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Diagnostic accuracy of DAT-SPECT and MIBG scintigraphy for dementia with Lewy bodies: an updated systematic review and Bayesian latent class model meta-analysis

机译:利用Lewy机构诊断Dat-Spect和MIBG Scintaphy的诊断准确性:更新的系统评论和贝叶斯潜在型号Meta分析

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Purpose Imperfect clinical reference standards can preclude accurately estimating the diagnostic accuracy of DAT-SPECT and MIBG myocardial scintigraphy for diagnosing DLB. To investigate the validity of unadjusted accuracy, we updated our previous meta-analysis. Methods Literature search was updated to March 18, 2018. We also examined published systematic review reports. Two investigators extracted data and rated study validity using the QUADAS-2 tool. We performed a Bayesian latent class model meta-analysis accounting for imperfect reference standards. Results We evaluated 27 studies including 2236 patients. With the exception of two DAT-SPECT studies that involved postmortem neuropathological verification, studies were susceptible to bias from imperfect reference standards. Compared with the unadjusted accuracy estimates, the adjusted sensitivity values were similar, whereas the adjusted specificity values were generally lower for detecting alpha-synuclein pathology in the brain. The adjusted summary sensitivity and specificity were 0.86 (95% credible interval [CrI], 0.76-0.95) and 0.81 (CrI, 0.70-0.92), and 0.93 (CrI, 0.74-1.00) and 0.75 (CI, 0.47-0.94) for visual and semi-quantitative assessments of DAT-SPECT, respectively; 0.92 (CrI, 0.81-0.99) and 0.80 (CrI, 0.67-0.93), and 0.87 (CrI, 0.74-0.98) and 0.80 (CrI, 0.69-0.93), for delayed- and early-phase scans of MIBG scintigraphy, respectively. When diagnosing the typical clinical syndrome, the adjusted accuracy values were similar to the unadjusted estimates. The adjusted sensitivity and specificity were 0.89 (CrI, 0.75-0.98) and 0.87 (CrI, 0.72-0.97), and 0.97 (CrI, 0.78-1.0) and 0.70 (CrI, 0.43-0.92) for visual and semi-quantitative assessments of DAT-SPECT, respectively; and 0.93 (CrI, 0.81-0.98) and 0.90 (CrI, 0.73-0.97), and 0.85 (CrI, 0.66-0.96) and 0.96 (95% CI, 0.83-1.0) for delayed- and early-phase scans of MIBG scintigraphy, respectively. Conclusions In our adjusted analyses, both imaging biomarkers had high diagnostic accuracy for detecting the hallmark pathology in the brain and for diagnosing the typical clinical syndrome.
机译:目的不完美的临床参考标准可以准确地估算DAT-SPECT和MIBG心肌闪烁诊断诊断DLB的诊断准确性。要调查不调整准确性的有效性,我们更新了我们以前的META分析。方法文献搜索已更新到2018年3月18日。我们还审查了已发布的系统审查报告。两位调查人员使用Quadas-2工具提取数据和额定研究有效性。我们执行了贝叶斯潜在级模型Meta分析核算,以实现不完美的参考标准。结果我们评估了27项研究,包括2236名患者。除了涉及后期神经病理学核查的两个DAT-SPECT研究外,研究易受来自不完美参考标准的偏见。与不调整的精度估计相比,调节的敏感性值相似,而调整后的特异性值通常降低用于检测大脑中的α-突触核蛋白病理学。调整后的摘要敏感性和特异性为0.86(95%可靠的间隔[CRI],0.76-0.95)和0.81(CRI,0.70-0.92),0.93(CRI,0.74-1.00)和0.75(CI,0.47-0.94)分别的Dat-Spect视觉和半定量评估; 0.92(CRI,0.81-0.99)和0.80(CRI,0.67-0.93)和0.87(CRI,0.74-0.98)和0.80(CRI,0.69-0.93),分别用于MIBG Scintigraphy的延迟和早期扫描。在诊断典型的临床综合征时,调整后的精度值类似于未调整的估计值。调节的敏感性和特异性为0.89(CRI,0.75-0.98)和0.87(CRI,0.72-0.97)和0.97(CRI,0.78-1.0)和0.70(CRI,0.43-0.92),用于视觉和半定量评估DAT-SPECT分别; 0.93(CRI,0.81-0.98)和0.90(CRI,0.73-0.97)和0.85(CRI,0.66-0.96)和0.96(95%CI,0.83-1.0),用于MIBG Scintaphy的延迟和早期扫描, 分别。结论在我们调整后的分析中,两种成像生物标志物都具有高诊断准确性,用于检测大脑中的标志病理学和诊断典型的临床综合征。

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