The synthesis of a tritium, carbon-14, and stable isotope-labeled cathepsin C inhibitors

Allen Paul; Bragg Ryan A.; Caffrey MoyaEricsson CeciliaHickey Michael J.Kingston Lee P.Elmore Charles S.

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The synthesis of a tritium, carbon-14, and stable isotope-labeled cathepsin C inhibitors

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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 isotopelabeled AZD5248 were successfully prepared through modifications of the medicinal chemistry synthetic route, enabling the use of available labeled intermediates.

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《Journal of labelled compounds & radiopharmaceuticals.》 |2017年第2期|124-129|共6页
作者
Allen Paul; Bragg Ryan A.; Caffrey MoyaEricsson CeciliaHickey Michael J.Kingston Lee P.Elmore Charles S.;
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作者单位

AstraZeneca, Innovat Med & Early Dev Biotech Unit, Pharmaceut Sci, Gothenburg, Sweden;

AstraZeneca, Innovat Med & Early Dev Biotech Unit, Pharmaceut Sci, Cambridge, England;

AstraZeneca, Innovat Med & Early Dev Biotech Unit, Resp Inflammat & Autoimmun, Gothenburg, Sweden;

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原文格式 PDF
正文语种英语
中图分类药学;
关键词
carbon-13; carbon-14; cathepsin C; dipeptidyl peptidase I; tritium;

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The synthesis of a tritium, carbon-14, and stable isotope-labeled cathepsin C inhibitors

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