Contribution of VEGF-B-Induced Endocardial Endothelial Cell Lineage in Physiological Versus Pathological Cardiac Hypertrophy

Ibrahim Sultan; Markus Ramste; Pim Peletier; Karthik Amudhala Hemanthakumar; Deepak Ramanujam; Annakaisa Tirronen; Ylva von Wright; Salli Antila; Pipsa Saharinen; Lauri Eklund; Eero Mervaala; Seppo Ylä-Herttuala; Stefan Engelhardt; Riikka Kivelä; Kari Alitalo

doi:10.1161/CIRCRESAHA.123.324136

Contribution of VEGF-B-Induced Endocardial Endothelial Cell Lineage in Physiological Versus Pathological Cardiac Hypertrophy

Circ Res. 2024 Apr 24. doi: 10.1161/CIRCRESAHA.123.324136. Online ahead of print.

Authors

Ibrahim Sultan^{1

2}, Markus Ramste^#^{1

2}, Pim Peletier^#^{1

2}, Karthik Amudhala Hemanthakumar^{1

2}, Deepak Ramanujam^{3

4}, Annakaisa Tirronen⁵, Ylva von Wright^{1

2}, Salli Antila^{1

2}, Pipsa Saharinen^{1

2}, Lauri Eklund⁶, Eero Mervaala⁷, Seppo Ylä-Herttuala⁵, Stefan Engelhardt³, Riikka Kivelä^{1

8

9}, Kari Alitalo^{1

2}

Affiliations

¹ Wihuri Research Institute, Faculty of Medicine, Biomedicum Helsinki, University of Helsinki, Finland. (I.S., M.R., P.P., K.A.H., Y.v.W., S.A., P.S., R.K., K.A.).
² Translational Cancer Medicine Program, Faculty of Medicine, Biomedicum Helsinki, University of Helsinki, Finland. (I.S., M.R., P.P., K.A.H., Y.v.W., S.A., P.S., K.A.).
³ Institute for Pharmacology and Toxicology, Technical University of Munich, DZHK partner site Munich Heart Alliance, Germany (D.R., S.E.).
⁴ RNATICS GmbH, Planegg, Germany (D.R.).
⁵ A.I. Virtanen Institute, University of Eastern Finland, Kuopio, Finland (A.T., S.Y.-H.).
⁶ Oulu Center for Cell-Matrix Research, Faculty of Biochemistry and Molecular Medicine, Biocenter Oulu, University of Oulu, Finland (L.E.).
⁷ Department of Pharmacology, Faculty of Medicine, University of Helsinki, Finland. (E.M.).
⁸ Stem Cells and Metabolism Research Program, Faculty of Medicine, University of Helsinki, Finland. (R.K.).
⁹ Faculty of Sport and Health Sciences, University of Jyväskylä, Finland (R.K.).

^# Contributed equally.

PMID: 38655691
DOI: 10.1161/CIRCRESAHA.123.324136

Abstract

Background: Preclinical studies have shown the therapeutic potential of VEGF-B (vascular endothelial growth factor B) in revascularization of the ischemic myocardium, but the associated cardiac hypertrophy and adverse side effects remain a concern. To understand the importance of endothelial proliferation and migration for the beneficial versus adverse effects of VEGF-B in the heart, we explored the cardiac effects of autocrine versus paracrine VEGF-B expression in transgenic and gene-transduced mice.

Methods: We used single-cell RNA sequencing to compare cardiac endothelial gene expression in VEGF-B transgenic mouse models. Lineage tracing was used to identify the origin of a VEGF-B-induced novel endothelial cell population and adeno-associated virus-mediated gene delivery to compare the effects of VEGF-B isoforms. Cardiac function was investigated using echocardiography, magnetic resonance imaging, and micro-computed tomography.

Results: Unlike in physiological cardiac hypertrophy driven by a cardiomyocyte-specific VEGF-B transgene (myosin heavy chain alpha-VEGF-B), autocrine VEGF-B expression in cardiac endothelium (aP2 [adipocyte protein 2]-VEGF-B) was associated with septal defects and failure to increase perfused subendocardial capillaries postnatally. Paracrine VEGF-B led to robust proliferation and myocardial migration of a novel cardiac endothelial cell lineage (VEGF-B-induced endothelial cells) of endocardial origin, whereas autocrine VEGF-B increased proliferation of VEGF-B-induced endothelial cells but failed to promote their migration and efficient contribution to myocardial capillaries. The surviving aP2-VEGF-B offspring showed an altered ratio of secreted VEGF-B isoforms and developed massive pathological cardiac hypertrophy with a distinct cardiac vessel pattern. In the normal heart, we found a small VEGF-B-induced endothelial cell population that was only minimally expanded during myocardial infarction but not during physiological cardiac hypertrophy associated with mouse pregnancy.

Conclusions: Paracrine and autocrine secretions of VEGF-B induce expansion of a specific endocardium-derived endothelial cell population with distinct angiogenic markers. However, autocrine VEGF-B signaling fails to promote VEGF-B-induced endothelial cell migration and contribution to myocardial capillaries, predisposing to septal defects and inducing a mismatch between angiogenesis and myocardial growth, which results in pathological cardiac hypertrophy.

Keywords: angiogenesis; coronary vessels; heart failure; myocardial infarction; pregnancy.