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1. DOT1L regulates chamber-specific transcriptional networks during cardiogenesis and mediates postnatal cell cycle withdrawal

2. Nexilin Is a New Component of Junctional Membrane Complexes Required for Cardiac T-Tubule Formation

4. Fate mapping and scRNA sequencing reveal origin and diversity of lymph node stromal precursors

5. Infarct Fibroblasts Do Not Derive From Bone Marrow Lineages

6. Are Perivascular Adipocyte Progenitors Mural Cells or Adventitial Fibroblasts?

7. Pericytes of Multiple Organs Do Not Behave as Mesenchymal Stem Cells In Vivo

8. Redox Paradox: Can Hypoxia Heal Ischemic Hearts?

10. HIF1α Represses Cell Stress Pathways to Allow Proliferation of Hypoxic Fetal Cardiomyocytes

11. Increasing Mononuclear Diploid Cardiomyocytes by Loss of E2F Transcription Factor 7/8 Fails to Improve Cardiac Regeneration After Infarct

12. The epigenetic modifier DOT1L regulates gene regulatory networks necessary for cardiac patterning and cardiomyocyte cell cycle withdrawal

14. IL-11 is a crucial determinant of cardiovascular fibrosis

16. The epigenetic modifier DOT1L regulates gene regulatory networks necessary for cardiac patterning and cardiomyocyte cell cycle withdrawal

20. Transcriptional heterogeneity of fibroblasts is a hallmark of the aging heart

21. Interleukin-11 is a therapeutic target in idiopathic pulmonary fibrosis

22. IL-11 is a therapeutic target in idiopathic pulmonary fibrosis

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24. Luma is not essential for murine cardiac development and function

27. Parallel Lineage-Tracing Studies Establish Fibroblasts as the Prevailing In VivoAdipocyte Progenitor

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