Literature DB >> 15929941

Conditional mutagenesis of the murine serum response factor gene blocks cardiogenesis and the transcription of downstream gene targets.

Zhiyv Niu1, Wei Yu, Shu Xing Zhang, Matthew Barron, Narasimhaswamy S Belaguli, Michael D Schneider, Michael Parmacek, Alfred Nordheim, Robert J Schwartz.   

Abstract

Serum response factor (SRF) homozygous-null embryos from our backcross of SRF(LacZ/)(+) "knock-in" mice failed to gastrulate and form mesoderm, similar to the findings of an earlier study (Arsenian, S., Weinhold, B., Oelgeschlager, M., Ruther, U., and Nordheim, A. (1998) EMBO J. 17, 6289-6299). Our use of embryonic stem cells provided a model system that could be used to investigate the specification of multiple embryonic lineages, including cardiac myocytes. We observed the absence of myogenic alpha-actins, SM22alpha, and myocardin expression and the failure to form beating cardiac myocytes in aggregated SRF null embryonic stem cells, whereas the appearance of transcription factors Nkx2-5 and GATA4 were unaffected. To study the role of SRF during heart organogenesis, we then performed cardiac-specific ablation of SRF by crossing the transgenic alpha-myosin heavy chain Cre recombinase line with SRF LoxP-engineered mice. Cardiac-specific ablation of SRF resulted in embryonic lethality due to cardiac insufficiency during chamber maturation. Conditional ablation of SRF also reduced cell survival concomitant with increased apoptosis and reduced cellularity. Significant reductions in SRF (> or =95%), atrial naturetic factor (> or =80%), and cardiac (> or =60%), skeletal (> or =90%), and smooth muscle (> or =75%) alpha-actin transcripts were also observed in the cardiac-conditional knock-out heart. This was consistent with the idea that SRF directs de novo cardiac and smooth muscle gene activities. Finally, quantitation of the knock-in LacZ reporter gene transcripts in the hearts of cardiac-conditional knock-out embryos revealed an approximately 30% reduction in gene activity, indicating SRF gene autoregulation during cardiogenesis.

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Year:  2005        PMID: 15929941     DOI: 10.1074/jbc.M501372200

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  55 in total

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Review 4.  Re-employment of developmental transcription factors in adult heart disease.

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Journal:  Semin Cell Dev Biol       Date:  2006-11-24       Impact factor: 7.727

5.  Defining the mammalian CArGome.

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6.  Requirement of myocardin-related transcription factor-B for remodeling of branchial arch arteries and smooth muscle differentiation.

Authors:  Jiyeon Oh; James A Richardson; Eric N Olson
Journal:  Proc Natl Acad Sci U S A       Date:  2005-10-04       Impact factor: 11.205

7.  Histone deacetylase 3 modulates Tbx5 activity to regulate early cardiogenesis.

Authors:  Sara L Lewandowski; Harish P Janardhan; Kevin M Smee; Marcos Bachman; Zheng Sun; Mitchell A Lazar; Chinmay M Trivedi
Journal:  Hum Mol Genet       Date:  2014-02-23       Impact factor: 6.150

8.  Serum response factor: positive and negative regulation of an epithelial gene expression network in the destrin mutant cornea.

Authors:  Sharolyn V Kawakami-Schulz; Angela M Verdoni; Shannon G Sattler; Erik Jessen; Winston W-Y Kao; Akihiro Ikeda; Sakae Ikeda
Journal:  Physiol Genomics       Date:  2014-02-18       Impact factor: 3.107

9.  Characteristics of the CArG-SRF binding context in mammalian genomes.

Authors:  Wenwu Wu; Xia Shen; Shiheng Tao
Journal:  Mamm Genome       Date:  2009-12-03       Impact factor: 2.957

10.  Effect of destrin mutations on the gene expression profile in vivo.

Authors:  Angela M Verdoni; Natsuyo Aoyama; Akihiro Ikeda; Sakae Ikeda
Journal:  Physiol Genomics       Date:  2008-04-01       Impact factor: 3.107

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