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Merck
  • SAH gene variants are associated with obesity-related hypertension in Caucasians: the PEGASE Study.

SAH gene variants are associated with obesity-related hypertension in Caucasians: the PEGASE Study.

Journal of hypertension (2007-02-07)
Ralph Telgmann, Eva Brand, Viviane Nicaud, Claudia Hagedorn, Katrin Beining, Jacqueline Schönfelder, Verena Brink-Spalink, Klaus Schmidt-Petersen, Theodoros Matanis, Peter Vischer, Jerzy-Roch Nofer, Sandra Hasenkamp, Pierre-François Plouin, Ludovic Drouet, François Cambien, Martin Paul, Laurence Tiret, Stefan-Martin Brand-Herrmann
摘要

The SAH gene locus has recently been proposed to be involved in obesity-related hypertension in Japanese individuals. To replicate independently the initial findings in another ethnic group, we scanned the entire SAH gene in 190 Caucasian chromosomes. A total of 651 patients with essential hypertension and 776 controls (PEGASE Study) were genotyped for all identified variants using allele-specific oligonucleotides, and single nucleotide polymorphism as well as haplotype analyses were carried out. We also performed transient transfection experiments, northern and western blots, immunoprecipitation, and acyl-coenzyme A synthetase activity assays. We identified five polymorphisms in the promoter region (C-1808T, G-1606A, -962ins/del, G-451A, T-67C), two in introns 5 and 7 (T+9/In5C, A+20/In7T), and one missense variant (K359N). Carriage of the -1606A allele was significantly associated with hypertension [odds ratio (OR) 1.28, P = 0.049] as was 359N (OR 1.35, P = 0.048) compared with non-carriers. Conversely, for -962del, the OR for hypertension was 0.80 (P = 0.042). The SAH alleles -1606A and 359N, but not -962ins/del, displayed a raising effect on body mass index (BMI; P = 0.004 and P = 0.030, respectively) in hypertensive as well as in control individuals. After adjustment for BMI in hypertensive individuals, only the OR associated with -962ins/del remained significant (OR 0.77, P = 0.028). Functional analyses in BHK did not reveal differences for SAH 359N or 359K-containing constructs, formally excluding K359N as the functional variant. We confirm recent evidence that the SAH locus is associated with obesity-related hypertension, in which pathophysiological context SAH variants affecting blood pressure remain, however, to be shown.