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急性卒中患者血浆β-珠蛋白DNA与S-100蛋白浓度的比较。

Comparison of plasma beta-globin DNA and S-100 protein concentrations in acute stroke.

作者信息

Rainer Timothy H, Wong Ka Sing, Lam Wynnie, Lam Nicole Y L, Graham Colin A, Lo Y M Dennis

机构信息

Accident and Emergency Medicine Academic Unit, The Chinese University of Hong Kong, Prince of Wales Hospital, Hong Kong, China.

出版信息

Clin Chim Acta. 2007 Feb;376(1-2):190-6. doi: 10.1016/j.cca.2006.08.025. Epub 2006 Aug 30.

Abstract

BACKGROUND

This study aimed to compare changes in plasma beta-globin DNA and serum S100 protein to diagnose stroke and for predicting mortality and morbidity.

METHODS

Patients with stroke-like symptoms presenting to the emergency department of a Hong Kong hospital were recruited. Plasma DNA was analyzed for the beta-globin gene with fluorescent-based PCR. S100 concentrations were determined using ELISA. Primary outcomes were diagnosis of stroke, mortality, and modified Rankin Score (mRS) after 6 months.

RESULTS

One hundred ninety-seven consecutive patients recruited, 118 (60%) ischemic stroke, 35 (18%) hemorrhage and 44 (22%) with no acute neuroimaging changes. Serum S100 and plasma DNA were increased in 126 (p<0.0010) and 36 (p=0.21) stroke patients respectively vs. controls. Median plasma DNA was higher in hemorrhagic stroke than those without (1725 vs. 1050 kilogenome-equivalents/l, p=0.0104). Median plasma DNA was higher in mRS>2 vs. mRS<or=2 (1350 vs. 1025, p=0.0103), and higher in non-survivors vs. survivors (1625 vs. 1050, p=0.0070). Median serum S100 higher in mRS>2 patients vs. mRS<or=2 (0.152 vs. 0.131 microg/l, p=0.0003). The odds ratio (OR) of discriminating hemorrhagic from non-hemorrhagic stroke with DNA was 4.24 (95% CI 1.88-9.56); S100 and DNA together give an OR of 16.55.

CONCLUSION

For stroke diagnosis, S100 performs better than DNA; DNA is a better marker for hemorrhage. For diagnosis of hemorrhagic stroke, combined S100 and DNA performs better than either alone. Plasma DNA and serum S100 predict morbidity and mortality in stroke.

摘要

背景

本研究旨在比较血浆β-珠蛋白DNA和血清S100蛋白的变化,以用于诊断中风以及预测死亡率和发病率。

方法

招募到香港一家医院急诊科出现类似中风症状的患者。采用荧光定量PCR分析血浆DNA中的β-珠蛋白基因。使用酶联免疫吸附测定法测定S100浓度。主要结局指标为中风诊断、死亡率以及6个月后的改良Rankin评分(mRS)。

结果

连续纳入197例患者,其中118例(60%)为缺血性中风,35例(18%)为出血性中风,44例(22%)无急性神经影像学改变。与对照组相比,中风患者中血清S100和血浆DNA升高的分别有126例(p<0.0010)和36例(p=0.21)。出血性中风患者的血浆DNA中位数高于无急性神经影像学改变者(1725对1050千基因组当量/升,p=0.0104)。mRS>2者的血浆DNA中位数高于mRS≤2者(1350对1025,p=0.0103),非幸存者的血浆DNA中位数高于幸存者(1625对1050,p=0.0070)。mRS>2患者的血清S100中位数高于mRS≤2者(0.152对0.131微克/升,p=0.0003)。用DNA区分出血性中风与非出血性中风的比值比(OR)为4.24(95%可信区间1.88 - 9.56);S100和DNA联合使用时OR为16.55。

结论

对于中风诊断,S100比DNA表现更好;DNA是出血的更好标志物。对于出血性中风的诊断,S100和DNA联合使用比单独使用任何一种表现更好。血浆DNA和血清S100可预测中风的发病率和死亡率。

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