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A Series of PSMA-Targeted Near-Infrared Fluorescent Imaging Agents

Ying Chen, Il Minn, Steven P. Rowe, Alla Lisok, Samit Chatterjee, Mary Brummet, Sangeeta Ray Banerjee, Ronnie C. Mease, Martin G. Pomper

BIOMOLECULES(2022)

Cited 1|Views14
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Abstract
We have synthesized a series of 10 new, PSMA-targeted, near-infrared imaging agents intended for use in vivo for fluorescence-guided surgery (FGS). Compounds were synthesized from the commercially available amine-reactive active NHS ester of DyLight800. We altered the linker between the PSMA-targeting urea moiety and the fluorophore with a view to improve the pharmacokinetics. Chemical yields for the conjugates ranged from 51% to 86%. The K-i values ranged from 0.10 to 2.19 nM. Inclusion of an N-bromobenzyl substituent at the epsilon-amino group of lysine enhanced PSMA(+) PIP tumor uptake, as did hydrophilic substituents within the linker. The presence of a polyethylene glycol chain within the linker markedly decreased renal uptake. In particular, DyLight800-10 demonstrated high specific uptake relative to background signal within kidney, confirmed by immunohistochemistry. These compounds may be useful for FGS in prostate, renal or other PSMA-expressing cancers.
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Key words
NIRF,molecular imaging,fluorescence-guided surgery,prostate-specific membrane antigen,DyLight800
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