| Literature DB >> 34363749 |
Rysa Zaman1, Homaira Hamidzada1, Crystal Kantores2, Anthony Wong1, Sarah A Dick3, Yiming Wang2, Abdul Momen2, Laura Aronoff4, Julia Lin1, Babak Razani5, Seema Mital6, Filio Billia7, Kory J Lavine8, Sara Nejat7, Slava Epelman9.
Abstract
Hypertension affects one-third of the world's population, leading to cardiac dysfunction that is modulated by resident and recruited immune cells. Cardiomyocyte growth and increased cardiac mass are essential to withstand hypertensive stress; however, whether immune cells are involved in this compensatory cardioprotective process is unclear. In normotensive animals, single-cell transcriptomics of fate-mapped self-renewing cardiac resident macrophages (RMs) revealed transcriptionally diverse cell states with a core repertoire of reparative gene programs, including high expression of insulin-like growth factor-1 (Igf1). Hypertension drove selective in situ proliferation and transcriptional activation of some cardiac RM states, directly correlating with increased cardiomyocyte growth. During hypertension, inducible ablation of RMs or selective deletion of RM-derived Igf1 prevented adaptive cardiomyocyte growth, and cardiac mass failed to increase, which led to cardiac dysfunction. Single-cell transcriptomics identified a conserved IGF1-expressing macrophage subpopulation in human cardiomyopathy. Here we defined the absolute requirement of RM-produced IGF-1 in cardiac adaptation to hypertension.Entities:
Keywords: IGF-1; cardiac; cardiomyocyte hypertrophy; fate mapping; heart failure; hypertension; macrophages; organ growth; resident macrophages; scRNA-seq
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Year: 2021 PMID: 34363749 DOI: 10.1016/j.immuni.2021.07.006
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745