Genome Wide Association Study Identifies the HMGCS2 Locus to be Associated With Chlorthalidone Induced Glucose Increase in Hypertensive Patients

Sonal Singh; Caitrin W McDonough; Yan Gong; Wael A Alghamdi; Meghan J Arwood; Salma A Bargal; Leanne Dumeny; Wen-Yi Li; Mai Mehanna; Bradley Stockard; Guang Yang; Felipe A de Oliveira; Natalie C Fredette; Mohamed H Shahin; Kent R Bailey; Amber L Beitelshees; Eric Boerwinkle; Arlene B Chapman; John G Gums; Stephen T Turner; Rhonda M Cooper-DeHoff; Julie A Johnson

doi:10.1161/JAHA.117.007339

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Genome Wide Association Study Identifies the HMGCS2 Locus to be Associated With Chlorthalidone Induced Glucose Increase in Hypertensive Patients

Journal article

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Peer reviewed

Genome Wide Association Study Identifies the HMGCS2 Locus to be Associated With Chlorthalidone Induced Glucose Increase in Hypertensive Patients

Sonal Singh, Caitrin W McDonough, Yan Gong, Wael A Alghamdi, Meghan J Arwood, Salma A Bargal, Leanne Dumeny, Wen-Yi Li, Mai Mehanna, Bradley Stockard, …

Journal of the American Heart Association, Vol.7(6), p.n/a

20/03/2018

DOI: https://doi.org/10.1161/JAHA.117.007339

PMCID: PMC5907544

PMID: 29523524

Abstract

Adult

African Americans - genetics

Antihypertensive Agents - adverse effects

Biomarkers - blood

Blood Glucose - drug effects

Blood Glucose - metabolism

Blood Pressure - drug effects

Chlorthalidone - adverse effects

Essential Hypertension - drug therapy

Essential Hypertension - ethnology

Essential Hypertension - physiopathology

European Continental Ancestry Group - genetics

Female

Genome-Wide Association Study

Humans

Hydroxymethylglutaryl-CoA Synthase - genetics

Hyperglycemia - blood

Hyperglycemia - chemically induced

Hyperglycemia - ethnology

Hyperglycemia - genetics

Male

Middle Aged

Pharmacogenomic Variants

Phenotype

Polymorphism, Single Nucleotide

Randomized Controlled Trials as Topic

Risk Factors

Sodium Chloride Symporter Inhibitors - adverse effects

United States - epidemiology

Thiazide and thiazide-like diuretics are first-line medications for treating uncomplicated hypertension. However, their use has been associated with adverse metabolic events, including hyperglycemia and incident diabetes mellitus, with incompletely understood mechanisms. Our goal was to identify genomic variants associated with thiazide-like diuretic/chlorthalidone-induced glucose change. Genome-wide analysis of glucose change after treatment with chlorthalidone was performed by race among the white (n=175) and black (n=135) participants from the PEAR-2 (Pharmacogenomic Evaluation of Antihypertensive Responses-2). Single-nucleotide polymorphisms with <5×10 were further prioritized using in silico analysis based on their expression quantitative trait loci function. Among blacks, an intronic single-nucleotide polymorphism (rs9943291) in the was associated with increase in glucose levels following chlorthalidone treatment (ß=12.5; =4.17×10 ). G-allele carriers of had higher glucose levels (glucose change=+16.29 mg/dL) post chlorthalidone treatment compared with noncarriers of G allele (glucose change=+2.80 mg/dL). This association was successfully replicated in an independent replication cohort of hydrochlorothiazide-treated participants from the PEAR study (ß=5.54; =0.023). A meta-analysis of the 2 studies was performed by race in Meta-Analysis Helper, where this single-nucleotide polymorphism, rs9943291, was genome-wide significant with a meta-analysis value of 3.71×10 . , a part of the HMG-CoA synthase family, is important for ketogenesis and cholesterol synthesis pathways that are essential in glucose homeostasis. These results suggest that is a promising candidate gene involved in chlorthalidone and Hydrochlorothiazide (HCTZ)-induced glucose change. This may provide insights into the mechanisms involved in thiazide-induced hyperglycemia that may ultimately facilitate personalized approaches to antihypertensive selection for hypertension treatment. URL: http://www.clinicaltrials.gov. Unique identifiers: NCT00246519 and NCT01203852.

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Title: Genome Wide Association Study Identifies the HMGCS2 Locus to be Associated With Chlorthalidone Induced Glucose Increase in Hypertensive Patients
Creators - without role: Sonal Singh - University of Florida
Caitrin W McDonough - University of Florida
Yan Gong - University of Florida
Wael A Alghamdi - University of Florida
Meghan J Arwood - University of Florida
Salma A Bargal - University of Florida
Leanne Dumeny - University of Florida
Wen-Yi Li - Department of Pharmacotherapy and Translational Research and Center for Pharmacogenomics, University of Florida, Gainesville, FL
Mai Mehanna - University of Florida
Bradley Stockard - University of Florida
Guang Yang - University of Florida
Felipe A de Oliveira - Department of Pharmacotherapy and Translational Research and Center for Pharmacogenomics, University of Florida, Gainesville, FL
Natalie C Fredette - University of Florida
Mohamed H Shahin - Department of Pharmacotherapy and Translational Research and Center for Pharmacogenomics, University of Florida, Gainesville, FL
Kent R Bailey - Mayo Clinic
Amber L Beitelshees - University of Maryland, Baltimore
Eric Boerwinkle - The University of Texas Health Science Center at Houston
Arlene B Chapman - University of Chicago
John G Gums - University of Florida
Stephen T Turner - Mayo Clinic
Rhonda M Cooper-DeHoff - University of Florida
Julie A Johnson - University of Florida
Publication Details: Journal of the American Heart Association, Vol.7(6), p.n/a
Grant note: UL1 TR001427 / NCATS NIH HHS UL1 TR000454 / NCATS NIH HHS UL1 TR000064 / NCATS NIH HHS UL1 TR000135 / NCATS NIH HHS UL1 TR002378 / NCATS NIH HHS U01 GM074492 / NIGMS NIH HHS
Identifiers: 9923851708331
Academic Unit: King Khalid University
Language: English
Resource Type: Journal article