Single-cell expression profiling reveals dynamic flux of cardiac stromal, vascular and immune cells in health and injury
| Autor: | Vaibhao Janbandhu, Robert E. Nordon, Joshua W. K. Ho, Ralph Patrick, Munira Xaymardan, Katharina Wystub-Lis, Aude Dorison, Richard P. Harvey, Nona Farbehi |
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| Rok vydání: | 2019 |
| Předmět: |
Male
0301 basic medicine Myeloid Stromal cell Mouse QH301-705.5 Science Cell Myocardial Infarction Cell Communication heart 030204 cardiovascular system & hematology Biology General Biochemistry Genetics and Molecular Biology Interstitial cell Transcriptome Mice 03 medical and health sciences 0302 clinical medicine scRNA-seq medicine Animals Regeneration Cell Lineage Biology (General) Fibroblast Wound Healing General Immunology and Microbiology Gene Expression Profiling General Neuroscience Regeneration (biology) Cell Biology General Medicine 3. Good health Cell biology Disease Models Animal 030104 developmental biology medicine.anatomical_structure Medicine Single-Cell Analysis Myofibroblast Research Article Computational and Systems Biology |
| Zdroj: | eLife eLife, Vol 8 (2019) |
| ISSN: | 2050-084X |
| Popis: | 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. eLife digest In our bodies, heart attacks lead to cell death and inflammation. This is then followed by a healing phase where the organ repairs itself. There are many types of heart cells, from muscle and pacemaker cells that help to create the beating motion, to so-called fibroblasts that act as a supporting network. Yet, it is still unclear how individual cells participate in the heart's response to injury. All cells possess the same genetic information, but they turn on or off different genes depending on the specific tasks that they need to perform. Spotting which genes are activated in individual cells can therefore provide clues about their exact roles in the body. Until recently, technological limitations meant that this information was difficult to access, because it was only possible to capture the global response of a group of cells in a sample. A new method called single-cell RNA sequencing is now allowing researchers to study the activities of many genes in thousands of individual cells at the same time. Here, Farbehi, Patrick et al. performed single-cell RNA sequencing on over 30,000 individual cells from healthy and injured mouse hearts. Computational approaches were then used to cluster cells into groups according to the activities of their genes. The experiments identified over 30 distinct sub-types of cell, including several that were previously unknown. For example, a group of fibroblasts that express a gene called Wif1 was discovered. Previous genetic studies have shown that Wif1 is essential for the heart's response to injury. Further experiments by Farbehi, Patrick et al. indicated that this new sub-type of cells may control the timing of the different aspects of heart repair after damage. Tens of millions of people around the world suffer from heart attacks and other heart diseases. Knowing how different types of heart cells participate in repair mechanisms may help to find new targets for drugs and other treatments. |
| Databáze: | OpenAIRE |
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