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Lipoprotein lipase variants associated with an endophenotype of hypertension: hypertension combined with elevated triglycerides

✍ Scribed by Pei Chen; Yuh-Shan Jou; Cathy SJ Fann; Jaw-Wen Chen; Chia-Min Chung; Chin-Yu Lin; Sheng-Yeu Wu; Mei-Jyh Kang; Ying-Chuang Chen; Yuh-Shiun Jong; Huey-Ming Lo; Chih-Sen Kang; Chien-Chung Chen; Huan-Cheng Chang; Nai-Kuei Huang; Yi-Lin Wu; Wen-Harn Pan


Book ID
102262864
Publisher
John Wiley and Sons
Year
2009
Tongue
English
Weight
269 KB
Volume
30
Category
Article
ISSN
1059-7794

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✦ Synopsis


Previously, we observed that young-onset hypertension was independently associated with elevated plasma triglyceride(s) (TG) levels to a greater extent than other metabolic risk factors. Thus, focusing on the endophenotype-hypertension combined with elevated TG-we designed a family-based haplotype association study to explore its genetic connection with novel genetic variants of lipoprotein lipase gene (LPL), which encodes a major lipid metabolizing enzyme. Young-onset hypertension probands and their families were recruited, numbering 1,002 individuals from 345 families. Singlenucleotide polymorphism discovery for LPL, linkage disequilibrium (LD) analysis, transmission disequilibrium tests (TDT), bin construction, haplotype TDT association and logistic regression analysis were performed. We found that the CC-haplotype (i) spanning from intron 2 to intron 4 and the ACATT haplotype (ii) spanning from intron 5 to intron 6 were significantly associated with hypertension-related phenotypes: hypertension (ii, P 5 0.05), elevated TG (i, P 5 0.01), and hypertension combined with elevated TG (i, P 5 0.001; ii, Po0.0001), according to TDT. The risk of this hypertension subtype increased with the number of risk haplotypes in the two loci, using logistic regression model after adjusting within-family correlation. The relationships between LPL variants and hypertension-related disorders were also confirmed by an independent association study. Finally, we showed a trend that individuals with homozygous risk haplotypes had decreased LPL expression after a fatty meal, as opposed to those with protective haplotypes. In conclusion, this study strongly suggests that two LPL intronic variants may be associated with development of the hypertension endophenotype with elevated TG.


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