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18F-PI-2620 作为一种强效 PET 放射性示踪剂,用于阿尔茨海默病和其他神经退行性疾病中 tau 蛋白的临床评估,与 18F-THK-5351 相比。

Clinical Evaluation of 18F-PI-2620 as a Potent PET Radiotracer Imaging Tau Protein in Alzheimer Disease and Other Neurodegenerative Diseases Compared With 18F-THK-5351.

机构信息

From the Departments of Nuclear Medicine.

Neurology, Asan Medical Center, University of Ulsan College of Medicine, Seoul, South Korea.

出版信息

Clin Nucl Med. 2020 Nov;45(11):841-847. doi: 10.1097/RLU.0000000000003261.

Abstract

PURPOSE

PET is a useful tool for detecting the presence and extent of brain tau accumulation. However, most first-generation tau PET tracers are limited for high off-target binding and detection of tau in non-Alzheimer disease (AD). This study evaluated potential clinical applications of F-PI-2620 as a novel PET tracer with a high binding affinity for tau deposition in AD and non-AD tauopathies.

METHODS

Twenty-six participants diagnosed with either mild cognitive impairment, probable AD, frontotemporal dementia, or parkinsonism, as well as healthy controls underwent a 60- to 90-minute brain PET scan after 7 mci (259 MBq) injection of F-PI-2620. Some participants had previous PET scans using F-THK-5351 or F-FP-CIT for dopamine transporter imaging.

RESULTS

All participants showed no increase in off-target binding in basal ganglia on F-PI-2620 PET images, as noted for first-generation tau tracers. Aβ+ mild cognitive impairment or AD patients showed diverse cortical F-PI-2620 uptake in frontotemporoparietal cortex that correlated with Mini-Mental Status Examination (ρ = -0.692, P = 0.013). Aβ+ Parkinson disease with dementia and (Aβ unknown) primary progressive aphasia patients also showed increased F-PI-2620 uptakes in the frontotemporoparietal cortex. Patients with parkinsonism showed increased uptakes in the pallidum compared with Aβ- healthy controls (left: 1.41 ± 0.14 vs 1.04 ± 0.13, P = 0.014; right: 1.18 ± 0.16 vs 0.95 ± 0.07, P = 0.014).

CONCLUSIONS

F-PI-2620 PET might be a sensitive tool to detect cortical tau deposits in patients with Aβ+ AD and Aβ+ non-AD tauopathies. Furthermore, this study showed that "off-target" binding in the basal ganglia does not affect F-PI-2620.

摘要

目的

正电子发射断层扫描(PET)是一种用于检测脑 tau 积聚的存在和程度的有用工具。然而,大多数第一代 tau PET 示踪剂由于与高脱靶结合和检测非阿尔茨海默病(AD)tau 有关,因此受到限制。本研究评估了 F-PI-2620 作为一种新型 PET 示踪剂的潜在临床应用,该示踪剂对 AD 和非 AD tau 病中的 tau 沉积具有高结合亲和力。

方法

26 名被诊断为轻度认知障碍、可能的 AD、额颞叶痴呆或帕金森病的参与者以及健康对照者在注射 7 mci(259 MBq)F-PI-2620 后进行了 60-90 分钟的脑 PET 扫描。一些参与者之前曾进行过使用 F-THK-5351 或 F-FP-CIT 进行多巴胺转运蛋白成像的 PET 扫描。

结果

所有参与者在 F-PI-2620 PET 图像上均未出现基底节的脱靶结合增加,这与第一代 tau 示踪剂一样。Aβ+轻度认知障碍或 AD 患者在前额顶颞叶皮层显示出不同的皮质 F-PI-2620 摄取,与简易精神状态检查(Mini-Mental State Examination,MMSE)呈负相关(ρ=-0.692,P=0.013)。Aβ+帕金森病伴痴呆和(Aβ 未知)原发性进行性失语症患者在前额顶颞叶皮层也显示出 F-PI-2620 摄取增加。与 Aβ-健康对照组相比,帕金森病患者的苍白球摄取增加(左侧:1.41±0.14 比 1.04±0.13,P=0.014;右侧:1.18±0.16 比 0.95±0.07,P=0.014)。

结论

F-PI-2620 PET 可能是一种灵敏的工具,可用于检测 Aβ+AD 和 Aβ+非 AD tau 病患者的皮质 tau 沉积。此外,本研究表明,基底节中的“脱靶”结合不会影响 F-PI-2620。

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