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

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

Besides cardiomyocytes (CM), the heart contains numerous interstitial cell types which play key roles in heart repair, regeneration and disease, including fibroblast, vascular and immune cells. However, a comprehensive understanding of this interactive cell community is lacking. We performed single-cell RNA-sequencing of the total non-CM fraction and enriched (Pdgfra-GFP+) fibroblast lineage cells from murine hearts at days 3 and 7 post-sham or myocardial infarction (MI) surgery. Clustering of >30,000 single cells identified >30 populations representing nine cell lineages, including a previously undescribed fibroblast lineage trajectory present in both sham and MI hearts leading to a uniquely activated cell state defined in part by a strong anti-WNT transcriptome signature. We also uncovered novel myofibroblast subtypes expressing either pro-fibrotic or anti-fibrotic signatures. Our data highlight non-linear dynamics in myeloid and fibroblast lineages after cardiac injury, and provide an entry point for deeper analysis of cardiac homeostasis, inflammation, fibrosis, repair and regeneration.

[1] P. Shannon,et al. Cytoscape: a software environment for integrated models of biomolecular interaction networks. , 2003, Genome research.

[2] M. Kawaichi,et al. Developmentally regulated expression of mouse HtrA3 and its role as an inhibitor of TGF‐β signaling , 2004, Development, growth & differentiation.

[3] Birger Rapp,et al. On the value of IT , 2005 .

[4] Arjun Deb,et al. Secreted frizzled related protein 2 (Sfrp2) is the key Akt-mesenchymal stem cell-released paracrine factor mediating myocardial survival and repair , 2007, Proceedings of the National Academy of Sciences.

[5] P. Libby,et al. The healing myocardium sequentially mobilizes two monocyte subsets with divergent and complementary functions , 2007, The Journal of experimental medicine.

[6] William Stafford Noble,et al. Transcription , 2003, Chemistry and Biology of Non‐Canonical Nucleic Acids.

[7] Mitsuru Nenoi,et al. Regulation of , 2004 .

[8] Hadley Wickham,et al. ggplot2 - Elegant Graphics for Data Analysis (2nd Edition) , 2017 .

[9] Zoltán Molnár,et al. Neurovascular congruence during cerebral cortical development. , 2009, Cerebral cortex.

[10] Juanjuan Shan,et al. Blockade of Wnt signaling inhibits angiogenesis and tumor growth in hepatocellular carcinoma. , 2009, Cancer research.

[11] N. Rosenthal,et al. Revealing New Mouse Epicardial Cell Markers through Transcriptomics , 2010, PloS one.

[12] N. S. Asli,et al. Adult cardiac-resident MSC-like stem cells with a proepicardial origin. , 2011, Cell stem cell.

[13] Leah B. Honor,et al. Adult mouse epicardium modulates myocardial injury by secreting paracrine factors. , 2011, The Journal of clinical investigation.

[14] L. Patthy,et al. Characterization of a Wnt‐binding site of the WIF‐domain of Wnt inhibitory factor‐1 , 2012, FEBS letters.

[15] Z. Popović,et al. Thrombospondin‐4 regulates fibrosis and remodeling of the myocardium in response to pressure overload , 2012, FASEB journal : official publication of the Federation of American Societies for Experimental Biology.

[16] Takako Sasaki,et al. The Wnt antagonist Wif‐1 interacts with CTGF and inhibits CTGF activity , 2012, Journal of cellular physiology.

[17] Steven L Salzberg,et al. Fast gapped-read alignment with Bowtie 2 , 2012, Nature Methods.

[18] D. Knapp,et al. Connective tissue cells, but not muscle cells, are involved in establishing the proximo-distal outcome of limb regeneration in the axolotl , 2013, Development.

[19] Lianfeng Zhang,et al. WIF1 causes dysfunction of heart in transgenic mice , 2013, Transgenic Research.

[20] Xiaoping Zhou,et al. Interferon Induced IFIT Family Genes in Host Antiviral Defense , 2013, International journal of biological sciences.

[21] Thomas R. Gingeras,et al. STAR: ultrafast universal RNA-seq aligner , 2013, Bioinform..

[22] D. Sahoo,et al. Clonal precursor of bone, cartilage, and hematopoietic niche stromal cells , 2013, Proceedings of the National Academy of Sciences.

[23] Andrew McDavid,et al. Data exploration, quality control and testing in single-cell qPCR-based gene expression experiments , 2012, Bioinform..

[24] N. Rosenthal,et al. Progressive replacement of embryo-derived cardiac macrophages with age , 2014, The Journal of experimental medicine.

[25] Burkhard Rost,et al. LocTree3 prediction of localization , 2014, Nucleic Acids Res..

[26] D. Brenner,et al. Resident fibroblast lineages mediate pressure overload-induced cardiac fibrosis. , 2014, The Journal of clinical investigation.

[27] P. Libby,et al. Chigh Monocytes Depend on Nr 4 a 1 to Balance Both Inflammatory and Reparative Phases in the Infarcted Myocardium , 2014 .

[28] R. Weissleder,et al. Differential Contribution of Monocytes to Heart Macrophages in Steady-State and After Myocardial Infarction , 2014, Circulation research.

[29] N. Frangogiannis,et al. Fibroblasts in myocardial infarction: a role in inflammation and repair. , 2014, Journal of molecular and cellular cardiology.

[30] M. Yoder,et al. Circulating and Tissue Resident Endothelial Progenitor Cells , 2013, Journal of cellular physiology.

[31] T. Vondriska,et al. Mesenchymal-endothelial-transition contributes to cardiac neovascularization , 2014, Nature.

[32] R Core Team,et al. R: A language and environment for statistical computing. , 2014 .

[33] Ansuman T. Satpathy,et al. Embryonic and adult-derived resident cardiac macrophages are maintained through distinct mechanisms at steady state and during inflammation. , 2014, Immunity.

[34] D. Mann,et al. Distinct macrophage lineages contribute to disparate patterns of cardiac recovery and remodeling in the neonatal and adult heart , 2014, Proceedings of the National Academy of Sciences.

[35] K. Ting,et al. Fibromodulin-Deficiency Alters Temporospatial Expression Patterns of Transforming Growth Factor-β Ligands and Receptors during Adult Mouse Skin Wound Healing , 2014, PloS one.

[36] S. Rho,et al. WIF1 can effectively co-regulate pro-apoptotic activity through the combination with DKK1. , 2014, Cellular signalling.

[37] Wei Shi,et al. featureCounts: an efficient general purpose program for assigning sequence reads to genomic features , 2013, Bioinform..

[38] E. Olson,et al. Macrophages are required for neonatal heart regeneration. , 2014, The Journal of clinical investigation.

[39] Richard T. Lee,et al. Nerves Regulate Cardiomyocyte Proliferation and Heart Regeneration. , 2015, Developmental cell.

[40] T. Shiomi,et al. Loss of Secreted Frizzled-Related Protein-1 Leads to Deterioration of Cardiac Function in Mice and Plays a Role in Human Cardiomyopathy , 2015, Circulation. Heart failure.

[41] Youmna Kfoury,et al. Mesenchymal cell contributions to the stem cell niche. , 2015, Cell stem cell.

[42] D. Mann,et al. Role of innate and adaptive immune mechanisms in cardiac injury and repair , 2015, Nature Reviews Immunology.

[43] Piero Carninci,et al. A draft network of ligand–receptor-mediated multicellular signalling in human , 2015, Nature Communications.

[44] Amitava Das,et al. Monocyte and macrophage plasticity in tissue repair and regeneration. , 2015, The American journal of pathology.

[45] Phillip G. Popovich,et al. Novel Markers to Delineate Murine M1 and M2 Macrophages , 2015, PloS one.

[46] I. Macaulay,et al. PDGFRα demarcates the cardiogenic clonogenic Sca1+ stem/progenitor cell in adult murine myocardium , 2015, Nature Communications.

[47] M. Neeman,et al. ERBB2 triggers mammalian heart regeneration by promoting cardiomyocyte dedifferentiation and proliferation , 2015, Nature Cell Biology.

[48] M. Entman,et al. Tumor necrosis factor: a mechanistic link between angiotensin-II-induced cardiac inflammation and fibrosis. , 2015, Circulation. Heart failure.

[49] Deepak Srivastava,et al. In Vivo Cellular Reprogramming: The Next Generation , 2016, Cell.

[50] Grace X. Y. Zheng,et al. Massively parallel digital transcriptional profiling of single cells , 2016, bioRxiv.

[51] N. Rosenthal,et al. Revisiting Cardiac Cellular Composition. , 2016, Circulation research.

[52] Peter Kohl,et al. Novel therapeutic strategies targeting fibroblasts and fibrosis in heart disease , 2016, Nature Reviews Drug Discovery.

[53] B. Aronow,et al. Genetic lineage tracing defines myofibroblast origin and function in the injured heart , 2016, Nature Communications.

[54] M. Nahrendorf,et al. Abandoning M1/M2 for a Network Model of Macrophage Function. , 2016, Circulation research.

[55] J. Kovacic,et al. Matricellular Protein CCN5 Reverses Established Cardiac Fibrosis. , 2016, Journal of the American College of Cardiology.

[56] S. Jacobsen,et al. Primitive Embryonic Macrophages are Required for Coronary Development and Maturation. , 2016, Circulation research.

[57] Carla M. T. Bauer,et al. Self-renewing resident arterial macrophages arise from embryonic CX3CR1+ precursors and circulating monocytes immediately after birth , 2015, Nature Immunology.

[58] Fabian J. Theis,et al. destiny: diffusion maps for large-scale single-cell data in R , 2015, Bioinform..

[59] Malina J. Ivey,et al. Defining the Cardiac Fibroblast. , 2016, Circulation journal : official journal of the Japanese Circulation Society.

[60] M. Czubryt,et al. The transcription factor scleraxis is a critical regulator of cardiac fibroblast phenotype , 2016, BMC Biology.

[61] K. Yutzey,et al. Cardiac Fibrosis: The Fibroblast Awakens. , 2016, Circulation research.

[62] Grace X. Y. Zheng,et al. Massively parallel digital transcriptional profiling of single cells , 2016, Nature Communications.

[63] Bin Yu,et al. iterative Random Forests to discover predictive and stable high-order interactions , 2017 .

[64] H. Niessen,et al. On the value of therapeutic interventions targeting the complement system in acute myocardial infarction. , 2017, Translational research : the journal of laboratory and clinical medicine.

[65] A. James,et al. Fibromodulin reduces scar formation in adult cutaneous wounds by eliciting a fetal-like phenotype , 2017, Signal Transduction and Targeted Therapy.

[66] Shaohua Zhang,et al. Preexisting endothelial cells mediate cardiac neovascularization after injury , 2017, The Journal of clinical investigation.

[67] C. Dieterich,et al. The cardiac microenvironment uses non‐canonical WNT signaling to activate monocytes after myocardial infarction , 2017, EMBO molecular medicine.

[68] A. Regev,et al. Scaling single-cell genomics from phenomenology to mechanism , 2017, Nature.

[69] Damian Szklarczyk,et al. The STRING database in 2017: quality-controlled protein–protein association networks, made broadly accessible , 2016, Nucleic Acids Res..

[70] M. Ramialison,et al. Multicellular Transcriptional Analysis of Mammalian Heart Regeneration , 2017, Circulation.

[71] Anushya Muruganujan,et al. PANTHER version 11: expanded annotation data from Gene Ontology and Reactome pathways, and data analysis tool enhancements , 2016, Nucleic Acids Res..

[72] N. Thielens,et al. C1q: A fresh look upon an old molecule. , 2017, Molecular immunology.

[73] Min S. Park,et al. Neurovascular patterning cues and implications for central and peripheral neurological disease , 2017, Surgical neurology international.

[74] C. Lien,et al. Frequency of mononuclear diploid cardiomyocytes underlies natural variation in heart regeneration , 2017, Nature Genetics.

[75] J. Molkentin,et al. Redefining the identity of cardiac fibroblasts , 2017, Nature Reviews Cardiology.

[76] A. Mescher. Macrophages and fibroblasts during inflammation and tissue repair in models of organ regeneration , 2017, Regeneration.

[77] N. Hacohen,et al. Single-cell RNA-seq reveals new types of human blood dendritic cells, monocytes, and progenitors , 2017, Science.

[78] S. V. Heesch,et al. IL-11 is a crucial determinant of cardiovascular fibrosis , 2017, Nature.

[79] J. Leor,et al. Loss of Macrophage Wnt Secretion Improves Remodeling and Function After Myocardial Infarction in Mice , 2017, Journal of the American Heart Association.

[80] D. Stainier,et al. Reciprocal analyses in zebrafish and medaka reveal that harnessing the immune response promotes cardiac regeneration , 2017, eLife.

[81] Andrej J. Savol,et al. IRF3 and Type I Interferons Fuel a Fatal Response to Myocardial Infarction , 2017, Nature Medicine.

[82] Andrej J. Savol,et al. Macrophages Facilitate Electrical Conduction in the Heart , 2017, Cell.

[83] J. Pollard,et al. Erythro-myeloid progenitors contribute endothelial cells to blood vessels , 2018, Nature.

[84] J. Molkentin,et al. Specialized fibroblast differentiated states underlie scar formation in the infarcted mouse heart , 2018, The Journal of clinical investigation.

[85] J. Kovacic,et al. Macrophage Biology, Classification, and Phenotype in Cardiovascular Disease: JACC Macrophage in CVD Series (Part 1). , 2018, Journal of the American College of Cardiology.

[86] N. Rosenthal,et al. The Macrophage in Cardiac Homeostasis and Disease: JACC Macrophage in CVD Series (Part 4). , 2018, Journal of the American College of Cardiology.

[87] N. S. Asli,et al. PDGFRα signaling in cardiac fibroblasts modulates quiescence, metabolism and self-renewal, and promotes anatomical and functional repair , 2017, bioRxiv.

[88] D. Kreisel,et al. The Human Heart Contains Distinct Macrophage Subsets with Divergent Origins and Functions , 2018, Nature Medicine.

[89] Paul Hoffman,et al. Integrating single-cell transcriptomic data across different conditions, technologies, and species , 2018, Nature Biotechnology.

[90] B. Wilkins,et al. Single-nucleus transcriptomic survey of cell diversity and functional maturation in postnatal mammalian hearts , 2018, Genes & development.

[91] A. van Oudenaarden,et al. Single-Cell Sequencing of the Healthy and Diseased Heart Reveals Cytoskeleton-Associated Protein 4 as a New Modulator of Fibroblasts Activation , 2018, Circulation.

[92] Jun Wang,et al. The Hippo pathway in the heart: pivotal roles in development, disease, and regeneration , 2018, Nature Reviews Cardiology.

[93] W. Matthijs Blankesteijn,et al. WNT Signaling in Cardiac and Vascular Disease , 2018, Pharmacological Reviews.

[94] M. Ni,et al. Single-Cell Transcriptome Analyses Reveal Endothelial Cell Heterogeneity in Tumors and Changes following Antiangiogenic Treatment. , 2018, Cancer research.

[95] F. Ginhoux,et al. Self-renewing resident cardiac macrophages limit adverse remodeling following myocardial infarction , 2018, Nature Immunology.

[96] M. Tallquist,et al. Resident fibroblast expansion during cardiac growth and remodeling. , 2018, Journal of molecular and cellular cardiology.

[97] M. Nahrendorf,et al. Cardioimmunology: the immune system in cardiac homeostasis and disease , 2018, Nature Reviews Immunology.

[98] James B. Brown,et al. Iterative random forests to discover predictive and stable high-order interactions , 2017, Proceedings of the National Academy of Sciences.

[99] K. Sigmundsson,et al. PDGFRα+ pericryptal stromal cells are the critical source of Wnts and RSPO3 for murine intestinal stem cells in vivo , 2018, Proceedings of the National Academy of Sciences.

[100] Daniel A. Skelly,et al. Single-Cell Transcriptional Profiling Reveals Cellular Diversity and Intercommunication in the Mouse Heart. , 2018, Cell reports.

[101] Jay A. Montgomery,et al. Multi-ethnic genome-wide association study for atrial fibrillation , 2018, Nature Genetics.

[102] D. Srivastava,et al. Regulation of Cell Cycle to Stimulate Adult Cardiomyocyte Proliferation and Cardiac Regeneration , 2017, Cell.

[103] Lianfeng Zhang,et al. Meox1 accelerates myocardial hypertrophic decompensation through Gata4 , 2018, Cardiovascular research.

[104] J. Kovacic,et al. Endothelial to Mesenchymal Transition in Cardiovascular Disease: JACC State-of-the-Art Review. , 2019, Journal of the American College of Cardiology.

[105] J. Kovacic,et al. Edinburgh Research Explorer Endothelial to Mesenchymal Transition in Cardiovascular Disease: Key Mechanisms and Clinical Translation Opportunities , 2022 .