's Hospital Medical Center, University of Cincinnati, College of MedicineOH, United States

Xu, N.; Heart Institute, Division of Molecular Cardiovascular Biology, Cincinnati Children's Hospital Medical Center, University of Cincinnati, College of MedicineOH, United States

Umeyama, K.; Meiji University International, Institute for Bio-Resource Research, Kawasaki, Japan

Hulin, Alexia ; Université de Liège - ULiège

Ponny, S. R.; Division of Human Genetics, Cincinnati Children's Hospital Medical Center, University of Cincinnati, College of MedicineOH, United States

Vagnozzi, R. J.; Heart Institute, Division of Molecular Cardiovascular Biology, Cincinnati Children's Hospital Medical Center, University of Cincinnati, College of MedicineOH, United States

Green, E. A.; Heart Institute, Division of Molecular Cardiovascular Biology, Cincinnati Children's Hospital Medical Center, University of Cincinnati, College of MedicineOH, United States

Hanson, P.; Center for Heart Lung Innovation, St. Paul's Hospital, University of British Columbia, Vancouver, Canada

McManus, B. M.; Center for Heart Lung Innovation, St. Paul's Hospital, University of British Columbia, Vancouver, Canada

Nagashima, H.

Yutzey, K. E.; Heart Institute, Division of Molecular Cardiovascular Biology, Cincinnati Children's Hospital Medical Center, University of Cincinnati, College of MedicineOH, United States

Language :

English

Title :

Deficiency of Circulating Monocytes Ameliorates the Progression of Myxomatous Valve Degeneration in Marfan Syndrome

Publication date :

2020

Journal title :

Circulation

ISSN :

0009-7322

eISSN :

1524-4539

Publisher :

Lippincott Williams & Wilkins, United States - Maryland

Pages :

132-146

Peer reviewed :

Peer Reviewed verified by ORBi

Available on ORBi :

since 29 July 2021

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