Chang Shurong, McKinsey Timothy A, Zhang Chun Li, Richardson James A, Hill Joseph A, Olson Eric N
Department of Molecular Biology, University of Texas Southwestern Medical Center, 6000 Harry Hines Blvd., Dallas, TX 75390-9148, USA.
Mol Cell Biol. 2004 Oct;24(19):8467-76. doi: 10.1128/MCB.24.19.8467-8476.2004.
The adult heart responds to stress signals by hypertrophic growth, which is often accompanied by activation of a fetal cardiac gene program and eventual cardiac demise. We showed previously that histone deacetylase 9 (HDAC9) acts as a suppressor of cardiac hypertrophy and that mice lacking HDAC9 are sensitized to cardiac stress signals. Here we report that mice lacking HDAC5 display a similar cardiac phenotype and develop profoundly enlarged hearts in response to pressure overload resulting from aortic constriction or constitutive cardiac activation of calcineurin, a transducer of cardiac stress signals. In contrast, mice lacking either HDAC5 or HDAC9 show a hypertrophic response to chronic beta-adrenergic stimulation identical to that of wild-type littermates, suggesting that these HDACs modulate a specific subset of cardiac stress response pathways. We also show that compound mutant mice lacking both HDAC5 and HDAC9 show a propensity for lethal ventricular septal defects and thin-walled myocardium. These findings reveal central roles for HDACs 5 and 9 in the suppression of a subset of cardiac stress signals as well as redundant functions in the control of cardiac development.
成年心脏通过肥大性生长对压力信号作出反应,这种生长通常伴随着胎儿心脏基因程序的激活以及最终的心脏死亡。我们之前表明,组蛋白去乙酰化酶9(HDAC9)作为心脏肥大的抑制因子,缺乏HDAC9的小鼠对心脏压力信号敏感。在此我们报告,缺乏HDAC5的小鼠表现出类似的心脏表型,并且在因主动脉缩窄或钙调神经磷酸酶(一种心脏压力信号转导因子)的组成性心脏激活导致压力过载时,心脏会显著增大。相比之下,缺乏HDAC5或HDAC9的小鼠对慢性β-肾上腺素能刺激的肥大反应与野生型同窝小鼠相同,这表明这些HDAC调节心脏压力反应途径的特定子集。我们还表明,同时缺乏HDAC5和HDAC9的复合突变小鼠有发生致命性室间隔缺损和薄壁心肌的倾向。这些发现揭示了HDAC5和HDAC9在抑制一部分心脏压力信号方面的核心作用以及在心脏发育控制中的冗余功能。
