浙江医学
浙江醫學
절강의학
ZHEJIANG MEDICAL JOURNAL
2013年
10期
881-884
,共4页
李彬斐%郑昌华%王希佳%陈亨平%张小罗
李彬斐%鄭昌華%王希佳%陳亨平%張小囉
리빈비%정창화%왕희가%진형평%장소라
帕金森病%G2385R基因型%单核苷酸
帕金森病%G2385R基因型%單覈苷痠
파금삼병%G2385R기인형%단핵감산
Parkinson’s disease%G2385R genetype%Single nucleotide
目的探讨LRRK2基因G2385R突变与中国沿海地区汉族人群帕金森病(PD)相关性,分析LRRK2基因多态在PD发病中的作用.方法收集PD患者197例(PD组)、健康对照者202例(对照组)的临床资料与基因组DNA.检测PD患者G2385R基因型;测定变异携带者及非携带者DNA序列.分析G2385R基因型在PD组和对照组中分布频率及其与性别、年龄相互作用,统计G2385R变异人群归因危险度百分比.结果 PD组[19例(9.64%)]患者GA基因型高于对照组[5例(2.48%)](字2=9.07, P<0.01,OR=5.04,95%CI=2.16~11.78).人群归因危险度百分比7.82%.未发现AA基因型.晚发型PD患者GA基因型为9.80%,与对照组(2.23%)比较,差异有统计学意义(P<0.01,OR=4.35,95%CI=1.76~12.93).携带G2385R患者与非携带患者临床表型在性别、发病年龄、临床症状、UPDRS评分及Hoehn-Yahr分级差异均无统计学意义(均P>0.05).结论 LRRK2基因G2385R变异在中国沿海地区汉族人群中与晚发性PD相关,存在不同地区差异.
目的探討LRRK2基因G2385R突變與中國沿海地區漢族人群帕金森病(PD)相關性,分析LRRK2基因多態在PD髮病中的作用.方法收集PD患者197例(PD組)、健康對照者202例(對照組)的臨床資料與基因組DNA.檢測PD患者G2385R基因型;測定變異攜帶者及非攜帶者DNA序列.分析G2385R基因型在PD組和對照組中分佈頻率及其與性彆、年齡相互作用,統計G2385R變異人群歸因危險度百分比.結果 PD組[19例(9.64%)]患者GA基因型高于對照組[5例(2.48%)](字2=9.07, P<0.01,OR=5.04,95%CI=2.16~11.78).人群歸因危險度百分比7.82%.未髮現AA基因型.晚髮型PD患者GA基因型為9.80%,與對照組(2.23%)比較,差異有統計學意義(P<0.01,OR=4.35,95%CI=1.76~12.93).攜帶G2385R患者與非攜帶患者臨床錶型在性彆、髮病年齡、臨床癥狀、UPDRS評分及Hoehn-Yahr分級差異均無統計學意義(均P>0.05).結論 LRRK2基因G2385R變異在中國沿海地區漢族人群中與晚髮性PD相關,存在不同地區差異.
목적탐토LRRK2기인G2385R돌변여중국연해지구한족인군파금삼병(PD)상관성,분석LRRK2기인다태재PD발병중적작용.방법수집PD환자197례(PD조)、건강대조자202례(대조조)적림상자료여기인조DNA.검측PD환자G2385R기인형;측정변이휴대자급비휴대자DNA서렬.분석G2385R기인형재PD조화대조조중분포빈솔급기여성별、년령상호작용,통계G2385R변이인군귀인위험도백분비.결과 PD조[19례(9.64%)]환자GA기인형고우대조조[5례(2.48%)](자2=9.07, P<0.01,OR=5.04,95%CI=2.16~11.78).인군귀인위험도백분비7.82%.미발현AA기인형.만발형PD환자GA기인형위9.80%,여대조조(2.23%)비교,차이유통계학의의(P<0.01,OR=4.35,95%CI=1.76~12.93).휴대G2385R환자여비휴대환자림상표형재성별、발병년령、림상증상、UPDRS평분급Hoehn-Yahr분급차이균무통계학의의(균P>0.05).결론 LRRK2기인G2385R변이재중국연해지구한족인군중여만발성PD상관,존재불동지구차이.
Objective To investigate the association between G2385R polymorphisms of LRRK2 gene and Parkinson's disease (PD). Methods The clinical data and peripheral blood samples were col ected from 197 PD patients and 202 healthy subjects. Polymerase Chain Reaction combined with restriction fragment length polymorphism(PCR-RFLP) was used to detected the G2385R genotypes of PD patients, the G2385R genotype was verified by the sequencing. The sex, age, clinical symptoms, UPDRS score and Hoehn-Yahr grade were compared among PD patients with different genotypes. The frequencies of genotype distribution of PD patients and healthy subjects were compared. The population attributable risk percent(PAR%)of G2385R varia-tions was counted and the synergy with gender and age interaction was analyzed. Results The genotype GA of G2385R was detected in 19 cases of PD(9.64%), while that was detected in 5 controls(2.48%)(χ2=9.07, P<0.01, OR=5.04, 95%CI:2.16~11.78) and the PAR%of 7.82%was gained. No PD patient with AA genotype was found. The genotype GA was detected in 15 cases of late-onset PD(9.80%), in the age-matched controls, there were only 4 subjects of GA genotype(2.23%)(P<0.01, OR=4.35, 95%CI:1.76~12.93). There were no significant differences in clinical phenotypes (sex, age, clinical symptoms, UPDRS score and Hoehn-Yahr grade)between patients carrying G2385R and those not carrying. Conclusion The G2385R variant in LRRK2 gene may be a risk factor of the late-onset Parkinson's disease in Han Chinese patients.
