纤维化
成纤维细胞
肌成纤维细胞
心脏纤维化
生物
骨膜炎
细胞生物学
癌症研究
炎症
免疫系统
免疫学
病理
细胞外基质
医学
细胞培养
遗传学
作者
Kory J. Lavine,Junedh M. Amrute,Xin Luo,Vinay Penna,Andrea L. Bredemeyer,Tracy Yamawaki,Steven Yang,Farid F. Kadyrov,Gyu Seong Heo,Sally Yu Shi,Paul C. Lee,Andrew L. Koenig,Christoph Kuppe,Cameran Jones,Benjamin J. Kopecky,Sikander Hayat,Pan Ma,Yuriko Terada,Angela Fu,Milena B. Furtado
出处
期刊:Research Square - Research Square
日期:2023-01-26
被引量:24
标识
DOI:10.21203/rs.3.rs-2402606/v1
摘要
Inflammation and tissue fibrosis co-exist and are causally linked to organ dysfunction. However, the molecular mechanisms driving immune-fibroblast crosstalk in human cardiac disease remains unexplored and there are currently no therapeutics to target fibrosis. Here, we performed multi-omic single-cell gene expression, epitope mapping, and chromatin accessibility profiling in 38 donors, acutely infarcted, and chronically failing human hearts. We identified a disease-associated fibroblast trajectory marked by cell surface expression of fibroblast activator protein (FAP), which diverged into distinct myofibroblasts and pro-fibrotic fibroblast populations, the latter resembling matrifibrocytes. Pro-fibrotic fibroblasts were transcriptionally similar to cancer associated fibroblasts and expressed high levels of collagens and periostin (
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