药效团
化学
谷氨酰胺
氢解
组合化学
蛋白酵素
蛋白酶
生物化学
立体化学
氨基酸
酶
催化作用
作者
Wayne Vuong,John C. Vederas
标识
DOI:10.1021/acs.joc.1c01299
摘要
An intermediate in the synthesis of numerous antiviral protease inhibitors is the glutamine analogue, (3S)-pyrrolid-2-one-3-yl-l-alanine. Preparations of compounds based on this pharmacophore are hindered by the lack of a reliably high yielding synthesis of protected forms of this amino acid. We describe an improved scalable route with readily available reagents and facile purification. This methodology employs γ-allylation of dimethyl N-BocGlu, further Boc N-protection, OsO4-periodate oxidation, O-Me oxime formation, and RaNi-catalyzed hydrogenolysis with concomitant cyclization under basic conditions.
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