PET 和 SPECT 成像是检测和鉴别神经退行性疾病非典型表型的可靠指南

Livia Ruffini, Alessandro Zilioli, Veronica Cervati, F. Lauretani, Francesco Misirocchi, Marcello Maggio, S. Migliari, T. Graziani, C. Cidda, Giorgio Baldari, M. Spallazzi, M. Scarlattei
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引用次数: 0

摘要

导言和目的。神经退行性疾病的非典型或混合表现可能会推迟或混淆最终诊断。利用正电子发射计算机断层扫描(PET)和单光子发射计算机断层扫描(SPECT)放射性配体进行分子成像可提供靶点特异性信息,并可通过 "体内 "检测神经病理基质(如 Aβ 沉积、黑质多巴胺能耗竭或 tau 包涵体)来预测诊断。这篇简短的综述将讨论 PET 和 SPECT 成像作为一种可靠的指南,在临床常规中更好地描述神经退行性变的非典型表型的潜力,它有可能推动个性化干预,提高临床试验的队列一致性,并作为靶向分子疗法的生物标记物。材料与方法使用电子数据库PubMed/MEDLINE和网络搜索引擎Google、Google Scholar进行文献检索,重点研究PET和SPECT成像在评估神经变性非典型表型中的作用。文献分析。新的改善病情药物在早期使用时可能会提高疗效,这对工作人士和出现不典型症状的年轻患者尤为重要。在老年人中,神经细胞变性、与年龄有关的变化、脑血管病变或抑郁症的同时存在,使得明确诊断变得十分困难。能够测量示踪剂分布的定量工具提高了分子神经成像的准确性,可绘制地形图,将受试者的数据与健康对照数据库进行比较。结论非典型表型可能与定量关键模式有关,从而可以更准确、更早期地诊断神经退行性疾病。最后,对病理基质的定量评估可让我们跟踪疾病进程并衡量治疗反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
PET and SPECT imaging as a solid guide to detect and discriminate atypical phenotypes of neurodegenerative disorders
Introduction and aim. Atypical or mixed presentations of neurodegenerative disorders may postpone or confound the final diagnosis. Molecular imaging with positron emission tomography (PET) and single photon emission computed tomography (SPECT) radioligands provide target-specific information and may anticipate the diagnosis by “in vivo” detection of the neuro pathological substrate, as Aβ deposition, nigrostriatal dopaminergic depletion or tau inclusions. This concise review will dis cuss the potential of PET and SPECT imaging as a solid guide to better characterize atypical phenotypes of neurodegeneration in the clinical routine, with the potential to drive personalized interventions, improve cohort uniformity for clinical trials, and serve as biomarkers for targeted molecular therapies. Material and methods. Literature search was performed focusing on the role of PET and SPECT imaging in assessing atypical phenotypes of neurodegeneration, using the electronic source of database PubMed/MEDLINE and the web-based search engines Google, Google Scholar. Analysis of the literature. New disease-modifying drugs may increase their effect with early initiation, which is especially im portant in working persons and younger subjects presenting atypical symptoms. In older individuals, the coexistence of neu rodegeneration, age-related changes, cerebrovascular lesions, or depression makes challenging a definitive diagnosis. Quantitative tools able to measure tracer distribution increase the accuracy of molecular neuroimaging creating topographic maps that compare subject’s data with healthy controls databases. Conclusion. Atypical phenotypes may be associated with quantitative key-pattern allowing a more precise and early diagnosis of the neurodegenerative disorder. Finally, quantitative assessment of the pathological substrates allows us to track the disease process and measure treatment response.
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