Literature DB >> 15699019

Identification of direct serum-response factor gene targets during Me2SO-induced P19 cardiac cell differentiation.

Shu Xing Zhang1, Eduardo Garcia-Gras, Diane R Wycuff, Suzanne J Marriot, Nijiati Kadeer, Wei Yu, Eric N Olson, Daniel J Garry, Michael S Parmacek, Robert J Schwartz.   

Abstract

Serum-response factor (SRF) is an obligatory transcription factor, required for the formation of vertebrate mesoderm leading to the origin of the cardiovascular system. Protein A-TEV-tagged chromatin immunoprecipitation technology was used to collect direct SRF-bound gene targets from pluripotent P19 cells, induced by Me2SO treatment into an enriched cardiac cell population. From 242 sequenced DNA fragments, we identified 188 genomic DNA fragments as potential direct SRF targets that contain CArG boxes and CArG-like boxes. Of the 92 contiguous genes that were identified, a subgroup of 43 SRF targets was then further validated by co-transfection assays with SRF. Expression patterns of representative candidate genes were compared with the LacZ reporter expression activity of the endogenous SRF gene. According to the Unigene data base, 84% of the SRF target candidates were expressed, at least, in the heart. In SRF null embryonic stem cells, 81% of these SRF target candidates were greatly affected by the absence of SRF. Among these SRF-regulated genes, Raf1, Map4k4, and Bicc1 have essential roles in mesoderm formation. The 12 regulated SRF target genes, Mapk10 (JNK3), Txnl2, Azi2, Tera, Sema3a, Lrp4, Actc1, Myl3, Hspg2, Pgm2, Hif3a, and Asb5, have been implicated in cardiovascular formation, and the Ski and Hes6 genes have roles in muscle differentiation. SRF target genes related to cell mitosis and cycle, E2f5, Npm1, Cenpb, Rbbp6, and Scyl1, expressed in the heart tissue were differentially regulated in SRF null ES cells.

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Year:  2005        PMID: 15699019     DOI: 10.1074/jbc.M413793200

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


  42 in total

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2.  Defining the mammalian CArGome.

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Journal:  Genome Res       Date:  2005-12-19       Impact factor: 9.043

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Review 4.  The short and long of noncoding sequences in the control of vascular cell phenotypes.

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6.  Ischemic cardiac tissue conditioned media induced differentiation of human mesenchymal stem cells into early stage cardiomyocytes.

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

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

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10.  Tbx1 regulates the BMP-Smad1 pathway in a transcription independent manner.

Authors:  F Gabriella Fulcoli; Tuong Huynh; Peter J Scambler; Antonio Baldini
Journal:  PLoS One       Date:  2009-06-25       Impact factor: 3.240

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