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Literature DB >> 24956219

Deletion of FoxO1 leads to shortening of QRS by increasing Na(+) channel activity through enhanced expression of both cardiac NaV1.5 and β3 subunit.

Benzhi Cai¹, Ning Wang², Weike Mao¹, Tao You¹, Yan Lu³, Xiang Li¹, Bo Ye¹, Faqian Li¹, Haodong Xu⁴.

Abstract

Our in vitro studies revealed that a transcription factor, Forkhead box protein O1 (FoxO1), negatively regulates the expression of NaV1.5, a main α subunit of the cardiac Na(+) channel, by altering the promoter activity of SCN5a in HL-1 cardiomyocytes. The in vivo role of FoxO1 in the regulation of cardiac NaV1.5 expression remains unknown. The present study aimed to define the role of FoxO1 in the regulation of NaV1.5 expression and cardiac Na(+) channel activity in mouse ventricular cardiomyocytes and assess the cardiac electrophysiological phenotype of mice with cardiac FoxO1 deletion. Tamoxifen-induced and cardiac-specific FoxO1 deletion was confirmed by polymerase chain reaction (PCR). Cardiac FoxO1 deletion failed to result in either cardiac functional changes or hypertrophy as assessed by echocardiography and individual ventricular cell capacitances, respectively. Western blotting showed that FoxO1 was significantly decreased while NaV1.5 protein level was significantly increased in mouse hearts with FoxO1 deletion. Reverse transcription-PCR (RT-PCR) revealed that FoxO1 deletion led to an increase in NaV1.5 and Na(+) channel subunit β3 mRNA, but not β1, 2, and 4, or connexin 43. Whole patch-clamp recordings demonstrated that cardiac Na(+) currents were significantly augmented by FoxO1 deletion without affecting the steady-state activation and inactivation, leading to accelerated depolarization of action potentials in mouse ventricular cardiomyocytes. Electrocardiogram recordings showed that the QRS complex was significantly shortened and the P wave amplitude was significantly increased in conscious and unrestrained mice with cardiac FoxO1 deletion. NaV1.5 expression was decreased in the peri-infarct (border-zone) of mice with myocardial infarction and FoxO1 accumulated in the cardiomyocyte nuclei of chronic ischemic human hearts. Our findings indicate that FoxO1 plays an important role in the regulation of NaV1.5 and β3 subunit expressions as well as Na(+) channel activity in the heart and that FoxO1 is involved in the modulation of NaV1.5 expression in ischemic heart disease.

Entities: CellLine Chemical Disease Gene Mutation Species

Keywords: Cardiac depolarization; FoxO1; Na(+) channel; Na(V)1.5; β3 subunit

Mesh：

Substances：

Year: 2014 PMID： 24956219 PMCID： PMC4158923 DOI： 10.1016/j.yjmcc.2014.06.006

Source DB: PubMed Journal: J Mol Cell Cardiol ISSN： 0022-2828 Impact factor: 5.000

46 in total

1. The sodium channel beta-subunit SCN3b modulates the kinetics of SCN5a and is expressed heterogeneously in sheep heart.

Authors: A I Fahmi; M Patel; E B Stevens; A L Fowden; J E John; K Lee; R Pinnock; K Morgan; A P Jackson; J I Vandenberg
Journal: J Physiol Date: 2001-12-15 Impact factor: 5.182

2. Uncoupling of acetylation from phosphorylation regulates FoxO1 function independent of its subcellular localization.

Authors: Li Qiang; Alexander S Banks; Domenico Accili
Journal: J Biol Chem Date: 2010-06-02 Impact factor: 5.157

3. Mutation in glycerol-3-phosphate dehydrogenase 1 like gene (GPD1-L) decreases cardiac Na+ current and causes inherited arrhythmias.

Authors: Barry London; Michael Michalec; Haider Mehdi; Xiaodong Zhu; Laurie Kerchner; Shamarendra Sanyal; Prakash C Viswanathan; Arnold E Pfahnl; Lijuan L Shang; Mohan Madhusudanan; Catherine J Baty; Stephen Lagana; Ryan Aleong; Rebecca Gutmann; Michael J Ackerman; Dennis M McNamara; Raul Weiss; Samuel C Dudley
Journal: Circulation Date: 2007-10-29 Impact factor: 29.690

Review 4. Frequency of sudden cardiac death and profiles of risk.

Authors: R J Myerburg; A Interian; R M Mitrani; K M Kessler; A Castellanos
Journal: Am J Cardiol Date: 1997-09-11 Impact factor: 2.778

5. Cardiac-specific overexpression of SCN5A gene leads to shorter P wave duration and PR interval in transgenic mice.

Authors: Teng Zhang; Sandro L Yong; Xiao-Li Tian; Qing K Wang
Journal: Biochem Biophys Res Commun Date: 2007-02-07 Impact factor: 3.575

6. Variable Na(v)1.5 protein expression from the wild-type allele correlates with the penetrance of cardiac conduction disease in the Scn5a(+/-) mouse model.

Authors: Anne-Laure Leoni; Bruno Gavillet; Jean-Sébastien Rougier; Céline Marionneau; Vincent Probst; Solena Le Scouarnec; Jean-Jacques Schott; Sophie Demolombe; Patrick Bruneval; Christopher L H Huang; William H Colledge; Andrew A Grace; Hervé Le Marec; Arthur A Wilde; Peter J Mohler; Denis Escande; Hugues Abriel; Flavien Charpentier
Journal: PLoS One Date: 2010-02-19 Impact factor: 3.240

Review 7. FoxO1 is crucial for sustaining cardiomyocyte metabolism and cell survival.

Authors: Prasanth Puthanveetil; Andrea Wan; Brian Rodrigues
Journal: Cardiovasc Res Date: 2012-12-21 Impact factor: 10.787

8. Hydrogen peroxide changes in ischemic and reperfused heart. Cytochemistry and biochemical and X-ray microanalysis.

Authors: J Slezak; N Tribulova; J Pristacova; B Uhrik; T Thomas; N Khaper; N Kaul; P K Singal
Journal: Am J Pathol Date: 1995-09 Impact factor: 4.307

9. Reactive oxygen species suppress cardiac NaV1.5 expression through Foxo1.

Authors: Weike Mao; Tao You; Bo Ye; Xiang Li; Henry H Dong; Joseph A Hill; Faqian Li; Haodong Xu
Journal: PLoS One Date: 2012-02-29 Impact factor: 3.240

10. Nav1.5 E1053K mutation causing Brugada syndrome blocks binding to ankyrin-G and expression of Nav1.5 on the surface of cardiomyocytes.

Authors: Peter J Mohler; Ilaria Rivolta; Carlo Napolitano; Guy LeMaillet; Stephen Lambert; Silvia G Priori; Vann Bennett
Journal: Proc Natl Acad Sci U S A Date: 2004-12-03 Impact factor: 11.205

14 in total

Review 1. Can heart function lost to disease be regenerated by therapeutic targeting of cardiac scar tissue?

Authors: Emily L Ongstad; Robert G Gourdie
Journal: Semin Cell Dev Biol Date: 2016-05-24 Impact factor: 7.727

2. Enhancement of β-catenin/T-cell factor 4 signaling causes susceptibility to cardiac arrhythmia by suppressing Na_V1.5 expression in mice.

Authors: Rong Huo; Chaowei Hu; Limei Zhao; Lihua Sun; Ning Wang; Yan Lu; Bo Ye; Arjun Deb; Faqian Li; Haodong Xu
Journal: Heart Rhythm Date: 2019-05-22 Impact factor: 6.343

Deletion of FoxO1 leads to shortening of QRS by increasing Na(+) channel activity through enhanced expression of both cardiac NaV1.5 and β3 subunit.

1. The sodium channel beta-subunit SCN3b modulates the kinetics of SCN5a and is expressed heterogeneously in sheep heart.

2. Uncoupling of acetylation from phosphorylation regulates FoxO1 function independent of its subcellular localization.

3. Mutation in glycerol-3-phosphate dehydrogenase 1 like gene (GPD1-L) decreases cardiac Na+ current and causes inherited arrhythmias.

Review 4. Frequency of sudden cardiac death and profiles of risk.

5. Cardiac-specific overexpression of SCN5A gene leads to shorter P wave duration and PR interval in transgenic mice.

6. Variable Na(v)1.5 protein expression from the wild-type allele correlates with the penetrance of cardiac conduction disease in the Scn5a(+/-) mouse model.

Review 7. FoxO1 is crucial for sustaining cardiomyocyte metabolism and cell survival.

8. Hydrogen peroxide changes in ischemic and reperfused heart. Cytochemistry and biochemical and X-ray microanalysis.

9. Reactive oxygen species suppress cardiac NaV1.5 expression through Foxo1.

10. Nav1.5 E1053K mutation causing Brugada syndrome blocks binding to ankyrin-G and expression of Nav1.5 on the surface of cardiomyocytes.

Review 1. Can heart function lost to disease be regenerated by therapeutic targeting of cardiac scar tissue?

2. Enhancement of β-catenin/T-cell factor 4 signaling causes susceptibility to cardiac arrhythmia by suppressing Na_V1.5 expression in mice.

3. A small-molecule LF3 abrogates β-catenin/TCF4-mediated suppression of Na_V1.5 expression in HL-1 cardiomyocytes.

4. Elevated MCU Expression by CaMKIIδB Limits Pathological Cardiac Remodeling.

5. Activation of Wnt/β-catenin signaling by hydrogen peroxide transcriptionally inhibits NaV1.5 expression.

Review 6. The cardiac sodium channel gene SCN5A and its gene product NaV1.5: Role in physiology and pathophysiology.

7. Elevated EZH2 in ischemic heart disease epigenetically mediates suppression of Na_V1.5 expression.

8. Cardiomyocyte Deletion of Bmal1 Exacerbates QT- and RR-Interval Prolongation in Scn5a ^+/ΔKPQ Mice.

9. Cardiac Nav 1.5 is modulated by ubiquitin protein ligase E3 component n-recognin UBR3 and 6.

Review 10. Forkhead box transcription factor 1: role in the pathogenesis of diabetic cardiomyopathy.