Critical role of Znhit1 for postnatal heart function and vacuolar cardiomyopathy
Yingchao Shi, Wenli Fan, Mingjie Xu, Xinhua Lin, Wukui Zhao, Zhongzhou Yang
Yingchao Shi, Wenli Fan, Mingjie Xu, Xinhua Lin, Wukui Zhao, Zhongzhou Yang
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Research Article Cardiology

Critical role of Znhit1 for postnatal heart function and vacuolar cardiomyopathy

Abstract

Ca2+ is critical for cardiac electrical conduction and contractility, and aberrant Ca2+ homeostasis causes arrhythmia and heart failure. Chromatin remodeling modulates gene expression involved in cardiac sarcomere assembly and postnatal heart function. However, the chromatin-remodeling regulatory mechanism of cardiac Ca2+ homeostasis is unknown. Here, we found that Znhit1, a core subunit of the SRCAP remodeling complex, was essential for heart function. Deletion of Znhit1 in postnatal hearts of mice resulted in arrhythmia, idiopathic vacuolar cardiomyopathy, rapid heart failure, and premature sudden death. In addition, the level of Casq1, a sarcoplasmic reticulum Ca2+ regulatory protein, was massively elevated while SERCA2a showed reduced protein level. Mechanistically, the Znhit1 modulated the expression of Casq1 and SERCA2a by depositing H2A.Z at their promoters. Deletion of Casq1 could substantially alleviate the vacuolar formation in Znhit1 Casq1 KO mice. These findings demonstrate that Znhit1 is required for postnatal heart function and maintains cardiac Ca2+ homeostasis and that accumulation of Casq1 might be a causative factor for vacuolar cardiomyopathy.

Authors

Yingchao Shi, Wenli Fan, Mingjie Xu, Xinhua Lin, Wukui Zhao, Zhongzhou Yang

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Figure 2

Znhit1 cKO mice had rapid heart failure and arrhythmia.

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Znhit1 cKO mice had rapid heart failure and arrhythmia. (A) Representati...
(A) Representative Echo images. (B and C) Quantitative analysis of ejection fraction (EF) and fractional shortening (FS). Ctrl, P21 (n = 6); P25 (n = 6); P27 (n = 5). cKO, P21 (n = 7); P25 (n = 9); P27 (n = 4). (D) Quantitative analysis of left ventricular internal dimension at diastole (LVID; d). (E) Quantitative analysis of left ventricular volume at diastole (LV vol; d). Numbers of mice were as follows: control (Ctrl), on P21 (n = 6), P25 (n = 6), and P27 (n = 5); cKO: on P21 (n = 7), P25 (n = 9), and P27 (n = 4). (F–H) ECG: left panels, Ctrl; right panels, Znhit1 cKO. (I) Quantitative analysis of R amplitude. Numbers of mice were as follows: Ctrl, on P21 (n = 24), P25 (n = 23), and P27 (n = 15); and cKO: on P21 (n = 20), P25 (n = 16), and P27 (n = 15). (J and K) Quantitative analysis of the RR interval and heart rate in Ctrl and Znhit1 cKO mice. Numbers of mice were as follows: Ctrl, on P21 (n = 21), P25 (n = 28), and P27 (n = 18); and cKO: on P21 (n = 18), P25 (n = 14), and P27 (n = 15). Ctrl mice were Znhit1fl/fl or Znhit1fl/+ littermates. Data are presented as mean ± SD. *P < 0.05, **P < 0.01, and ***P < 0.001 by unpaired 2-tailed Student’s t test.