中华神经医学杂志
中華神經醫學雜誌
중화신경의학잡지
CHINESE JOURNAL OF NEUROMEDICINE
2010年
10期
1037-1041
,共5页
高思山%谭兰%于楠楠%郁金泰%宋敬卉%马腾%王乃东
高思山%譚蘭%于楠楠%鬱金泰%宋敬卉%馬騰%王迺東
고사산%담란%우남남%욱금태%송경훼%마등%왕내동
神经肽Y%启动子%基因多态性%脑梗死%TOAST分型
神經肽Y%啟動子%基因多態性%腦梗死%TOAST分型
신경태Y%계동자%기인다태성%뇌경사%TOAST분형
Neuropeptide Y%Promoter%Gene polymorphism%Cerebral stroke%Subtype according to TOAST criteria
目的 针对脑梗死多因素致病特点,探讨神经肽Y(NPY)启动子基因多态性与脑梗死TOAST分型各亚型的关系. 方法 采用聚合酶链反应(PCR)和基因测序技术,检测549例脑梗死患者NPY启动子基因-399T/C、-883Tgins/del和-602G/T基因型及等位基因,其中大动脉粥样硬化型(LAA)190例,小动脉闭塞型(SAO)260例,心源性栓塞型(CE)60例,其他明确原因型(ODE)29例,原因不明型(UE)10例,并与423例汉族健康体检者对照.Logistic回归分析去除混杂因素影响,分析NPY启动子基因多态性与脑梗死TOAST分型各亚型的相关性. 结果 SAO亚型-399T/C突变基因型CC和等位基因C频率与对照组比较差异均有统计学意义(P=0.046,P=0.010);LAA亚型和SAO亚型高尿酸、高血压、心脏病和DM病史较对照组明显增高,比较差异有统计学意义(P<0.05);SAO亚型-883Tgins/del缺失突变基因型DD、等位基因D频率与对照组比较差异无统计学意义(P=0.061,P=0.155);-399T/C、-883Tgins/del、-602G/T多态性与LAA亚型、CE亚型、ODE亚型和UE亚型患者均无相关性. 结论 NPY启动子基因-399T/C多态性可能与脑梗死SAO亚型发病存在相关性,高频率等位基因-399C个体可能是SAO亚型重要危险因素.没发现-399T/C、-883Tgins/del、-602G/T基因多态性与LAA亚型、CE亚型、ODE亚型和UE亚型患者有相关性.高尿酸、高血压、心脏病和糖尿病史是LAA亚型和SAO亚型危险因素.
目的 針對腦梗死多因素緻病特點,探討神經肽Y(NPY)啟動子基因多態性與腦梗死TOAST分型各亞型的關繫. 方法 採用聚閤酶鏈反應(PCR)和基因測序技術,檢測549例腦梗死患者NPY啟動子基因-399T/C、-883Tgins/del和-602G/T基因型及等位基因,其中大動脈粥樣硬化型(LAA)190例,小動脈閉塞型(SAO)260例,心源性栓塞型(CE)60例,其他明確原因型(ODE)29例,原因不明型(UE)10例,併與423例漢族健康體檢者對照.Logistic迴歸分析去除混雜因素影響,分析NPY啟動子基因多態性與腦梗死TOAST分型各亞型的相關性. 結果 SAO亞型-399T/C突變基因型CC和等位基因C頻率與對照組比較差異均有統計學意義(P=0.046,P=0.010);LAA亞型和SAO亞型高尿痠、高血壓、心髒病和DM病史較對照組明顯增高,比較差異有統計學意義(P<0.05);SAO亞型-883Tgins/del缺失突變基因型DD、等位基因D頻率與對照組比較差異無統計學意義(P=0.061,P=0.155);-399T/C、-883Tgins/del、-602G/T多態性與LAA亞型、CE亞型、ODE亞型和UE亞型患者均無相關性. 結論 NPY啟動子基因-399T/C多態性可能與腦梗死SAO亞型髮病存在相關性,高頻率等位基因-399C箇體可能是SAO亞型重要危險因素.沒髮現-399T/C、-883Tgins/del、-602G/T基因多態性與LAA亞型、CE亞型、ODE亞型和UE亞型患者有相關性.高尿痠、高血壓、心髒病和糖尿病史是LAA亞型和SAO亞型危險因素.
목적 침대뇌경사다인소치병특점,탐토신경태Y(NPY)계동자기인다태성여뇌경사TOAST분형각아형적관계. 방법 채용취합매련반응(PCR)화기인측서기술,검측549례뇌경사환자NPY계동자기인-399T/C、-883Tgins/del화-602G/T기인형급등위기인,기중대동맥죽양경화형(LAA)190례,소동맥폐새형(SAO)260례,심원성전새형(CE)60례,기타명학원인형(ODE)29례,원인불명형(UE)10례,병여423례한족건강체검자대조.Logistic회귀분석거제혼잡인소영향,분석NPY계동자기인다태성여뇌경사TOAST분형각아형적상관성. 결과 SAO아형-399T/C돌변기인형CC화등위기인C빈솔여대조조비교차이균유통계학의의(P=0.046,P=0.010);LAA아형화SAO아형고뇨산、고혈압、심장병화DM병사교대조조명현증고,비교차이유통계학의의(P<0.05);SAO아형-883Tgins/del결실돌변기인형DD、등위기인D빈솔여대조조비교차이무통계학의의(P=0.061,P=0.155);-399T/C、-883Tgins/del、-602G/T다태성여LAA아형、CE아형、ODE아형화UE아형환자균무상관성. 결론 NPY계동자기인-399T/C다태성가능여뇌경사SAO아형발병존재상관성,고빈솔등위기인-399C개체가능시SAO아형중요위험인소.몰발현-399T/C、-883Tgins/del、-602G/T기인다태성여LAA아형、CE아형、ODE아형화UE아형환자유상관성.고뇨산、고혈압、심장병화당뇨병사시LAA아형화SAO아형위험인소.
Objective To explore the relationship between gene polymorphism of neuropeptide Y (NPY) promoter and cerebral stroke subtypes according to TOAST (Trail of ORG 10172 in Acute Stroke Treatment) criteria in Chinese Han population. Methods The gene polymorphisms at position of-399T/C, -883Tgins/del and -602G/T in NPY promoter were detected by PCR method and gene sequencing in 190 cases of large-artery atherosclerosis stroke (LAA), 260 cases of small-artery occlusion (SAO), 60 cases of cardioembolism stroke (CE), 29 cases of stroke of other demonstrated etiology (ODE),10 cases of stroke of other undemonstrated etiology (UE) and 423 healthy control subjects. The PCR products were directly sequenced. Multivariate logistic regression was performed to analyze the relationship between gene polymorphism of NPY promoter and cerebral stroke subtypes according to TOAST by removing the confounding variables. Results Significant differences in the frequency of genotype CC and allele C at position of-399T/C were noted between the patients with SAO and controls (P=0.046, P=0.010). Compared with the control group, patients with LAA and SAO were more likely having high level of uric acid, hypertension, diabetes mellitus and heard disease (P<0.05). No statistic differences in the frequency of genotype DD and allele D at position of-883Tgins/del were noted between patients with SAO and controls (P=0.0605, P=0.155). Gene polymorphisms of-399T/C,-883Tgins/del and -602G/T did not associate with an increased risk of having LAA, CE, ODE and UE.Conclusions The gene polymorphisms of promoter in position of-399T/C gene maybe associate with the happening of SAO; allele C at the position of-399T/C may raise the risk of the disease. There is no relationship between the gene polymorphisms of promoter at position of-399T/C, -883Tgins/del, -602G/T and the patients with LAA, CE, ODE and UE. High level of uric acid, hypertension, diabetes mellitus and heard disease history are the risk factors of LAA and SAO.
