Single-cell expression profiling reveals dynamic flux of cardiac stromal, vascular and immune cells in health and injury

Farbehi, Nona; Patrick, Ralph; Dorison, Aude; Xaymardan, Munira; Janbandhu, Vaibhao; Wystub-Lis, Katharina; Ho, Joshua W. K.; Nordon, Robert E.; Harvey, Richard P.

doi:10.7554/elife.43882

Cited by 409 publications

(526 citation statements)

References 98 publications

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“…These include fibroblasts (Pdgfra, Col1a1), pericytes (Pdgfrb, Vtn), smooth muscle cells (SMCs; Acta2, Myh11), Schwann cells (Plp1, Kcna1), endothelial cells (Pecam, Ly6c1), macrophages (Fcgr1, Csf1r), and other immune cell populations 6 (granulocytes, B cells, T cells and NK cells). A subset of fibroblasts (Fibroblast-Wif1) showed distinct gene expression patterns including active Wnt signaling and specific expression of Wif1, in line with our previous report [4] and the findings of Farbehi et al [5]. Additional less well-characterized cell populations included CMs (Ttn, Myh6), epicardial cells (Msln, Upk3b), lymphatic endothelial cells (Lyve1, Cldn5) and endocardial cells (Npr3, Cytl1) ( Figure 1B-D).…”

Section: Resultssupporting

confidence: 89%

“…Previous large-scale single cell transcriptomic studies exploring cardiac cellular diversity have failed to profile key cardiac cell populations including CMs [3][4][5][6] due to a reliance on dropletbased sequencing approaches that are incompatible with large cell isolation. Moreover, extraction of CMs from rodent hearts typically requires retro-aortic perfusion with proteases to liberate cells from the extracellular matrix; this is a relatively time-consuming process that has limited applicability for cell preparation in transcriptomic studies [7].…”

Section: Resultsmentioning

confidence: 99%

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High-resolution transcriptomic profiling of the heart during chronic stress reveals cellular drivers of cardiac fibrosis and hypertrophy

McLellan

Skelly

Dona

et al. 2019

Preprint

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Background: Cardiac fibrosis is a key antecedent to many types of cardiac dysfunction including heart failure. Physiological factors leading to cardiac fibrosis have been recognized for decades. However, the specific cellular and molecular mediators that drive cardiac fibrosis, and the relative impact of disparate cell populations on cardiac fibrosis, remain unclear. Methods:We developed a novel cardiac single-cell transcriptomics strategy to characterize the cardiac cellulome-the network of cells that forms the heart. This method was utilized to profile the cardiac cellular ecosystem in response to two weeks of continuous administration of Angiotensin II, a pro-fibrotic stimulus which drives pathological cardiac remodeling. Results: This analysis uncovered multiple cell populations contributing to pathological remodeling of the extracellular matrix of the heart. Two phenotypically distinct fibroblast populations emerged after induction of tissue stress to promote fibrosis in the absence of smooth muscle actin-expressing myofibroblasts, a key pro-fibrotic cell population. Further, the cellular responses to Angiotensin II and the relative abundance of fibrogenic cells were sexually dimorphic. Conclusions: These results offer a valuable resource for exploring the cardiac cellular landscape in health and after chronic cardiovascular stress. These data provide insights into the cellular and molecular mechanisms that promote pathological remodeling of the mammalian heart, highlighting early transcriptional changes which precede chronic cardiac fibrosis.35

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Section: Resultssupporting

confidence: 89%

Section: Resultsmentioning

confidence: 99%

High-resolution transcriptomic profiling of the heart during chronic stress reveals cellular drivers of cardiac fibrosis and hypertrophy

McLellan

Skelly

Dona

et al. 2019

Preprint

View full text Add to dashboard Cite

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“…However, both populations of CF are characterized by different markers, most probably because of the low number of Mki67 + CF included in the scRNA-seq study, and the reporter mice used. Interestingly, Faberhi et al described 9 subpopulations of PDGFRα + CF with a similar transcriptomic profiles that our subpopulations of Col1α1-GFP + CF at 7dpi 30 . However, our data indicate that CF that express Pdgfrα are contained within Col1α1-GFP + CF ( Fig.…”

Section: Discussionsupporting

confidence: 84%

“…CTHRC1 is a secreted protein that has the ability to inhibit collagen matrix synthesis through inhibition of TGF-β signaling 20,21,33 and that appears as a top marker gene for IRCF. Although expression of Cthrc1 has been previously identified as a potential marker for activated CF after MI in mice 9,30 and humans 29 , the longer follow-up in our study (up to 30dpi) may explain why it was not previously identified as a key player in the cardiac repair process. According to our results, expression of Cthrc1 peaks at 14dpi and decreases thereafter.…”

Section: Discussionmentioning

confidence: 68%

“…Non-myocyte cardiac cell heterogeneity has been recently characterized based on FACS sorting different populations of immune, endothelial and cardiac fibroblast 14,28,29 or on the usage of lineage tracing models such as PDGFRα 30 or POSTN 9 reporter mice. Most of these studies, focus on the early phase after cardiac injury 30 and assessed other pathological conditions 9,28,29 .…”

Section: Discussionmentioning

confidence: 99%

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Single-cell RNA-seq analysis reveals the crucial role of Collagen Triplex Helix Repeat Containing 1 (CTHRC1) cardiac fibroblasts for ventricular remodeling after myocardial infarction

Ruiz‐Villalba

Romero

Hernandez

et al. 2019

Preprint

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Cardiac fibroblasts have a central role during the ventricular remodeling process associated with different types of cardiac injury. Recent studies have shown that fibroblasts do not respond homogeneously to heart damage, suggesting that the adult myocardium may contain specialized fibroblast subgroups with specific functions. Due to the limited set of bona fide fibroblast markers, a proper characterization of fibroblast population dynamics in response to cardiac damage is still missing. Using single-cell RNA-seq, we identified and characterized a fibroblast subpopulation that emerges in response to myocardial infarction (MI) in a murine model. These activated fibroblasts exhibit a clear pro-fibrotic signature, express high levels of the hormone CTHRC1 and of the immunomodulatory co-receptor CD200 and localize to the injured myocardium. Combining epigenomic profiling with functional assays, we show Sox9 and the non-canonical TGF-β signaling as important regulators mediating their response to cardiac damage. We show that the absence of CTHRC1, in this activated fibroblast subpopulation, results in pronounced lethality due to ventricular rupture in a mouse model of myocardial infarction. Finally, we find evidence for the existence of similar mechanisms in a pig preclinical model of MI and establish a correlation between CTHRC1 levels and cardiac function after MI.

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Fibroblast‐mediated intercellular crosstalk in the healthy and diseased heart

et al. 2021

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Cardiac fibroblasts constitute a major cell population in the heart. They secrete extracellular matrix components and various other factors shaping the microenvironment of the heart. In silico analysis of intercellular communication based on single‐cell RNA sequencing revealed that fibroblasts are the source of the majority of outgoing signals to other cell types. This observation suggests that fibroblasts play key roles in orchestrating cellular interactions that maintain organ homeostasis but that can also contribute to disease states. Here, we will review the current knowledge of fibroblast interactions in the healthy, diseased, and aging heart. We focus on the interactions that fibroblasts establish with other cells of the heart, specifically cardiomyocytes, endothelial cells and immune cells, and particularly those relying on paracrine, electrical, and exosomal communication modes.

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Single-cell expression profiling reveals dynamic flux of cardiac stromal, vascular and immune cells in health and injury

Cited by 409 publications

References 98 publications

High-resolution transcriptomic profiling of the heart during chronic stress reveals cellular drivers of cardiac fibrosis and hypertrophy

High-resolution transcriptomic profiling of the heart during chronic stress reveals cellular drivers of cardiac fibrosis and hypertrophy

Single-cell RNA-seq analysis reveals the crucial role of Collagen Triplex Helix Repeat Containing 1 (CTHRC1) cardiac fibroblasts for ventricular remodeling after myocardial infarction

Fibroblast‐mediated intercellular crosstalk in the healthy and diseased heart

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