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The synthesis of a tritium,carbon‐14, and stable isotope‐labeled cathepsin C inhibitors
Abstract:
As part of a medicinal chemistry program aimed at developing a highly potent and selective cathepsin C inhibitor, tritium, carbon‐14, and stable isotope‐labeled materials were required. The synthesis of tritium‐labeled methanesulfonate 5 was achieved via catalytic tritiolysis of a chloro precursor, albeit at a low radiochemical purity of 67%. Tritium‐labeled AZD5248 was prepared via a 3‐stage synthesis, utilizing amide‐directed hydrogen isotope exchange. Carbon‐14 and stable isotope‐labeled AZD5248 were successfully prepared through modifications of the medicinal chemistry synthetic route, enabling the use of available labeled intermediates.
Keywords:carbon‐13  carbon‐14  cathepsin C  dipeptidyl peptidase I  tritium
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