4.8 Article

Pioneering function of Isl1 in the epigenetic control of cardiomyocyte cell fate

Journal

CELL RESEARCH
Volume 29, Issue 6, Pages 486-501

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/s41422-019-0168-1

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Funding

  1. LOEWE Center for Cell and Gene Therapy (CGT) - Hessian Ministry of Higher Education, Research and Arts [III L 4-518/17.004]
  2. Hessian Ministry of Higher Education, Research and Arts [III L 4-518/17.004 (2013)]
  3. DFG [SFB TRR 81, SFB 873, SFB 1213, SFB 1366]
  4. state of Baden-Wurttemberg
  5. Ministry of Science and Technology China [2013CB967400]
  6. National Natural Science Foundation of China (NSFC) [81570285]
  7. NIH [HL123747, HL119967]
  8. NSFC [SFB 1213, 81370196, 81670448]

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Generation of widely differing and specialized cell types from a single totipotent zygote involves large-scale transcriptional changes and chromatin reorganization. Pioneer transcription factors play key roles in programming the epigenome and facilitating recruitment of additional regulatory factors during successive cell lineage specification and differentiation steps. Here we show that Isl1 acts as a pioneer factor driving cardiomyocyte lineage commitment by shaping the chromatin landscape of cardiac progenitor cells. Using an Isl1 hypomorphic mouse line which shows congenital heart defects, genome-wide profiling of Isl1 binding together with RNA- and ATAC-sequencing of cardiac progenitor cells and their derivatives, we uncover a regulatory network downstream of Isl1 that orchestrates cardiogenesis. Mechanistically, we show that Isl1 binds to compacted chromatin and works in concert with the Brg1-Baf60c-based SWI/SNF complex to promote permissive cardiac lineage-specific alterations in the chromatin landscape not only of genes with critical functions in cardiac progenitor cells, but also of cardiomyocyte structural genes that are highly expressed when Isl1 itself is no longer present. Thus, the Isl1/Brg1-Baf60c complex plays a crucial role in orchestrating proper cardiogenesis and in establishing epigenetic memory of cardiomyocyte fate commitment.

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