Resident Cardiac Macrophages Mediate Adaptive Myocardial Remodeling

Wong, Nicole R.; Mohan, J.; Kopecky, B.; Guo, Shikong; Du, Liming; Leid, Jamison; Dmytrenko, Oleksandr; Luehmann, Hannah; Bajpai, Geetika; Ewald, Laura; Bell, Lauren N.; Patel, Nikhil; Lokshina, Inessa; Bredemeyer, AL; Weinheimer, Carla J.; Negro, J M; Kovács, Attila; Morimoto, Sachio; Bayguinov, PO; Fisher, Max R.; Fitzpatrick, J. A. J.; Epelman, Slava; Kreisel, Daniel; Sah, Rajan; Liu, Y.; Hu, Hongzhen; Lavine, Kory J.

doi:10.1101/2021.01.28.428724

Cited by 13 publications

(31 citation statements)

References 69 publications

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“…These macrophages later shift to a reparative M2 phenotype, secrete anti-inflammatory cytokines, and instigate myocardial repair (14)(15)(16). Single cell (sc) RNA-seq experiments have implicated cardiac resident macrophages (RMs) in mediating the inflammatory response to cardiac injury (17)(18)(19). C-C chemokine receptor 2expressing (CCR2 + ) RMs (derived from recruited monocytes) and CCR2 -RMs (maintained independent of monocyte recruitment) promote and inhibit, respectively, monocyte recruitment after MI (20).…”

Section: Introductionmentioning

confidence: 99%

Nrf2 attenuates the innate immune response after experimental myocardial infarction

Bromage

Trevelin

Huntington

et al. 2022

Preprint

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Objectives: We aimed to investigate the contribution of the transcription factor nuclear factor erythroid-derived 2-like 2 (Nrf2) to the inflammatory response after experimental myocardial infarction (MI. Background: There is compelling evidence implicating dysregulated inflammation in the mechanism of ventricular remodeling and heart failure (HF) after MI. The transcription factor Nrf2 (encoded by Nfe2l2) is a promising target in this context. It impedes transcriptional upregulation of pro-inflammatory cytokines and is anti-inflammatory in various murine models. Methods: We subjected Nrf2-/- mice and wild type (WT) controls to permanent left coronary artery (LCA) ligation. The inflammatory response was investigated with fluorescence-activated cell sorting (FACS) analysis of peripheral blood and heart cell suspensions, together with qRT-PCR of infarcted tissue for chemokines and their receptors. To investigate whether Nrf2-mediated transcription is a dedicated function of leukocytes, we interrogated publicly available RNA-sequencing (RNA-seq) data from mouse hearts after permanent LCA ligation for Nrf2-regulated gene (NRG) expression. Results: FACS analysis demonstrated a profoundly inflamed phenotype in the hearts of global Nrf2-/- mice as compared to WT mice after MI. Moreover, infarcted tissue from Nrf2-/- mice displayed higher expression of inflammatory cytokines, chemokines, and their receptors, including IL6, Ccl2, and Cxcr4. RNA-seq analysis showed upregulated NRG expression in WT mice after MI compared to untreated mice, which was significantly higher in bioinformatically isolated CCR2+ cells. Conclusions: Taken together, the results suggest that Nrf2 signalling in leukocytes, and possibly CCR2+ monocyte-derived cardiac resident macrophages, may be potential targets to prevent post-MI ventricular remodeling.

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Section: Introductionmentioning

confidence: 99%

Nrf2 attenuates the innate immune response after experimental myocardial infarction

Bromage

Trevelin

Huntington

et al. 2022

Preprint

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“…18,19 In the remodeling non-infarcted myocardium, mechanical stress may activate macrophages and can contribute to adverse fibrotic remodeling and dysfunction. 10,20 The members of the TGF-β superfamily potently modulate myeloid cell phenotype and function. 21,22 In the healing infarct, all three TGF-β isoforms are induced and activated, and have been suggested to regulate inflammation, repair, remodeling, and fibrosis.…”

Section: Introductionmentioning

confidence: 99%

The role of endogenous Smad7 in regulating macrophage phenotype following myocardial infarction

Tuleta

et al. 2022

The FASEB Journal

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Smad7 restrains TGF‐β responses, and has been suggested to exert both pro‐ and anti‐inflammatory actions that may involve effects on macrophages. Myocardial infarction triggers a macrophage‐driven inflammatory response that not only plays a central role in cardiac repair, but also contributes to adverse remodeling and fibrosis. We hypothesized that macrophage Smad7 expression may regulate inflammation and fibrosis in the infarcted heart through suppression of TGF‐β responses, or via TGF‐independent actions. In a mouse model of myocardial infarction, infiltration with Smad7+ macrophages peaked 7 days after coronary occlusion. Myeloid cell‐specific Smad7 loss in mice had no effects on homeostatic functions and did not affect baseline macrophage gene expression. RNA‐seq predicted that Smad7 may promote TREM1‐mediated inflammation in infarct macrophages. However, these alterations in the transcriptional profile of macrophages were associated with a modest and transient reduction in infarct myofibroblast infiltration, and did not affect dysfunction, chamber dilation, scar remodeling, collagen deposition, and macrophage recruitment. In vitro, RNA‐seq and PCR arrays showed that TGF‐β has profound effects on macrophage profile, attenuating pro‐inflammatory cytokine/chemokine expression, modulating synthesis of matrix remodeling genes, inducing genes associated with sphingosine‐1 phosphate activation and integrin signaling, and inhibiting cholesterol biosynthesis genes. However, Smad7 loss did not significantly affect TGF‐β‐mediated macrophage responses, modulating synthesis of only a small fraction of TGF‐β‐induced genes, including Itga5, Olfml3, and Fabp7. Our findings suggest a limited role for macrophage Smad7 in regulation of post‐infarction inflammation and repair, and demonstrate that the anti‐inflammatory effects of TGF‐β in macrophages are not restrained by endogenous Smad7 induction.

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“…Regulation of immune function and inflammatory response is an important strategy for the treatment of CVMDs [20][21][22][23][24]. Increasing evidences show that tissue-resident immune cells are involved in regulating the pathophysiological processes of CVMDs [25][26][27][28]. Local tissues, such as vascular endothelium and adipose tissue, also have an important impact on the occurrence and development of CVMDs [29][30][31][32].…”

Section: Introductionmentioning

confidence: 99%

Developmental endothelial locus-1 in cardiovascular and metabolic diseases: a promising biomarker and therapeutic target

Zhao

Zheng

et al. 2022

Preprint

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Cardiovascular and metabolic diseases (CVMDs) are a leading cause of death worldwide and imposes a huge socioeconomic burden on individuals and healthcare systems, underscoring the urgent need to develop new drug therapies. Developmental endothelial locus-1 (DEL-1) is a secreted multifunctional domain protein that can bind to integrins and play an important role in the occurrence and development of various diseases. Recently, DEL-1 has attracted great interest for its pharmacological role in the treatment and/or management of CVMDs. In this review, we present the current knowledge on the predictive and therapeutic role of DEL-1 in a variety of CVMDs, such as atherosclerosis, hypertension, cardiac remodeling, ischemic heart disease, obesity, and insulin resistance. Collectively, DEL-1 is a promising biomarker and therapeutic target for CVMDs.

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Resident Cardiac Macrophages Mediate Adaptive Myocardial Remodeling

Cited by 13 publications

References 69 publications

Nrf2 attenuates the innate immune response after experimental myocardial infarction

Nrf2 attenuates the innate immune response after experimental myocardial infarction

The role of endogenous Smad7 in regulating macrophage phenotype following myocardial infarction

Developmental endothelial locus-1 in cardiovascular and metabolic diseases: a promising biomarker and therapeutic target

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