Chamber identity programs drive early functional partitioning of the heart

Christian Mosimann(Boston Children's Hospital), Daniela Panáková(Brigham and Women's Hospital), Andreas A. Werdich(Brigham and Women's Hospital), Gabriel Musso(Brigham and Women's Hospital), Alexa Burger(University of Zurich), Katy L. Lawson(Boston Children's Hospital), Logan A. Carr(Boston Children's Hospital), Kathleen R. Nevis(Harvard University), M. Khaled Sabeh(Brigham and Women's Hospital), Yi Zhou(Boston Children's Hospital), Alan J. Davidson(Boston Children's Hospital), Anthony DiBiase(Boston Children's Hospital), Caroline E. Burns(Harvard University), C. Geoffrey Burns(Harvard University), Calum A. MacRae(Brigham and Women's Hospital), Leonard I. Zon(Boston Children's Hospital)
Nature Communications
August 26, 2015
Cited by 127Open Access
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Abstract

The vertebrate heart muscle (myocardium) develops from the first heart field (FHF) and expands by adding second heart field (SHF) cells. While both lineages exist already in teleosts, the primordial contributions of FHF and SHF to heart structure and function remain incompletely understood. Here we delineate the functional contribution of the FHF and SHF to the zebrafish heart using the cis-regulatory elements of the draculin (drl) gene. The drl reporters initially delineate the lateral plate mesoderm, including heart progenitors. Subsequent myocardial drl reporter expression restricts to FHF descendants. We harnessed this unique feature to uncover that loss of tbx5a and pitx2 affect relative FHF versus SHF contributions to the heart. High-resolution physiology reveals distinctive electrical properties of each heart field territory that define a functional boundary within the single zebrafish ventricle. Our data establish that the transcriptional program driving cardiac septation regulates physiologic ventricle partitioning, which successively provides mechanical advantages of sequential contraction.


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