Abstract

Arrhythmias remain a major cause of morbidity and mortality. Brugada syndrome is a rare, autosomal dominant, male predominant form of idiopathic ventricular fibrillation characterized by a right bundle branch block pattern and ST elevation in the right precordial leads of the surface EKG. The only effective therapy is an implantable cardioverter-defibrillator. Mutations of the cardiac Na+ channel SCN5A cause ~20% of cases of Brugada syndrome by decreasing inward Na+ current, and Na+ channel blockers such as procainamide exacerbate the EKG findings. The genetic basis for most remaining Brugada syndrome patients is unknown. During the initial periods of this project, we identified a large family with Brugada syndrome characterized by progressive conduction disease, age- and sex-dependent penetrance, and minimal response to the Na+ channel blocker procainamide. Linkage was identified to a ~1 cM region on chromosome 3p24 (max LOD score > 4.0) and SCN5A was excluded (LOD score < -2). Direct sequencing of candidates in the region identified an alanine to valine substitution in a conserved amino acid (A280V) in exon 6 of the glycerol-3- phosphate dehydrogenase 1-like gene (GPD1-L, KIAA0089). The mutation was present in all affected individuals and was absent in >200 unaffected controls of mixed racial background. Northern and Western blot analysis confirmed expression in the heart. Whole cell patch clamp studies of a stably transfected HEK cell line expressing SCN5A showed an ~60% reduction in peak Na current in cells transfected with the A280V mutant compared to the wild type GPD1-L (p=0.01). Confocal microscopy showed expression of the wild type but not the mutant GPD1-L protein on the plasma membrane, along with reduced SCN5A in the membrane of cells expressing the A280V mutant. NADH is increased in cells expressing A280V GPD1-L, and QRS duration on the surface EKG is prolonged in transgenic mice overexpressing A280V GPD1-L. In this competing renewal, we will test the hypothesis that GPD1-L is a novel ion channel modulator and that mutations of GPD1-L decrease Na+ current by altering intracellular NAD+/NADH levels. We will 1) define the mechanisms by which mutant GPD1-L alters ion channel trafficking and current in-vitro using cell lines and neonatal rat ventricular myocytes; 2) identify downstream mechanisms by which GPD1-L affects ion channel trafficking, and 3) study transgenic and gene-targeted mouse models to confirm its physiological role. Over 250,000 people in the United States die suddenly each year. Most sudden death occurs during heart attacks or in patients with weak hearts from prior damage, but we have no good ways to predict who is at highest risk of deaths and no drug therapies to prevent sudden death. In this proposal, we will study a family with an inherited genetic form of sudden death with the hope that we can develop new treatments for the more common causes of this devastating and unpredictable condition. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
2R01HL062300-07A1
Application #
7384876
Study Section
Electrical Signaling, Ion Transport, and Arrhythmias Study Section (ESTA)
Program Officer
Wang, Lan-Hsiang
Project Start
1999-04-01
Project End
2011-12-31
Budget Start
2008-01-15
Budget End
2008-12-31
Support Year
7
Fiscal Year
2008
Total Cost
$337,501
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
004514360
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Refaat, Marwan M; Tanaka, Toshikazu; Kormos, Robert L et al. (2012) Survival benefit of implantable cardioverter-defibrillators in left ventricular assist device-supported heart failure patients. J Card Fail 18:140-5
Frangiskakis, J Michael; London, Barry (2010) Targeting device therapy: genomics of sudden death. Heart Fail Clin 6:93-100
Shusterman, Vladimir; McTiernan, Charles F; Goldberg, Anna et al. (2010) Adrenergic stimulation promotes T-wave alternans and arrhythmia inducibility in a TNF-alpha genetic mouse model of congestive heart failure. Am J Physiol Heart Circ Physiol 298:H440-50
Shusterman, Vladimir; Lampert, Rachel; London, Barry (2009) The many faces of repolarization instability: which one is prognostic? J Electrocardiol 42:511-6
Liu, Man; Sanyal, Shamarendra; Gao, Ge et al. (2009) Cardiac Na+ current regulation by pyridine nucleotides. Circ Res 105:737-45
Pfahnl, Arnold E; Viswanathan, Prakash C; Weiss, Raul et al. (2007) A sodium channel pore mutation causing Brugada syndrome. Heart Rhythm 4:46-53
London, Barry; Michalec, Michael; Mehdi, Haider et al. (2007) Mutation in glycerol-3-phosphate dehydrogenase 1 like gene (GPD1-L) decreases cardiac Na+ current and causes inherited arrhythmias. Circulation 116:2260-8
Bedi, Maninder; McNamara, Dennis; London, Barry et al. (2006) Genetic susceptibility to atrial fibrillation in patients with congestive heart failure. Heart Rhythm 3:808-12
London, Barry (2006) CaM kinase inhibition: apply directly to the heart? Circ Res 99:1027-8
McNamara, Dennis M; Holubkov, Richard; Postava, Lisa et al. (2004) Pharmacogenetic interactions between angiotensin-converting enzyme inhibitor therapy and the angiotensin-converting enzyme deletion polymorphism in patients with congestive heart failure. J Am Coll Cardiol 44:2019-26

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