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Literature DB >> 19496216

AKAP10 (I646V) functional polymorphism predicts heart rate and heart rate variability in apparently healthy, middle-aged European-Americans.

Serina A Neumann¹, Whittemore G Tingley, Bruce R Conklin, Catherine J Shrader, Eloise Peet, Matthew F Muldoon, J Richard Jennings, Robert E Ferrell, Stephen B Manuck.

Abstract

Previous evidence suggests that the dual-specific A kinase-anchoring protein 2 functional polymorphism (AKAP10 (A/G) I646V) influences heart rate (HR) and heart rate variability (HRV) in mice and humans (N=122) with cardiovascular disease. Here, we asked whether this AKAP10 variant predicts HR and HRV in a large sample of healthy humans. Resting HR and short-term time and frequency domain measures of HRV (5 min during paced and unpaced respiration conditions) were assessed in a U.S. community sample (N=1,033) of generally healthy men and women (age 30-54) of European ancestry. Each person was genotyped for the AKAP10 variant. As with previous work, the AKAP10 Val allele predicted greater resting HR (Paced p<.01; Unpaced p<.03) and diminished HRV (Paced ps <.05) suggesting that this variant may modulate the sensitivity of cardiac pacemaker cells to autonomic inputs, possibly conferring risk for arrhythmias and sudden cardiac death.

Entities: Chemical Disease Gene Mutation Species

Mesh：

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Year: 2009 PMID： 19496216 PMCID： PMC2890278 DOI： 10.1111/j.1469-8986.2009.00802.x

Source DB: PubMed Journal: Psychophysiology ISSN： 0048-5772 Impact factor: 4.016

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