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首页> 外文期刊>Annals of laboratory medicine. >Clinical Usefulness of Cell-based Indirect Immunofluorescence Assay for the Detection of Aquaporin-4 Antibodies in Neuromyelitis Optica Spectrum Disorder
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Clinical Usefulness of Cell-based Indirect Immunofluorescence Assay for the Detection of Aquaporin-4 Antibodies in Neuromyelitis Optica Spectrum Disorder

机译:基于细胞的间接免疫荧光分析在视神经脊髓炎光谱障碍中检测Aquaporin-4抗体的临床实用性

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Background: The presence of antibodies to aquaporin-4 (AQP4) has been identified as a key characteristic of neuromyelitis optica spectrum disorder (NMOSD), an autoimmune inflammatory demyelinating central nervous system (CNS) disorder. We evaluated the performance of a cell-based indirect immunofluorescence assay (CIIFA) for detecting AQP4 antibodies using antigen prepared with a recombinant AQP4 peptide transfection technique and assessed the usefulness of CIIFA for diagnosis of NMOSD in routine clinical practice. Methods: Forty-six serum samples from 36 patients as a comparison set and another 101 patients enrolled consecutively from a neurology clinic were included. CIIFA and fluorescence immunoprecipitation assays (FIPA) were performed. CIIFA was performed at 2 different institutions for comparison purposes. Results: CIIFA and FIPA sensitivity in the comparison set was 86% and 79% in neuromyelitis optica (NMO) patients and 55% and 36% in high-risk NMO patients, respectively. The semiquantitative titer measured by CIIFA correlated well with the arbitrary unit (fluorescence units [FU]) derived from FIPA (r=0.66). Titers measured by CIIFA and FIPA were elevated in NMO patients compared to high-risk NMO patients (1:240 vs. 1:180 and 8,390 vs. 4,059 FU, respectively). The frequency of AQP4 antibody detection by CIIFA in 101 consecutively enrolled patients was 100% in NMO and 23% in high-risk NMO patients, while only 4.6% in control patients, including those with multiple sclerosis. Conclusions: Detection of AQP4 antibodies by CIIFA provides sensitive and highly specific diagnostic information for NMO and high-risk NMO patients, which can be used to differentiate these conditions from other demyelinating CNS diseases.
机译:背景:水通道蛋白4(AQP4)抗体的存在已被确定为视神经脊髓炎光谱症(NMOSD)的关键特征,这是一种自身免疫性炎性脱髓鞘性中枢神经系统(CNS)疾病。我们评估了使用基于重组AQP4肽转染技术制备的抗原的基于细胞的间接免疫荧光测定(CIIFA)检测AQP4抗体的性能,并评估了CIIFA在常规临床实践中对NMOSD诊断的有用性。方法:包括来自36例患者的46份血清样本作为比较集,另外101例来自神经病学诊所连续入组的患者。进行了CIIFA和荧光免疫沉淀试验(FIPA)。 CIIFA在两个不同的机构进行了比较。结果:对照组的CIIFA和FIPA敏感性分别为视神经脊髓炎(NMO)患者的86%和79%,高危NMO患者的CIIFA和FIPA敏感性分别为55%和36%。 CIIFA测得的半定量滴定度与FIPA衍生的任意单位(荧光单位[FU])具有良好的相关性(r = 0.66)。与高风险的NMO患者相比,NMO患者通过CIIFA和FIPA测得的滴度升高(分别为1:240对1:180和8,390对4,059 FU)。 CIIFA在101名连续入组的患者中通过CIIFA检测AQP4抗体的频率在NMO中为100%,在高危NMO患者中为23%,而在对照组(包括多发性硬化症)中只有4.6%。结论:通过CIIFA检测AQP4抗体可为NMO和高危NMO患者提供灵敏且高度特异性的诊断信息,可用于将这些疾病与其他脱髓鞘的CNS疾病区分开来。

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