脑脊液神经颗粒蛋白和 YKL-40 作为阿尔茨海默病的生物标志物。
Cerebrospinal fluid neurogranin and YKL-40 as biomarkers of Alzheimer's disease.
机构信息
Clinical Memory Research Unit Department of Clinical Sciences, Malmö Lund University Malmö Sweden.
Clinical Memory Research Unit Department of Clinical Sciences, Malmö Lund University Malmö Sweden; Memory Clinic Skåne University Hospital Malmö Sweden.
出版信息
Ann Clin Transl Neurol. 2015 Nov 20;3(1):12-20. doi: 10.1002/acn3.266. eCollection 2016 Jan.
OBJECTIVE
Widespread implementation of cerebrospinal fluid (CSF) biomarkers of Alzheimer's disease (AD) in clinical settings requires improved accuracy for diagnosis of prodromal disease and for distinguishing AD from non-AD dementias. Novel and promising CSF biomarkers include neurogranin, a marker of synaptic degeneration, and YKL-40, a marker of neuroinflammation.
METHODS
CSF neurogranin and YKL-40 were measured in a cohort of 338 individuals including cognitively healthy controls and patients with stable mild cognitive impairment (sMCI), MCI who later developed AD (MCI-AD), AD dementia, Parkinson's disease dementia (PDD), dementia with Lewy bodies (DLB), vascular dementia (VaD), and frontotemporal dementia (FTD). The diagnostic accuracy of neurogranin and YKL-40 were compared with the core AD biomarkers, β-amyloid (Aβ42 and Aβ40) and tau.
RESULTS
Neurogranin levels were increased in AD and decreased in non-AD dementia compared with healthy controls. As a result, AD patients showed considerably higher CSF levels of neurogranin than DLB/PDD, VaD and FTD patients. CSF YKL-40 levels were increased in AD compared with DLB/PDD but not with VaD or FTD. Neither CSF neurogranin nor YKL-40 levels differed significantly between sMCI patients and MCI-AD patients. Both biomarkers correlated positively with CSF Aβ40 and tau. CSF neurogranin and YKL-40 could separate AD dementia from non-AD dementias (neurogranin, area under the curve [AUC] = 0.761; YKL-40, AUC = 0.604; Aβ42/neurogranin, AUC = 0.849; Aβ42/YKL-40, AUC = 0.785), but the diagnostic accuracy was not better compared to CSF Aβ and tau (Aβ42, AUC = 0.755; tau AUC = 0.858; Aβ42/tau, AUC = 0.895; Aβ42/Aβ40, AUC = 0.881). Similar results were obtained when separating sMCI from MCI-AD cases.
INTERPRETATION
CSF neurogranin and YKL-40 do not improve the diagnostic accuracy of either prodromal AD or AD dementia when compared to the core CSF AD biomarkers. Nevertheless, the CSF level of neurogranin is selectively increased in AD dementia, whereas YKL-40 is increased in both AD and FTD suggesting that synaptic degeneration and glial activation may be important in these neurodegenerative conditions.
目的
为了在临床环境中广泛应用阿尔茨海默病(AD)的脑脊液(CSF)生物标志物,有必要提高对疾病前驱期的诊断准确性,以及对 AD 与非 AD 痴呆的鉴别能力。新型且有前景的 CSF 生物标志物包括神经颗粒蛋白,一种突触退化的标志物,以及 YKL-40,一种神经炎症的标志物。
方法
在包括认知健康对照者以及稳定轻度认知障碍(sMCI)、后来发展为 AD(MCI-AD)的 MCI、AD 痴呆、帕金森病痴呆(PDD)、路易体痴呆(DLB)、血管性痴呆(VaD)和额颞叶痴呆(FTD)的患者队列中,测量了 338 名个体的 CSF 神经颗粒蛋白和 YKL-40。比较了神经颗粒蛋白和 YKL-40 与核心 AD 生物标志物(β-淀粉样蛋白(Aβ42 和 Aβ40)和 tau)的诊断准确性。
结果
AD 患者的 CSF 神经颗粒蛋白水平升高,而非 AD 痴呆患者的 CSF 神经颗粒蛋白水平降低,与健康对照组相比。因此,AD 患者的 CSF 神经颗粒蛋白水平明显高于 DLB/PDD、VaD 和 FTD 患者。AD 患者的 CSF YKL-40 水平高于 DLB/PDD,但与 VaD 或 FTD 患者无差异。sMCI 患者与 MCI-AD 患者的 CSF 神经颗粒蛋白和 YKL-40 水平均无显著差异。两种生物标志物均与 CSF Aβ40 和 tau 呈正相关。CSF 神经颗粒蛋白和 YKL-40 可以将 AD 痴呆与非 AD 痴呆区分开(神经颗粒蛋白,曲线下面积 [AUC] = 0.761;YKL-40,AUC = 0.604;Aβ42/神经颗粒蛋白,AUC = 0.849;Aβ42/YKL-40,AUC = 0.785),但与 CSF Aβ 和 tau 相比,诊断准确性并无提高(Aβ42,AUC = 0.755;tau AUC = 0.858;Aβ42/tau,AUC = 0.895;Aβ42/Aβ40,AUC = 0.881)。当将 sMCI 与 MCI-AD 病例进行区分时,也得到了类似的结果。
解释
与核心 CSF AD 生物标志物相比,CSF 神经颗粒蛋白和 YKL-40 并不能提高 AD 前驱期或 AD 痴呆的诊断准确性。然而,AD 痴呆患者的 CSF 神经颗粒蛋白水平选择性升高,而 YKL-40 在 AD 和 FTD 中均升高,这表明突触退化和神经胶质激活可能在这些神经退行性疾病中很重要。
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