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Development of a novel radioiodinated glucose derivative with interaction to hexokinase

✍ Scribed by Yasuhiro Magata; Hideo Saji; Yoshiro Ohmomo; Chiaki Tanaka; Junji Konishi; Akira Yokoyama


Publisher
John Wiley and Sons
Year
1992
Tongue
French
Weight
592 KB
Volume
31
Category
Article
ISSN
0022-2135

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✦ Synopsis


Abstract

Development of an ^123^I‐labeled glucose derivative that interacted with hexokinase was attempted. By introducing a benzene ring into the glucosamine molecule, we were able to secure a radioiodinated compound, N‐iodobenzoyl‐D‐glucosamine (BGA), with enhanced stability. As a result, a non‐competitive inhibitory agent on the hexokinase‐regulated phosphorylation reaction was achieved. The inhibitory action and lipophilic property of this novel compound were closely related to an amide bond in its structural configuration. Moreover, on investigating the biodistribution in mice, although this ^125^I‐labeled compound did not display any uptake into the brain, it demonstrated rapid clearance from the blood with high systemic stability. From the above findings, it is highly possible to develop a clinically feasible ^123^I‐labeled radioligand that can monitor the quantitative changes and biodistribution of hexokinase.


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