Effects of the angiotensinogen gene M235T and A(-6)G variants on blood pressure and other vascular risk factors in a Spanish population

Rodríguez‐Pérez, José Carlos; Rodrı́guez-Esparragón, Francisco; Hernández‐Perera, Octavio; Fiuza-Pérez, M. Dolores; Anabitarte-Prieto, Aránzazu; Losada-Cabrera, A

doi:10.1038/sj.jhh.1001110

Cited by 21 publications

(14 citation statements)

References 34 publications

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“…Rodriguez-Perez et al 23 refer similar results to ours in allelic and/or genotype differences in two angiotensinogen polymorphisms between normotensives and hypertensives (even with similar numbers of study participants) but with no association with BMI and smoking. Cooper et al 24 did not found a similar association of ATG genotype (M235T) in obese hypertensive population when obesity is defined as BMI above 31 kg/m 2 .…”

Section: Journal Of Human Hypertensionsupporting

confidence: 75%

An association of BMI with A (-6) G, M235T and T174M polymorphisms in angiotensinogen gene in essential hypertension

et al. 2002

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The aim of the study was to assess the existence of possible associations among frequent polymorphisms in angiotensinogen genes and some of the risk factors for essential hypertension, especially body mass index (BMI) and smoking. A total of 192 control subjects (aged 45.87 ± 3.0 years) and 206 patients with the essential hypertension (aged 48.71 ± 8.42 years) were compared at three angiotensinogen gene polymorphisms by considering BMI and smoking status. No significant differences in genotype and/or allelic distribution for either A (-6) G ATG, M235T or T174M polymorphisms between the hypertensive and control groups were proved. Significantly more hypertensives than control persons with BMI above 25 kg/m 2 were observed (P corr = 0.009), independently on sex distribution. A percentage of 44.6% of smokers in the control group vs 46.0% of smokers in the hypertensive groups were found. No significant dif-

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Section: Journal Of Human Hypertensionsupporting

confidence: 75%

An association of BMI with A (-6) G, M235T and T174M polymorphisms in angiotensinogen gene in essential hypertension

et al. 2002

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“…Failure of previous genderstratified studies [13][14][15] to show an association may be due to small sample size and/or lack of stratification by gender. A(Ϫ20)C has previously been shown to modify an estrogenresponsive element located in the regulatory region of the show mean values for all women and men, respectively, in the general population.…”

Section: Blood Pressure As a Dichotomous Variablementioning

confidence: 99%

“…5 SNPs in the transcription factor binding region (Ϫ25 to Ϫ1) of the angiotensinogen gene promoter have been reported to affect gene expression. 6 -8 The Ϫ6A SNP has been associated with increased gene transcription, 8,9 elevated blood pressure, and increased risk of IHD in some 10 -12 but not in all studies, [13][14][15] whereas the Ϫ20C SNP has been associated with increased gene transcription, elevated angiotensinogen levels, and elevated blood pressure in one 7 but not in other studies. 1,10,15 These conflicting results may be due to small sample size in previous studies, which have included between 301 and 1232 participants.…”

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confidence: 99%

Angiotensinogen Single Nucleotide Polymorphisms, Elevated Blood Pressure, and Risk of Cardiovascular Disease

et al. 2003

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Abstract-In this study of 10 690 individuals, associations with elevated blood pressure, ischemic heart disease, and ischemic cerebrovascular disease were determined for two noncoding [A(Ϫ20)C, G(Ϫ6)A] and two coding (T174M, M235T) single nucleotide polymorphisms, analyzed alone and in combination (haplotypes). Participants from the general population with (nϭ4950) and without (nϭ4234) elevated blood pressure were compared (study 1), as were participants from the general population without ischemic heart disease and ischemic cerebrovascular disease (nϭ7965) and cases with either ischemic heart disease (nϭ1850, study 2) or ischemic cerebrovascular disease (nϭ848, study 3). Finally, 22-year follow-up of 9184 individuals from the general population examined risk of ischemic heart disease (study 4) and ischemic cerebrovascular disease (study 5). Individuals with Ϫ6AA, 174TT, or 235TT had plasma angiotensinogen levels increased by 80 ng/mL (Pϭ0.01 and 0.05 for women and men) compared with individuals with Ϫ6GG, 174TT, or 235 MM. In women, this difference was associated with an odds ratio of elevated blood pressure of 1.25 (1.03 to 1.51), which increased to 1.63 (1.05 to 2.51) in postmenopausal women receiving hormone replacement therapy. The promoter single nucleotide polymorphisms alone or as haplotypes did not predict the continuous variables of systolic, diastolic, or pulse pressure in cross section or the risk of ischemic heart disease or ischemic cerebrovascular disease in either gender in case-control or prospective studies. Individuals with Ϫ6AA, 174TT, or 235TT in the angiotensinogen gene have increased plasma angiotensinogen levels and moderately increased risk of elevated blood pressure (women only) but unaltered blood pressure examined as a continuous variable and unaltered risk of ischemic heart disease and ischemic cerebrovascular disease. Key Words: blood pressure Ⅲ hypertension, genetic Ⅲ cardiovascular diseases Ⅲ cerebrovascular disorders S ingle nucleotide polymorphisms (SNPs) in the angiotensinogen gene have been associated with elevated angiotensinogen levels, 1 elevated blood pressure, 1 ischemic heart disease (IHD), 2 and ischemic cerebrovascular disease (ICVD). 3 In the Copenhagen City Heart Study, 4 we have previously shown that the M235T SNP (T-allele) was associated with elevated plasma angiotensinogen levels in both genders and a 30% increased risk of elevated blood pressure in women homozygous for 235T. However, the risk of IHD and ICVD was not associated with variation in genotype. 5 SNPs in the transcription factor binding region (Ϫ25 to Ϫ1) of the angiotensinogen gene promoter have been reported to affect gene expression. 6 -8 The Ϫ6A SNP has been associated with increased gene transcription, 8,9 elevated blood pressure, and increased risk of IHD in some 10 -12 but not in all studies, [13][14][15] whereas the Ϫ20C SNP has been associated with increased gene transcription, elevated angiotensinogen levels, and elevated blood pressure in one 7 but not in other studies. 1,10,15 These ...

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“…For example, studies of variants in the angiotensinogen gene, one of the genes with the most consistent findings, still have a large number of both positive [7][8][9][10] and negative results [11][12][13][14]. This may be because the effects of the variants under study are small to undetectable in many genetic backgrounds/populations because they are effectively masked by effects of unstudied gene(s) that affect the phenotype [4,15].…”

Section: Introductionmentioning

confidence: 99%

Multilocus Analysis of Hypertension: A Hierarchical Approach

et al. 2004

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While hypertension is a complex disease with a well-documented genetic component, genetic studies often fail to replicate findings. One possibility for such inconsistency is that the underlying genetics of hypertension is not based on single genes of major effect, but on interactions among genes. To test this hypothesis, we studied both single locus and multilocus effects, using a case-control design of subjects from Ghana. Thirteen polymorphisms in eight candidate genes were studied. Each candidate gene has been shown to play a physiological role in blood pressure regulation and affects one of four pathways that modulate blood pressure: vasoconstriction (angiotensinogen, angiotensin converting enzyme – ACE, angiotensin II receptor), nitric oxide (NO) dependent and NO independent vasodilation pathways and sodium balance (G protein-coupled receptor kinase, GRK4). We evaluated single site allelic and genotypic associations, multilocus genotype equilibrium and multilocus genotype associations, using multifactor dimensionality reduction (MDR). For MDR, we performed systematic reanalysis of the data to address the role of various physiological pathways. We found no significant single site associations, but the hypertensive class deviated significantly from genotype equilibrium in more than 25% of all multilocus comparisons (2,162 of 8,178), whereas the normotensive class rarely did (11 of 8,178). The MDR analysis identified a two-locus model including ACE and GRK4 that successfully predicted blood pressure phenotype 70.5% of the time. Thus, our data indicate epistatic interactions play a major role in hypertension susceptibility. Our data also support a model where multiple pathways need to be affected in order to predispose to hypertension.

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Effects of the angiotensinogen gene M235T and A(-6)G variants on blood pressure and other vascular risk factors in a Spanish population

Cited by 21 publications

References 34 publications

An association of BMI with A (-6) G, M235T and T174M polymorphisms in angiotensinogen gene in essential hypertension

An association of BMI with A (-6) G, M235T and T174M polymorphisms in angiotensinogen gene in essential hypertension

Angiotensinogen Single Nucleotide Polymorphisms, Elevated Blood Pressure, and Risk of Cardiovascular Disease

Multilocus Analysis of Hypertension: A Hierarchical Approach

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