Peptide substitution stabilizes GRPR antagonist while maintaining its biological features

Oct. 21, 2022

The suboptimal metabolic stability of radiolabeled gastrin-releasing peptide receptor (GRPR) antagonists has been a hindering factor of these promising theranostic candidates for prostate cancer. Uppsala University researchers have recently reported the development of [111In]DOTAGA-PEG-2-SAR11-RM-26, after replacement of Gly11 by Sar11 in the peptidic chain.

BioWorld Science Conferences New compound Diagnostics

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Peptide substitution stabilizes GRPR antagonist while maintaining its biological features