关于心肌α-肌动蛋白(ACTC1)基因突变对血清反应因子(SRF)信号传导作用的数据。
Data on the role of cardiac α-actin (ACTC1) gene mutations on SRF-signaling.
作者信息
Rangrez Ashraf Yusuf, Kilian Lucia, Stiebeling Katharina, Dittmann Sven, Yadav Pankaj, Schulze-Bahr Eric, Frey Norbert, Frank Derk
机构信息
Department of Internal Medicine III, Cardiology and Angiology, University Medical Center Schleswig-Holstein, Campus Kiel, Kiel, Germany.
Institute for Genetics of Heart Diseases (IfGH), Department of Cardiovascular Medicine, University Hospital Münster, Münster, Germany.
出版信息
Data Brief. 2020 Jan 2;28:105071. doi: 10.1016/j.dib.2019.105071. eCollection 2020 Feb.
We recently reported a novel, heterozygous, and non-synonymous ACTC1 mutation (p.Gly247Asp or G247D) in a large, multi-generational family, causing atrial-septal defect followed by late-onset dilated cardiomyopathy (DCM). We also found that the G247D ACTC1 mutation negatively regulated serum response (SRF)-signaling thereby contributing to the late-onset DCM observed in human patients carrying this mutation ("A cardiac α-actin (ACTC1) p. Gly247Asp mutation inhibits SRF-signaling in vitro in neonatal rat cardiomyocytes" [1]). There are some ACTC1 mutations known to date, majority of which, though, have not been investigated for their functional consequence. We thus aimed at determining the functional impact of various ACTC1 gene mutations on SRF-signaling using SM22-response element driven firefly luciferase activity assays in C2C12 cells.
我们最近在一个大型的多代家族中报道了一种新的、杂合的非同义ACTC1突变(p.Gly247Asp或G247D),该突变导致房间隔缺损,随后发展为迟发性扩张型心肌病(DCM)。我们还发现,G247D ACTC1突变对血清反应因子(SRF)信号传导具有负调控作用,从而导致携带该突变的人类患者出现迟发性DCM(“心脏α-肌动蛋白(ACTC1)p.Gly247Asp突变在新生大鼠心肌细胞中体外抑制SRF信号传导”[1])。迄今为止已知一些ACTC1突变,不过其中大多数尚未对其功能后果进行研究。因此,我们旨在使用C2C12细胞中由SM22反应元件驱动的萤火虫荧光素酶活性测定法,来确定各种ACTC1基因突变对SRF信号传导的功能影响。
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