化学
表面改性
金属化
组合化学
基础(拓扑)
模块化设计
立体化学
计算机科学
程序设计语言
数学
数学分析
物理化学
作者
Matheus Andrade Meirelles,Ian de Toledo,Samuel Thurow,Gabriela Barreiro,Rafael M. Couñago,Ronaldo A. Pilli
标识
DOI:10.1021/acs.joc.3c00500
摘要
Two routes to the antimalarial diaminopyrimidine P218 were developed based on the C-6 metalation of suitable 2,4-dichloro-5-alkoxy pyrimidines using (TMP)2Zn·2MgCl2·2LiCl base. One approach involves a late-stage modification of the C-6 position, while the other allows for tail fragment modification of P218. Both routes have proven reliable in synthesizing P218, as well as eight analogues. These innovative strategies have the potential to contribute to the search for new antimalarial drugs.
科研通智能强力驱动
Strongly Powered by AbleSci AI