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Functional BSND variants in essential hypertension.

Functional BSND variants in essential hypertension. Research Abstract Details 

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  • Functional BSND variants in essential hypertension. Abstract Text:

    saba sileSaba Sile,niloufar b gillaniNiloufar B Gillani,digna r velezDigna R Velez,carlos g vanoyeCarlos G Vanoye,chang yuChang Yu,loretta m byrneLoretta M Byrne,james v gainerJames V Gainer,nancy j brownNancy J Brown,scott m williamsScott M Williams,alfred l georgeAlfred L George,saba sileSaba Sile,niloufar b gillaniNiloufar B Gillani,digna r velezDigna R Velez,carlos g vanoyeCarlos G Vanoye,chang yuChang Yu,loretta m byrneLoretta M Byrne,james v gainerJames V Gainer,nancy j brownNancy J Brown,scott m williamsScott M Williams,alfred l georgeAlfred L George,

    BACKGROUND: Defects in the handling of renal salt reabsorption may contribute to interindividual differences in blood-pressure regulation and susceptibility to hypertension. Sodium chloride reabsorption in the thick ascending limb (TAL) is dependent in part on the chloride channel, ClC-Kb (encoded by CLCNKB), and its accessory subunit, barttin (encoded by BSND). METHODS: We investigated genetic variations in BSND in a screening population, and genotyped a homogenous cohort of normotensive and hypertensive Ghanaian subjects, in addition to four ethnically defined control populations. Functional consequences of the identified BSND variants were examined using a heterologous expression system. RESULTS: Three novel, nonsynonymous coding-sequence single-nucleotide polymorphisms were identified (V43I, E255Q, and G284D) in the screening population. BSND-V43I was identified in African American, Asian, and Hispanic subjects, with minor allele frequencies of 0.14, 0.18, and 0.01, respectively, but it was absent in the Caucasian population. BSND-E225Q and BSND-G284D were rare variants. Two of these variants (V43I and G284D) exhibited partial loss-of-function phenotypes when heterologously expressed with ClC-Kb chloride channels in cultured cells. In logistic regression analyses, we observed no association between hypertension and BSND-I43 in our study population. However, we did observe significant deviation from Hardy-Weinberg equilibrium in the normotensive population. CONCLUSIONS: We conclude that BSND-V43I, a common variant conferring partial loss of function, exhibits significant deviation from Hardy-Weinberg equilibrium in the Ghanaian normotensive control population. However, it does not independently confer protection against hypertension.

    Functional BSND variants in essential hypertension. Publishing Authors By Initials

    s sileS Sile,nb gillaniNB Gillani,dr velezDR Velez,cg vanoyeCG Vanoye,c yuC Yu,lm byrneLM Byrne,jv gainerJV Gainer,nj brownNJ Brown,sm williamsSM Williams,al georgeAL George,s sileS Sile,nb gillaniNB Gillani,dr velezDR Velez,cg vanoyeCG Vanoye,c yuC Yu,lm byrneLM Byrne,jv gainerJV Gainer,nj brownNJ Brown,sm williamsSM Williams,al georgeAL George,

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    PUBMED ID PMID:

    MEDLINE DATE:

    Functional BSND variants in essential hypertension. Journal Published:

    PUBLICATION TYPE: Research Support, Non-U.S. Gov

    Journal: American journal of hypertension : journal of the

    VOLUME: 20

    Page Numbers: 1176-1182

    Journal Abbreviation: Am. J. Hypertens.

    ISSN: 0895-7061

    DAY: 23

    MONTH: Nov

    YEAR: 2007

    Functional BSND variants in essential hypertension. Information

    Number of References:

    LANGUAGE: eng

    NlmUniqueID: 8803676

    Functional BSND variants in essential hypertension. Keywords Mesh Terms:

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    Grant and Affiliation Information for Functional BSND variants in essential hypertension.

    AFFILIATION: Department of Medicine, Vanderbilt University, Nashville, Tennessee 37232-0275, USA. saba.sile@vanderbilt.edu

    Country: United States

    United States Research PublicationUnited States Research Publication

    AGENCY: United States NIDDK

    GRANT: DK071742

    ACRONYM: DK

    MEDLINETA: Am J Hypertens

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