Agrawal S, Tripathi Gaurav, Prajnya R, Sinha Nakul, Gilmour A, Bush L, Mastana S
Department of Medical Genetics, Sanjay Gandhi Postgraduate Institute of Medical Sciences, Lucknow, India.
Indian J Med Sci. 2009 Aug;63(8):335-44.
Polymorphisms in paraoxonase 1 (PON1) coding for PON1 enzyme have been studied as genetic markers of coronary artery disease (CAD). PON1 Q192R and PON1 L55M polymorphisms have been analyzed extensively, but data on association and role of these polymorphisms in the etiology of CAD are conflicting. In this study, we tested the genetic association between PON1 Q192R and PON1 L55M polymorphisms and CAD among north Indians.
Two hundred eighty-five angiographically proven patients with coronary artery disease and 200 sex-matched and ethnically matched controls were genotyped for 2 PON1 polymorphisms by the polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) technique. Genotype/ allele frequencies were compared in patients and controls using the chi-square test.
At PON1-192 locus, there were significant differences between patients and controls (P< 0.05), leading to significant odds ratios for RR genotype (OR= 1.92, CI: 1.19-3.10) and *R allele (OR= 1.30, CI: 1.00-1.70). These odds ratios were higher in the sub-sample of smokers (2.84 and 1.45, respectively). Binary logistic regression analysis also confirmed that *R allele carriers (QR and RR) have a higher risk of CAD (OR= 3.54, CI: 1.67-5.53). PON1-55 locus did not show significant differences between patients and controls, but LL genotype and *L allele were significant risk factors in the nonsmoker group. RL haplotype was also significantly associated with CAD risk (OR= 1.44, CI: 1.08-1.93).
PON1-192R allele and RR genotype are significantly associated with CAD patients from the north Indian population (Uttar Pradesh). This association was stronger in smokers, supporting the conclusion that an interaction between PON1 activity and smoking augments CAD risk. Further studies with larger sample size are warranted to confirm these associations in different Indian populations.
对编码对氧磷酶1(PON1)的对氧磷酶1基因多态性作为冠状动脉疾病(CAD)的遗传标记进行了研究。PON1 Q192R和PON1 L55M多态性已得到广泛分析,但这些多态性在CAD病因学中的关联及作用的数据存在冲突。在本研究中,我们检测了北印度人群中PON1 Q192R和PON1 L55M多态性与CAD之间的遗传关联。
采用聚合酶链反应-限制性片段长度多态性(PCR-RFLP)技术对285例经血管造影证实的冠状动脉疾病患者和200例性别及种族匹配的对照进行了2种PON1多态性的基因分型。采用卡方检验比较患者和对照的基因型/等位基因频率。
在PON1-192位点,患者与对照之间存在显著差异(P<0.05),导致RR基因型(OR=1.92,CI:1.19-3.10)和R等位基因(OR=1.30,CI:1.00-1.70)的优势比显著。在吸烟者亚组中,这些优势比更高(分别为2.84和1.45)。二元逻辑回归分析也证实R等位基因携带者(QR和RR)患CAD的风险更高(OR=3.54,CI:1.67-5.53)。PON1-55位点在患者与对照之间未显示出显著差异,但LL基因型和*L等位基因在非吸烟者组中是显著的危险因素。RL单倍型也与CAD风险显著相关(OR=1.44,CI:1.08-1.93)。
PON1-192R等位基因和RR基因型与来自北印度人群(北方邦)的CAD患者显著相关。这种关联在吸烟者中更强,支持了PON1活性与吸烟之间的相互作用增加CAD风险的结论。需要进行更大样本量的进一步研究以在不同印度人群中证实这些关联。
