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钯(II)介导的复杂药物 C-H 氚化反应。

Palladium(II)-Mediated C-H Tritiation of Complex Pharmaceuticals.

机构信息

Department of Process Research & Development, MRL, Merck Sharp & Dohme Corp., Rahway, NJ, 07065, USA.

出版信息

Angew Chem Int Ed Engl. 2018 Feb 12;57(7):1883-1887. doi: 10.1002/anie.201711364. Epub 2018 Feb 1.

Abstract

Tritium-labeled molecules are critical tools for elucidating the binding and metabolic properties of bioactive compounds, particularly during pharmaceutical discovery. Direct tritiation of inert C-H bonds with T gas is an ideal approach for tritium labeling, but significant gaps remain for direct tritiation of structurally complex molecules with diverse functional groups. Here we report the first application of palladium(II) C-H activation chemistry for tritiation with T gas. This practical transformation exhibits novel substrate scope and greater functional group tolerance compared to previous state of the art tritiation methods, and has been applied to directly tritiate 9 complex pharmaceuticals and an unprotected dipeptide. The isolated tritium-labeled products exhibit >15 Ci mmol specific activity, exceeding the typical requirements for application in studies of molecular interaction and metabolism.

摘要

氚标记分子是阐明生物活性化合物结合和代谢特性的关键工具,特别是在药物发现过程中。用 T 气体直接氚化惰性 C-H 键是氚标记的理想方法,但对于具有多种官能团的结构复杂的分子的直接氚化仍存在显著差距。在这里,我们报告了钯 (II) C-H 活化化学用于 T 气体氚化的首次应用。与先前的最先进的氚化方法相比,这种实用的转化具有新颖的底物范围和更大的官能团耐受性,并已应用于直接氚标记 9 种复杂药物和一种未保护的二肽。分离的氚标记产物的比活度>15 Ci mmol,超过了在分子相互作用和代谢研究中应用的典型要求。

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