原发性高血压相关新基因的发现--D1S249位点与汉族EH相关联

原发性高血压(essential hypertension, EH)被认为是多基因、多因素相互作用引起的复杂疾病. 过去10年中, 高血压相关基因研究虽然已取得令人高兴的进展, 但究竟有多少基因参与发病, 及其之间的相互作用仍不清楚. 以北京房山区高血压群体及家系为研究对象, 应用全基因组扫描技术, 通过病例-对照相关研究和98对受累同胞对连锁分析, 筛查鉴定与汉族原发性高血压相关联的新基因位点. 病例-对照群体分析结果表明, 位于1号染色体长臂1q32区的D1S249微卫星多态性位点与汉族原发性高血压相关联,χ2 = 14.6, P = 0.002. 该位点存在12种等位基因, A9等位基因(181 bp)频率在高血压组较对照组明显升高, 两组间频率为13.6% v.s 2.7%, χ2 = 6.30, P = 0.01(OR = 4.57, 95% CI = 1.21～25.4); 98对受累同胞对等位基因共享连锁分析显示, χ2 = 3.78, P = 0.048. 上述结果提示, D1S249微卫星多态位点与北京房山区汉族原发性高血压遗传易感相关联, 致病基因可能于D1S249位点存在连锁不平衡.     

Evidence for association of D1S249 locus on human chromosome 1 with the susceptibility to essential hypertension in Han Chinese

Essential hypertension (EH) is thought to result from the interaction of environmental and genetic factors. The molecular genetics of EH has witnessed considerable progress during the past few years. However, the number of genes involved, their chromosomal location and the magnitude of their effect on EH susceptibility are unknown. We conducted the present study to screen susceptibility genes to essential hypertension using a genome-wide scanning method in a group of Han people from Fangshan district located in the southwest of Beijing. A case-control study and affected sibpair were performed. Genotyping was carried out using a fluorescence-based semiautomated technique on automated DNA sequencer (ABI 377, PE). The basis for the genome-screen was the ABI prism linkage mapping sets of 400 microsatellite markers (version 2, PE, Co.). PCR for amplification of markers was carried out as multiplex reactions with Ampli Taq gold (PE, Co.) following protocols developed in our laboratory. Data were exported as a