4.2 Article

Assessment of brain beta-amyloid deposition in transgenic mouse models of Alzheimer's disease with PET imaging agents 18F-flutemetamol and 18F-florbetaben

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BMC NEUROSCIENCE
卷 19, 期 -, 页码 -

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BMC
DOI: 10.1186/s12868-018-0447-7

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PET/CT imaging; Alzheimer's disease; transgenic mouse model; F-18-flutemetamol; F-18-florbetaben

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Background: Although amyloid beta (A beta) imaging is widely used for diagnosing and monitoring Alzheimer's disease in clinical fields, paralleling comparison between F-18-flutemetamol and F-18-florbetaben was rarely attempted in AD mouse model. We performed a comparison of A beta PET images between F-18-flutemetamol and F-18-florbetaben in a recently developed APPswe mouse model, C57BL/6-Tg (NSE-hAPPsw) Korl. Results: After an injection (0.23 mCi) of F-18-flutemetamol and F-18-florbetaben at a time interval of 2-3 days, we compared group difference of SUVR and kinetic parameters between the AD (n = 7) and control (n = 7) mice, as well as between F-18-flutemetamol and F-18-florbetaben image. In addition, bio-distribution and histopathology were conducted. With visual image and VOI-based SUVR analysis, the AD group presented more prominent uptake than did the control group in both the F-18-florbetaben and F-18-flutemetamol images. With kinetic analysis, the F-18-florbetaben images showed differences in K1 and k4 between the AD and control groups, although F-18-flutemetamol images did not show significant difference. F-18-florbetaben images showed more prominent cortical uptake and matched well to the thioflavin S staining images than did the F-18-flutemetamol image. In contrast, F-18-flutemetamol images presented higher K1, k4, K1/k2 values than those of F-18-florbetaben images. Also, F-18-flutemetamol images presented prominent uptake in the bowel and bladder, consistent with higher bio-distribution in kidney, lung, blood and heart. Conclusions: Compared with F-18-flutemetamol images, F-18-florbetaben images showed prominent visual uptake intensity, SUVR, and higher correlations with the pathology. In contrast, F-18-flutemetamol was more actively metabolized than was F-18-florbetaben (Son et al. in J Nucl Med 58(Suppl 1): S278, 2017].

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