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Abstract
Aim
The aim of this study was to investigate the association of the Pro12Ala polymorphism of the human peroxisome proliferator-activated receptor gamma 2 (PPARγ2) gene with hypertension and obesity in a highly consanguineous aboriginal Qatari population.
Design
A cross-sectional survey conducted from January 2011–December 2012.
Setting
Primary health care clinics.
Subjects
A random sample of 1,528 Qatari male and female population older than 20 years of age.
Materials and methods
Data on age, sex, income, level of education, occupation status, body mass index, and blood pressure and lipid profile were obtained. The Pro12Ala in the PPARγ2 gene was detected on the LightCycler® using two specific probes: (Sensor [G] 5′-CTC CTA TTG ACG CAG AAA GCG-FL and PPAR Anchor 5′ LC Red 640- TCC TTC ACT GAT ACA CTG TCT GCA AAC ATA TC-PH). Univariate and multivariate logistic regression were performed.
Result
Out of a total 1,528 participants, 220 were diagnosed with essential hypertension, and 420 were obese. Participants with consanguinity were significantly higher among hypertensive than normotensive (41.9% versus 30.8%; P=0.001). Altogether, more than three-fourths (89%) of the participants had a wild genotype (Pro12Pro), 9.8% were heterozygous with Pro12Ala, and only 1.2% was homozygous with the Ala12Ala genotype. The frequency of the Pro allele was 94.5% in normotensive versus 90.5% in hypertensive, while the distribution of the Ala allele was 5.5% in normotensive versus 9.5% in the hypertensive group (P=0.001). The odds of hypertension were 1.7 times higher among the participants with the Ala allele as compared to those with the Pro, while adjusting for other potential confounders (adjusted odds ratio 1.69; 95% confidence interval 1.12–2.55; P=0.012). There was no association between the PPARγ2Ala allele and obesity (P=0.740).
Conclusion
The current study revealed an association between the PPARγ2Ala allele and hypertension in Qatar’s population. On the other hand, this study found no association between the Ala allele and obesity.
Acknowledgments
The project was supported and funded by the support of the Qatar Diabetic Association and the Qatar Foundation. We also would like to thank the Hamad Medical Corporation for its approval of this study (Hamad Medical Center Research Protocol #10262-1027A/2011).
Author Contributions
Authors AB and SD organized the study, collected the data and revised the manuscript. Also, AB guided statistical analysis and wrote the first draft of the manuscript. MTY analyzed the data, interpreted results, and critically revised the first draft of manuscript. AOAAAH and RMM contributed to the interpretation of data and writing the manuscript.
Disclosure
The authors report no conflicts of interest in this work.