Literature DB >> 19996987

Blood pressure response to potassium supplementation is associated with genetic variation in endothelin 1 and interactions with E selectin in rural Chinese.

May E Montasser1, Lawrence C Shimmin, Donfeng Gu, Jing Chen, Charles Gu, Tanika N Kelly, Cashell E Jaquish, Treva Rice, D C Rao, Jie Cao, Jichun Chen, De-Pei Liu, Paul Whelton, Jiang He, James E Hixson.   

Abstract

OBJECTIVE: Although beneficial effects of potassium intake on blood pressure (BP) are well established, little is known about genetic factors that underlie interindividual variability in BP response to dietary potassium. In a previous study, we reported the first evidence for significant heritabilities for BP response in a dietary intervention study in rural Chinese. In this report, we extend our genetic studies to examine associations with polymorphisms in genes in vascular endothelial pathways.
METHODS: We genotyped study participants for 23 single nucleotide polymorphisms (SNPs) in endothelin 1 (EDN1), nitric oxide synthase 3, and E selectin (SELE). We tested 17 of these SNPs for associations with BP response to potassium supplementation in 1843 participants. Association tests used population-based [generalized estimation equation (GEE)] and family-based (quantitative transmission disequilibrium test) methods, as well as tests for gene-by-gene (GxG) interaction (generalized multifactor dimensionalilty reduction and GEE).
RESULTS: Single SNP analysis identified significant associations for several SNPs in EDN1 with multiple measures of BP response to potassium supplementation. The cumulative effects of the minor EDN1 alleles that showed significant associations were to reduce measures of BP response by 0.5-0.9 mmHg. We found significant evidence for effects of GxG interactions between EDN1 and SELE, even in the absence of individual associations with SELE variants.
CONCLUSION: Our results implicate variability in EDN1 and SELE as genetic factors that influence BP response to potassium intake. Although such epidemiological studies do not allow direct determination of physiologic mechanisms, our findings of joint effects identify EDN1 and SELE as targets for functional studies to determine their interactions in BP response to potassium intake.

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Year:  2010        PMID: 19996987      PMCID: PMC2919321          DOI: 10.1097/HJH.0b013e3283355672

Source DB:  PubMed          Journal:  J Hypertens        ISSN: 0263-6352            Impact factor:   4.844


  41 in total

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Authors:  F J He; G A MacGregor
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5.  Effect of potassium supplementation on blood pressure in Chinese: a randomized, placebo-controlled trial.

Authors:  D Gu; J He; X Wu; X Duan; P K Whelton
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9.  Relationship between E-selectin L/F554 polymorphism and blood pressure in the Stanislas cohort.

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  6 in total

1.  Genome-wide linkage and positional candidate gene study of blood pressure response to dietary potassium intervention: the genetic epidemiology network of salt sensitivity study.

Authors:  Tanika N Kelly; James E Hixson; Dabeeru C Rao; Hao Mei; Treva K Rice; Cashell E Jaquish; Lawrence C Shimmin; Karen Schwander; Chung-Shuian Chen; Depei Liu; Jichun Chen; Concetta Bormans; Pramila Shukla; Naveed Farhana; Colin Stuart; Paul K Whelton; Jiang He; Dongfeng Gu
Journal:  Circ Cardiovasc Genet       Date:  2010-09-22

Review 2.  Potassium and Its Discontents: New Insight, New Treatments.

Authors:  David H Ellison; Andrew S Terker; Gerardo Gamba
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3.  Dietary potassium: a key mediator of the cardiovascular response to dietary sodium chloride.

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Journal:  J Am Soc Hypertens       Date:  2013-06-02

4.  G-231A and G+70C Polymorphisms of Endothelin Receptor Type-A Gene could Affect the Psoriasis Area and Severity Index Score and Endothelin 1 Levels.

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Journal:  Indian J Dermatol       Date:  2015 Mar-Apr       Impact factor: 1.494

5.  Genetic variants in adiponectin and blood pressure responses to dietary sodium or potassium interventions: a family-based association study.

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Journal:  J Hum Hypertens       Date:  2016-03-24       Impact factor: 3.012

6.  Relationship between the A(8002)G intronic polymorphism of pre-pro-endothelin-1 gene and the endothelin-1 concentration among Tunisian coronary patients.

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  6 in total

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