机构地区:[1]包头医学院第一附属医院神经内科,014010
出 处:《国际脑血管病杂志》2011年第7期503-509,共7页International Journal of Cerebrovascular Diseases
基 金:包头市医药卫生科技发展基金(2009S1001-32)
摘 要:目的探讨基质金属蛋白酶(matrix metalloproteinase,MMP)-2C735T和MMP-9C1562T基因多态性与缺血性卒中患者的TOAST分型和转归的关系。方法232例缺血性卒中患者根据TOAST标准分被为大动脉粥样硬化性卒中(large artery atherosclerosis,LAA)(n=37)、心源性脑栓塞(cardioembolism,CE)(n=31)、小动脉闭塞性卒中(small artery occlusion,SAO)(n=65)、其他明确原因导致的卒中(stroke of other demonstrated etiology,SOE)(n=2)和原因不明性卒中(stroke of undemonstrated etiology,SUE)(n=97);对照组为235名健康者。采用限制性片段长度多态性技术检测MMP-2基因C735T和MMP-9基因C1562T多态性。采用Barthel指数(Barthel Index,BI)评价缺血性卒中患者发病21d和90d时的转归。结果缺血性卒中组(CC基因型:63.36%对54.04%,χ2=4.182,P=0.014;C等位基因:79.31%对74.04%,χ2=3.936;P=0.047)及其LAA亚型(CC基因型:78.37%对54.04%,χ2=7.740,P=0.005;C等位基因:87.83%对74.04%,χ2=6.655,P=0.01)MMP-2735CC基因型和C等位基因频率均显著高于对照组;缺血性卒中组(CT+TT基因型:21.98%对13.19%,χ2=6.233,P=0.013;T等位基因:11.64%对7.02%,χ2=5.891,P=0.015)及其LAA亚型(cT+TT基因型:32.43%对13.19%,χ2=8.892,P=0.003;T等位基因:20.27%对13.19%,χ2=13.950,P=0.000)MMP-91562CT+TT基因型频率和T等位基因频率也均显著高于对照组。多变量logistic回归分析显示,MMP-2735CC基因型(缺血性卒中:优势比1.099,95%可信区间1.038~1.260,P=0.028;LAA:优势比1.360,95%可信区间1.167~5.774,P=0.009)和MMP-91562TT基因型(缺血性卒中:优势比9.409,95%可信区间1.154—76.722,P=0.036;LAA:优势比8.962,95%可信区间1.380~58.218,P=0.022)携带者缺血性卒中以及LAA�Objective To investigate the association between matrix metalloproteinase (MMP) -2 C735T and MMP-9 C1562T polymorphisms and TOAST subtypes, the outcome in patients with stroke. Methods A total of 232 patients with ischemic stroke were divided into large artery atherosclerosis (LAA, n =37), cardioembolism (CE, n =31), small artery Occlusion (SAO, n = 65) stroke, stroke of other demonstrated etiology (SOE, n = 2), and stroke of undemonstrated etiology (SUE, n =97) according to TOAST criteria. A total of 235 healthy subjects in the outpatient served as control. Genetic polymorphisms of MMP-2 C735T and MMP-9 C1562T were identified by polymerase chain reaction-restriction fragnent length polymorphism. The outcome of patients was evaluated with Barthel Index (BI) at day 21 and 90 after stroke. Results The frequencies of MMP-2 735CC genotype and C allele in the ischemic stroke group (CC genotype: 63.36% vs. 54. 04%,χ2 =4. 182, P=0. 014; C allele: 79. 31%vs. 74. 04%, χ2 = 3. 936, P = 0. 047 ) and its LAA subtype ( CC genotype: 78.37% vs. 54. 04%, χ2 = 7. 740, P =0. 005; C allele: 87. 83% vs. 74. 04%, χ2 = 6. 655, P = 0. 01 ) were significantly higher than those in the control group. The frequencies of MMP-9 1562CT + TT genotype and T allele in the ischemic stroke group (CT +TT genotypes: 21.98% vs. 13.19%,χ2 =6. 233, P = 0. 013; T allele: 11.64% vs. 7. 02%,X2 =5. 891, P=0. 015) and its LAA subtype(CT +TT genotypes: 32.43% vs. 13.19% ,χ2 =8. 892, P =0. 003; T allele: 20. 27% vs. 13.19% ,χ2 = 13. 950, P = 0. 000). Multivariate logistic regression analysis indicated that risk of ischemic stroke and its LAA subtype with MMP-2 735CC genotype (ischemic stroke: odds ratio [ OR] 1. 099, 95% confidence interval [ CI] 1. 038-1. 260, P = 0. 028; LAA: OR 1. 360, 95% CI 1. 167-5. 774, P = 0. 009) and with MMP-9 1562TT genotype (ischemic stroke: OR 9. 409, 95% CI 1. 154-76. 722, P = 0. 036; LAA: OR 8. 962, 95% CI 1. 380-58. 218, P = 0. 022) increa
关 键 词:基质金属蛋白酶2 基质金属蛋白酶9 多态现象 遗传学 卒中 脑缺血 预后
分 类 号:R743.3[医药卫生—神经病学与精神病学]
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