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首页> 外文期刊>Journal of Neurology >Diagnostic value of CSF protein profile in a Portuguese population of sCJD patients
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Diagnostic value of CSF protein profile in a Portuguese population of sCJD patients

机译:脑脊液蛋白谱在葡萄牙sCJD患者人群中的诊断价值

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摘要

The clinical diagnosis of sporadic Creutzfeldt–Jakob disease (sCJD) is difficult, and reliable markers are highly desired. In this work we assess the value of several cerebrospinal fluid (CSF) markers for sCJD diagnosis. Within the framework of the Portuguese Epidemiological Surveillance Program for Human Prion Diseases, CSF samples from 71 patients with clinically suspected sCJD, 30 definite sCJD and 41 non-CJD patients, were analysed for the presence of 14-3-3 protein. CSF levels of tau (t-tau), and phosphorylated tau (p-tau181), S-100b and β amyloid (Aβ42) proteins were determined. The influence of clinical and genetic characteristics on CSF markers sensitivity was also evaluated. Protein 14-3-3 was detected in 29/30 sCJD patients and 9/41 non-CJD patients. Extremely elevated t-tau and S-100b protein levels were found in sCJD patients, while p-tau181 levels were only slightly elevated and Aβ42 showed no differences compared to controls. 14-3-3 was the most sensitive parameter (97%), but its specificity was low (78%); sensitivity/specificity for other proteins were: S-100b—93/93%, t-tau—93/95%, with maximum accuracy being obtained by a combination of tests (14-3-3 combined with either t-tau or S-100b, or combining S-100b with t-tau/Aβ42 or p-tau/t-tau ratios). The sensitivity of 14-3-3, as well as of p-tau181/t-tau ratio, was decreased in younger patients with long disease duration, with the PrP-2 isotype and MV genotype. Both 14-3-3, t-tau and S-100b are sensitive markers for sCJD, but 14-3-3 specificity seems to be lower in this special clinical setting of rapidly progressing dementias. We propose that in cases with a 14-3-3 weak positive result, or in young patients with long disease duration, a second CSF marker would be valuable for the diagnosis of sCJD.
机译:散发性克雅氏病(sCJD)的临床诊断很困难,并且高度需要可靠的标记物。在这项工作中,我们评估了几种脑脊液(CSF)标记物对sCJD诊断的价值。在葡萄牙人类Pri病毒疾病流行病学监测计划的框架内,分析了71名临床疑似sCJD,30例确诊sCJD和41例非CJD患者的CSF样本中14-3-3蛋白的存在。测定了tau(t-tau)和磷酸化tau(p-tau181),S-100b和β淀粉样蛋白(Aβ42)的CSF水平。还评估了临床和遗传特征对脑脊液标志物敏感性的影响。在29/30 sCJD患者和9/41非CJD患者中检测到蛋白质14-3-3。在sCJD患者中发现t-tau和S-100b蛋白水平极度升高,而p-tau181水平仅轻微升高,而Aβ42与对照组相比无差异。 14-3-3是最敏感的参数(97%),但特异性较低(78%);对其他蛋白质的敏感性/特异性为:S-100b-93 / 93%,t-tau-93 / 95%,通过组合测试(14-3-3与t-tau或S -100b,或将S-100b与t-tau /Aβ42或p-tau / t-tau比例结合使用)。在患有病程长,具有PrP-2同型和MV基因型的年轻患者中,14-3-3的敏感性以及p-tau181 / t-tau比的敏感性降低。 14-3-3,t-tau和S-100b都是sCJD的敏感标志物,但在这种快速发展的痴呆症的特殊临床环境中14-3-3特异性似乎较低。我们建议在阳性结果为14-3-3的情况下或在病程长的年轻患者中,第二个CSF标记物对于sCJD的诊断将是有价值的。

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