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Transcriptional heterogeneity of fibroblasts is a hallmark of the aging heart

Item Type:Article
Title:Transcriptional heterogeneity of fibroblasts is a hallmark of the aging heart
Creators Name:Vidal, R. and Wagner, J.U.G. and Braeuning, C. and Fischer, C. and Patrick, R. and Tombor, L. and Muhly-Reinholz, M. and John, D. and Kliem, M. and Conrad, T. and Guimarães-Camboa, N. and Harvey, R. and Dimmeler, S. and Sauer, S.
Abstract:Aging is a major risk factor for cardiovascular disease. Although the impact of aging has been extensively studied, little is known regarding the aging processes in cells of the heart. Here we analyzed the transcriptomes of hearts of 12-week-old and 18-month-old mice by single-nucleus RNA-sequencing. Among all cell types, aged fibroblasts showed most significant differential gene expression, increased RNA dynamics, and network entropy. Aged fibroblasts exhibited significantly changed expression patterns of inflammatory, extracellular matrix organization angiogenesis, and osteogenic genes. Functional analyses indicated deterioration of paracrine signatures between fibroblasts and endothelial cells in old hearts. Aged heart-derived fibroblasts had impaired endothelial cell angiogenesis and autophagy and augmented proinflammatory response. In particular, expression of Serpine1 and Serpine2 were significantly increased and secreted by old fibroblasts to exert antiangiogenic effects on endothelial cells, an effect that could be significantly prevented by using neutralizing antibodies. Moreover, we found an enlarged subpopulation of aged fibroblasts expressing osteoblast genes in the epicardial layer associated with increased calcification. Taken together this study provides system-wide insights and identifies molecular changes of aging cardiac fibroblasts, which may contribute to declined heart function.
Keywords:Aging, Fibroblasts, Heart, Myocardium, Serpins, Transcriptome, Vascular Calcification, Animals, Mice
Source:JCI Insight
ISSN:2379-3708
Publisher:American Society for Clinical Investigation
Volume:4
Number:22
Page Range:e131092
Date:14 November 2019
Additional Information:copyright © 2019 American Society for Clinical Investigation
Official Publication:https://doi.org/10.1172/jci.insight.131092
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