PROX1 Inhibits PDGF-B Expression to Prevent Myxomatous Degeneration of Heart Valves

Yen-Chun Ho; Xin Geng; Anna O'Donnell; Jaime Ibarrola; Amaya Fernandez-Celis; Rohan Varshney; Kumar Subramani; Zheila J Azartash-Namin; Jang Kim; Robert Silasi; Jill Wylie-Sears; Zahra Alvandi; Lijuan Chen; Boksik Cha; Hong Chen; Lijun Xia; Bin Zhou; Florea Lupu; Harold M Burkhart; Elena Aikawa; Lorin E Olson; Jasimuddin Ahamed; Natalia López-Andrés; Joyce Bischoff; Katherine E Yutzey; R Sathish Srinivasan

doi:10.1161/CIRCRESAHA.123.323027

PROX1 Inhibits PDGF-B Expression to Prevent Myxomatous Degeneration of Heart Valves

Circ Res. 2023 Sep;133(6):463-480. doi: 10.1161/CIRCRESAHA.123.323027. Epub 2023 Aug 9.

Authors

Yen-Chun Ho¹, Xin Geng^#^{1

2}, Anna O'Donnell^#³, Jaime Ibarrola^{4

5}, Amaya Fernandez-Celis⁵, Rohan Varshney¹, Kumar Subramani¹, Zheila J Azartash-Namin¹, Jang Kim^{1

6}, Robert Silasi¹, Jill Wylie-Sears⁷, Zahra Alvandi⁷, Lijuan Chen¹, Boksik Cha^{1

8}, Hong Chen⁷, Lijun Xia¹, Bin Zhou⁹, Florea Lupu¹, Harold M Burkhart¹⁰, Elena Aikawa¹¹, Lorin E Olson¹, Jasimuddin Ahamed¹, Natalia López-Andrés⁵, Joyce Bischoff⁷, Katherine E Yutzey³, R Sathish Srinivasan^{1

5}

Affiliations

¹ Cardiovascular Biology Research Program, Oklahoma Medical Research Foundation, Oklahoma City, OK (Y.-C.H., X.G., R.V., K.S., Z.J.A.-N., J.K., R.S., L.C., B.C., L.X., F.L., L.E.O., J.A., R.S.S.).
² Now with Sanegene Bio, Woburn, MA (X.G.).
³ Division of Molecular Cardiovascular Biology, Cincinnati Children's Hospital Medical Center, Cincinnati, OH (A.O., K.E.Y.).
⁴ Molecular Cardiology Research Institute, Tufts Medical Center, Boston, MA (J.I.).
⁵ Cardiovascular Translational Research, Navarrabiomed (Miguel Servet Foundation), Instituto de Investigación Sanitaria de Navarra (IdiSNA), Hospital Universitario de Navarra (HUN), Universidad Pública de Navarra (UPNA), Pamplona, Spain (J.I., A.F.-C., N.L.-A., R.S.S.).
⁶ Department of Cell Biology, University of Oklahoma Health Sciences Center (J.K.).
⁷ Vascular Biology Program, Boston Children's Hospital, Boston, MA (J.W.-S., Z.A., H.C., J.B.).
⁸ Now with Daegu Gyeongbuk Medical Innovation Foundation, Republic of Korea (B.C.).
⁹ Department of Genetics, Albert Einstein College of Medicine, Bronx, NY (B.Z.).
¹⁰ Oklahoma Children's Hospital, University of Oklahoma Health Heart Center, Oklahoma City, OK (H.M.B.).
¹¹ Department of Medicine, Cardiovascular Division, Brigham and Women's Hospital, Boston, MA (E.A.).

^# Contributed equally.

Abstract

Background: Cardiac valve disease is observed in 2.5% of the general population and 10% of the elderly people. Effective pharmacological treatments are currently not available, and patients with severe cardiac valve disease require surgery. PROX1 (prospero-related homeobox transcription factor 1) and FOXC2 (Forkhead box C2 transcription factor) are transcription factors that are required for the development of lymphatic and venous valves. We found that PROX1 and FOXC2 are expressed in a subset of valvular endothelial cells (VECs) that are located on the downstream (fibrosa) side of cardiac valves. Whether PROX1 and FOXC2 regulate cardiac valve development and disease is not known.

Methods: We used histology, electron microscopy, and echocardiography to investigate the structure and functioning of heart valves from Prox1^ΔVEC mice in which Prox1 was conditionally deleted from VECs. Isolated valve endothelial cells and valve interstitial cells were used to identify the molecular mechanisms in vitro, which were tested in vivo by RNAScope, additional mouse models, and pharmacological approaches. The significance of our findings was tested by evaluation of human samples of mitral valve prolapse and aortic valve insufficiency.

Results: Histological analysis revealed that the aortic and mitral valves of Prox1^ΔVEC mice become progressively thick and myxomatous. Echocardiography revealed that the aortic valves of Prox1^ΔVEC mice are stenotic. FOXC2 was downregulated and PDGF-B (platelet-derived growth factor-B) was upregulated in the VECs of Prox1^ΔVEC mice. Conditional knockdown of FOXC2 and conditional overexpression of PDGF-B in VECs recapitulated the phenotype of Prox1^ΔVEC mice. PDGF-B was also increased in mice lacking FOXC2 and in human mitral valve prolapse and insufficient aortic valve samples. Pharmacological inhibition of PDGF-B signaling with imatinib partially ameliorated the valve defects of Prox1^ΔVEC mice.

Conclusions: PROX1 antagonizes PDGF-B signaling partially via FOXC2 to maintain the extracellular matrix composition and prevent myxomatous degeneration of cardiac valves.

Keywords: aortic valve; endothelial cells; extracellular matrix; mitral valve; prolapse.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Endothelial Cells / metabolism
Heart Valve Diseases* / genetics
Heart Valve Diseases* / metabolism
Heart Valve Diseases* / prevention & control
Humans
Mice
Mitral Valve / metabolism
Mitral Valve Prolapse* / metabolism
Proto-Oncogene Proteins c-sis / metabolism
Transcription Factors / metabolism

Substances

Transcription Factors
prospero-related homeobox 1 protein
Proto-Oncogene Proteins c-sis

Abstract

Publication types

MeSH terms

Substances

Grants and funding