Literature DB >> 24680892

AcvR1-mediated BMP signaling in second heart field is required for arterial pole development: implications for myocardial differentiation and regional identity.

Penny S Thomas1, Sudha Rajderkar1, Jamie Lane1, Yuji Mishina1, Vesa Kaartinen2.   

Abstract

BMP signaling plays an essential role in second heart field-derived heart and arterial trunk development, including myocardial differentiation, right ventricular growth, and interventricular, outflow tract and aortico-pulmonary septation. It is mediated by a number of different BMP ligands, and receptors, many of which are present simultaneously. The mechanisms by which they regulate morphogenetic events and degree of redundancy amongst them have still to be elucidated. We therefore assessed the role of BMP Type I receptor AcvR1 in anterior second heart field-derived cell development, and compared it with that of BmpR1a. By removing Acvr1 using the driver Mef2c[AHF]-Cre, we show that AcvR1 plays an essential role in arterial pole morphogenesis, identifying defects in outflow tract wall and cushion morphology that preceded a spectrum of septation defects from double outlet right ventricle to common arterial trunk in mutants. Its absence caused dysregulation in gene expression important for myocardial differentiation (Isl1, Fgf8) and regional identity (Tbx2, Tbx3, Tbx20, Tgfb2). Although these defects resemble to some degree those in the equivalent Bmpr1a mutant, a novel gene knock-in model in which Bmpr1a was expressed in the Acvr1 locus only partially restored septation in Acvr1 mutants. These data show that both BmpR1a and AcvR1 are needed for normal heart development, in which they play some non-redundant roles, and refine our understanding of the genetic and morphogenetic processes underlying Bmp-mediated heart development important in human congenital heart disease.
Copyright © 2014 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  BMP signaling; Cardiac development; Conotruncal defects; Receptors; Second heart field

Mesh:

Substances:

Year:  2014        PMID: 24680892      PMCID: PMC4057048          DOI: 10.1016/j.ydbio.2014.03.008

Source DB:  PubMed          Journal:  Dev Biol        ISSN: 0012-1606            Impact factor:   3.582


  77 in total

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2.  Isl1Cre reveals a common Bmp pathway in heart and limb development.

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3.  Distinct roles of Wnt/beta-catenin and Bmp signaling during early cardiogenesis.

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Journal:  Dev Dyn       Date:  2008-10       Impact factor: 3.780

5.  Morphogenesis of outflow tract rotation during cardiac development: the pulmonary push concept.

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Journal:  Dev Dyn       Date:  2012-07-30       Impact factor: 3.780

6.  Fibroblast growth factor 10 gene regulation in the second heart field by Tbx1, Nkx2-5, and Islet1 reveals a genetic switch for down-regulation in the myocardium.

Authors:  Yusuke Watanabe; Stéphane Zaffran; Atsushi Kuroiwa; Hiroaki Higuchi; Toshihiko Ogura; Richard P Harvey; Robert G Kelly; Margaret Buckingham
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Journal:  Biochimie       Date:  2013-05-28       Impact factor: 4.079

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  14 in total

1.  BMP signaling mediated by constitutively active Activin type 1 receptor (ACVR1) results in ectopic bone formation localized to distal extremity joints.

Authors:  Shailesh Agarwal; Shawn J Loder; Cameron Brownley; Oluwatobi Eboda; Jonathan R Peterson; Satoru Hayano; Bingrou Wu; Bin Zhao; Vesa Kaartinen; Victor C Wong; Yuji Mishina; Benjamin Levi
Journal:  Dev Biol       Date:  2015-02-23       Impact factor: 3.582

2.  BMP2 expression in the endocardial lineage is required for AV endocardial cushion maturation and remodeling.

Authors:  Jacob G Saxon; Daniel R Baer; Julie A Barton; Travis Hawkins; Bingruo Wu; Thomas C Trusk; Stephen E Harris; Bin Zhou; Yuji Mishina; Yukiko Sugi
Journal:  Dev Biol       Date:  2017-08-06       Impact factor: 3.582

3.  Analysis of Bone-Cartilage-Stromal Progenitor Populations in Trauma Induced and Genetic Models of Heterotopic Ossification.

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Journal:  Stem Cells       Date:  2016-05-18       Impact factor: 6.277

Review 4.  Cardiopulmonary and Neurologic Dysfunctions in Fibrodysplasia Ossificans Progressiva.

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Journal:  Biomedicines       Date:  2021-02-05

5.  Characterization of Cells Isolated from Genetic and Trauma-Induced Heterotopic Ossification.

Authors:  Shailesh Agarwal; James Drake; Ammar T Qureshi; Shawn Loder; Shuli Li; Kay Shigemori; Jonathan Peterson; David Cholok; Jonathan A Forsberg; Yuji Mishina; Thomas A Davis; Benjamin Levi
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7.  Evaluation of Salivary Cytokines for Diagnosis of both Trauma-Induced and Genetic Heterotopic Ossification.

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Journal:  Front Endocrinol (Lausanne)       Date:  2017-04-24       Impact factor: 5.555

8.  Mutations in Hnrnpa1 cause congenital heart defects.

Authors:  Zhe Yu; Paul Lf Tang; Jing Wang; Suying Bao; Joseph T Shieh; Alan Wl Leung; Zhao Zhang; Fei Gao; Sandra Yy Wong; Andy Lc Hui; Yuan Gao; Nelson Dung; Zhi-Gang Zhang; Yanhui Fan; Xueya Zhou; Yalun Zhang; Dana Sm Wong; Pak C Sham; Abid Azhar; Pui-Yan Kwok; Patrick Pl Tam; Qizhou Lian; Kathryn Se Cheah; Binbin Wang; You-Qiang Song
Journal:  JCI Insight       Date:  2018-01-25

Review 9.  BMP signaling and skeletal development in fibrodysplasia ossificans progressiva (FOP).

Authors:  Oscar Will Towler; Eileen M Shore
Journal:  Dev Dyn       Date:  2021-06-26       Impact factor: 2.842

10.  Global gene expression analysis combined with a genomics approach for the identification of signal transduction networks involved in postnatal mouse myocardial proliferation and development.

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