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Ichiro Manabe, Gary K. Owens
J Clin Invest. 2001;
107(7):823
doi:10.1172/JCI11385
Abstract |
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E
xpression of smooth muscle myosin heavy chain (SM-MHC) is tightly controlled depending on the differentiated state of smooth muscle cells (SMCs). To better understand the mechanisms that regulate transcription of the SM-MHC gene in vivo, we tested the function of several conserved CArG elements contained within the –4200 to +11600 region of this gene that we had previously shown to drive SMC-specific expression in transgenic mice. CArG1 in the 5′-flanking sequence was required for all SMCs, while CArG2 and a novel intronic CArG element were differentially required in SMC subtypes. Of particular note, mutation of the intronic CArG selectively abolished expression in large arteries. A promoter construct containing three repeats of a conserved 227-bp intronic CArG-containing region was sufficient to direct transcription in vascular SMCs in transgenic mice, although this construct was also expressed in skeletal and cardiac muscle. These results support a model in which transcriptional regulation of SM-MHC is controlled by multiple positive and negative modular control regions that differ between SMCs and non-SMCs and among SMC subtypes. We also demonstrated that the CArG elements of the endogenous SM-MHC gene were bound by SRF in chromatin.
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(19)
| Title and authors |
Publication |
Year |
Epigenetic Control of Smooth Muscle Cell Differentiation and Phenotypic Switching in Vascular Development and Disease
Matthew R. Alexander, Gary K. Owens
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Annu. Rev. Physiol.
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2012 |
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Basic & Clinical Pharmacology & Toxicology
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2011 |
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Rutger J. Wierda, Sacha B. Geutskens, J. Wouter Jukema, Paul H.A. Quax, Peter J. Van Den Elsen
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Journal of Cellular and Molecular Medicine
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2010 |
Cardiac fibroblasts are essential for the adaptive response of the murine heart to pressure overload
Norifumi Takeda, Ichiro Manabe, Yuichi Uchino, Kosei Eguchi, Sahohime Matsumoto, Satoshi Nishimura, Takayuki Shindo, Motoaki Sano, Kinya Otsu, Paige Snider, Simon J. Conway, Ryozo Nagai
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J. Clin. Invest.
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2009 |
Smooth muscle phenotypic modulation is an early event in aortic aneurysms.
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The Journal of Thoracic and Cardiovascular Surgery
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2009 |
Forkhead box M1 transcriptional factor is required for smooth muscle cells during embryonic development of blood vessels and esophagus.
Vladimir Ustiyan, I-Ching Wang, Xiaomeng Ren, Yufang Zhang, Jonathan Snyder, Yan Xu, Susan E Wert, James L Lessard, Tanya V Kalin, Vladimir V Kalinichenko
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Developmental Biology
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2009 |
The role of lysophosphatidic acid receptors in phenotypic modulation of vascular smooth muscle cells
Zhibin Zhou, Jianping Niu, Zhijun Zhang
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Mol Biol Rep
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2009 |
The effects of stretch on vascular smooth muscle cell phenotype in vitro
Anastassi T. Halka, Neill J. Turner, Andrew Carter, Jonathan Ghosh, Michael O. Murphy, John P. Kirton, Cay M. Kielty, Michael G. Walker
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Cardiovascular Pathology
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2008 |
5′ CArG degeneracy in smooth muscle α-actin is required for injury-induced gene suppression in vivo
Jennifer A. Hendrix, Brian R. Wamhoff, Oliver G. McDonald, Sanjay Sinha, Tadashi Yoshida, Gary K. Owens
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J. Clin. Invest.
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2005 |
Krüppel-like transcription factor KLF5 is a key regulator of adipocyte differentiation
Yumiko Oishi, Ichiro Manabe, Kazuyuki Tobe, Kensuke Tsushima, Takayuki Shindo, Katsuhito Fujiu, Go Nishimura, Koji Maemura, Toshimasa Yamauchi, Naoto Kubota, Ryo Suzuki, Toshio Kitamura, Shizuo Akira, Takashi Kadowaki, Ryozo Nagai
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Cell Metabolism
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2005 |
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