WNK1 Kinase Polymorphism and Blood Pressure Response to a Thiazide Diuretic

doi:10.1161/01.HYP.0000186240.81996.57

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on September 19, 2005

Hypertension. 2005
Published online before print September 19, 2005, doi: 10.1161/01.HYP.0000186240.81996.57

A more recent version of this article appeared on October 1, 2005

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Submitted on March 25, 2005
Revised on April 18, 2005

WNK1 Kinase Polymorphism and Blood Pressure Response to a Thiazide Diuretic

Stephen T. Turner^*; Gary L. Schwartz; Arlene B. Chapman; and Eric Boerwinkle

From the Division of Nephrology and Hypertension, Department of Internal Medicine, Mayo Clinic and Foundation, Rochester, Minn (G.L.S., S.T.T.); Renal Division, Emory University, Atlanta, Ga (A.B.C.); and Institute of Molecular Medicine and Human Genetics Center, University of Texas Health Sciences Center, Houston (E.B.).

^* To whom correspondence should be addressed. E-mail: turner.stephen{at}mayo.edu.

Abstract--Single nucleotide polymorphisms (SNPs) in genes encodingor influencing renal sodium transport systems were investigatedas potential predictors of blood pressure (BP) response to athiazide diuretic. A sample of 585 adults with essential hypertension(30 to 59.9 years of age; 50% blacks; 47% women) were treatedwith hydrochlorothiazide for 4 weeks (25 mg daily, orally) todetermine office BP responses. Ambulatory BP responses weremeasured in a subset of 228 subjects. After adjustment for ethnicity,sex, age, and waist-to-hip ratio, 3 SNPs in WNK1 (rs2107614,rs2277869, and rs1159744), encoding a lysine-deficient proteinkinase that regulates thiazide-sensitive sodium-potassium cotransport,made statistically significant contributions to predicting ambulatoryBP responses, accounting for 2% to 4% of variation in systolicand diastolic responses (P<0.05). SNPs in the ${beta}$ ₂-adrenoceptor(rs2400707) and the epithelial sodium channel ${gamma}$ -subunit (rs5723and rs5729) were associated with similar magnitude of variationin ambulatory systolic BP response (P=0.028) or office diastolicBP response (P<0.05), respectively. However, SNPs evaluatedin the furosemide-sensitive sodium-potassium chloride cotransporter,potassium inwardly rectifying channel, chloride channel, thiazide-sensitivesodium chloride cotransporter, epithelial sodium channel ${beta}$ -subunit,and the mineralocorticoid receptor were not associated withsignificant variation in ambulatory or office BP responses.Polymorphisms in genes regulating renal sodium transport, inparticular WNK1, predict interindividual differences in antihypertensiveresponses to hydrochlorothiazide.

Key words: polymorphism • genetics • diuretics • blood pressure

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