Association of lipoprotein lipase gene polymorphisms with coronary artery disease among Filipinos

Studies have shown association of lipoprotein lipase (LPL) polymorphisms with coronary artery disease (CAD); however, limited studies on the genetics of CAD have been done in the Philippines. Because of their effects on high-density lipoprotein and triglyceride metabolism, the G-allele of the Ser447...

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Veröffentlicht in:International journal of molecular epidemiology and genetics 2019-01, Vol.10 (5), p.77-84
Hauptverfasser: Gerodias, Ferdinand R, Posas, Fabio Enrique B, Baclig, Michael O, Repotente, Elmer Casley T, Pelat, Jonnah Fatima B, Rogelio, Gregorio G, San Jose, Maria Cristina Z, Mapua, Cynthia A, Daroy, Ma Luisa G
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container_title International journal of molecular epidemiology and genetics
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creator Gerodias, Ferdinand R
Posas, Fabio Enrique B
Baclig, Michael O
Repotente, Elmer Casley T
Pelat, Jonnah Fatima B
Rogelio, Gregorio G
San Jose, Maria Cristina Z
Mapua, Cynthia A
Daroy, Ma Luisa G
description Studies have shown association of lipoprotein lipase (LPL) polymorphisms with coronary artery disease (CAD); however, limited studies on the genetics of CAD have been done in the Philippines. Because of their effects on high-density lipoprotein and triglyceride metabolism, the G-allele of the Ser447X variant of LPL gene has been shown to be atheroprotective, while III polymorphism has been shown to be pro-atherogenic. We assessed 1301 patients undergoing coronary angiography to determine the prevalence of III and Ser447X polymorphisms and their association with angiographically significant CAD. Genotyping for III and Ser447X variants were analyzed by real-time PCR. Multivariate analyses were performed to determine the interaction between LPL polymorphisms and risk factors of CAD. CAD+ group (72%) was predominantly male (76%) with a mean age of 60.17 ± 11.01 with hypertension (89%), dyslipidemia (84%) and smoking (54%) as the most common risk factors. III carriage frequency among the CAD+ group was 20.3% with a genotypic distribution of 78.71% (T/T), 19.83% (T/G) and 1.46% (G/G). Ser447X carriage frequency among the CAD+ group was 8.0% with a genotypic distribution of 91.39% (C/C), 8.38% (C/G) and 0.23% (G/G). III and Ser447X polymorphisms were both not significantly associated with CAD. LPL polymorphic allele III was common, while Ser447X was rare. Present study did not show association of LPL polymorphisms with the development of CAD. However, among patients with dyslipidemia, presence of Ser447X allele is associated with an increased risk (OR 2.6; 95% CI 2.1-3.7; value < 0.001) of developing CAD than those without LPL polymorphisms.
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Because of their effects on high-density lipoprotein and triglyceride metabolism, the G-allele of the Ser447X variant of LPL gene has been shown to be atheroprotective, while III polymorphism has been shown to be pro-atherogenic. We assessed 1301 patients undergoing coronary angiography to determine the prevalence of III and Ser447X polymorphisms and their association with angiographically significant CAD. Genotyping for III and Ser447X variants were analyzed by real-time PCR. Multivariate analyses were performed to determine the interaction between LPL polymorphisms and risk factors of CAD. CAD+ group (72%) was predominantly male (76%) with a mean age of 60.17 ± 11.01 with hypertension (89%), dyslipidemia (84%) and smoking (54%) as the most common risk factors. III carriage frequency among the CAD+ group was 20.3% with a genotypic distribution of 78.71% (T/T), 19.83% (T/G) and 1.46% (G/G). Ser447X carriage frequency among the CAD+ group was 8.0% with a genotypic distribution of 91.39% (C/C), 8.38% (C/G) and 0.23% (G/G). III and Ser447X polymorphisms were both not significantly associated with CAD. LPL polymorphic allele III was common, while Ser447X was rare. Present study did not show association of LPL polymorphisms with the development of CAD. 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Because of their effects on high-density lipoprotein and triglyceride metabolism, the G-allele of the Ser447X variant of LPL gene has been shown to be atheroprotective, while III polymorphism has been shown to be pro-atherogenic. We assessed 1301 patients undergoing coronary angiography to determine the prevalence of III and Ser447X polymorphisms and their association with angiographically significant CAD. Genotyping for III and Ser447X variants were analyzed by real-time PCR. Multivariate analyses were performed to determine the interaction between LPL polymorphisms and risk factors of CAD. CAD+ group (72%) was predominantly male (76%) with a mean age of 60.17 ± 11.01 with hypertension (89%), dyslipidemia (84%) and smoking (54%) as the most common risk factors. III carriage frequency among the CAD+ group was 20.3% with a genotypic distribution of 78.71% (T/T), 19.83% (T/G) and 1.46% (G/G). Ser447X carriage frequency among the CAD+ group was 8.0% with a genotypic distribution of 91.39% (C/C), 8.38% (C/G) and 0.23% (G/G). III and Ser447X polymorphisms were both not significantly associated with CAD. LPL polymorphic allele III was common, while Ser447X was rare. Present study did not show association of LPL polymorphisms with the development of CAD. 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Because of their effects on high-density lipoprotein and triglyceride metabolism, the G-allele of the Ser447X variant of LPL gene has been shown to be atheroprotective, while III polymorphism has been shown to be pro-atherogenic. We assessed 1301 patients undergoing coronary angiography to determine the prevalence of III and Ser447X polymorphisms and their association with angiographically significant CAD. Genotyping for III and Ser447X variants were analyzed by real-time PCR. Multivariate analyses were performed to determine the interaction between LPL polymorphisms and risk factors of CAD. CAD+ group (72%) was predominantly male (76%) with a mean age of 60.17 ± 11.01 with hypertension (89%), dyslipidemia (84%) and smoking (54%) as the most common risk factors. III carriage frequency among the CAD+ group was 20.3% with a genotypic distribution of 78.71% (T/T), 19.83% (T/G) and 1.46% (G/G). Ser447X carriage frequency among the CAD+ group was 8.0% with a genotypic distribution of 91.39% (C/C), 8.38% (C/G) and 0.23% (G/G). III and Ser447X polymorphisms were both not significantly associated with CAD. LPL polymorphic allele III was common, while Ser447X was rare. Present study did not show association of LPL polymorphisms with the development of CAD. However, among patients with dyslipidemia, presence of Ser447X allele is associated with an increased risk (OR 2.6; 95% CI 2.1-3.7; value &lt; 0.001) of developing CAD than those without LPL polymorphisms.</abstract><cop>United States</cop><pub>e-Century Publishing Corporation</pub><pmid>31988698</pmid><tpages>8</tpages></addata></record>
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title Association of lipoprotein lipase gene polymorphisms with coronary artery disease among Filipinos
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