Verna and Marrs McLean Department of Biochemistry and Molecular Pharmacology, Baylor College of Medicine, One Baylor Plaza, Houston, Texas 77030, United States.
Department of Chemistry, Rice University, 6100 Main Street, Houston, Texas 77005, United States.
Org Lett. 2024 May 3;26(17):3493-3497. doi: 10.1021/acs.orglett.4c00528. Epub 2024 Mar 20.
The morpholine heterocycle is a structural unit found in many bioactive compounds and FDA-approved drugs, but the generation of more complex C-functionalized morpholine derivatives remains considerably underexplored. Using systematic chemical diversity (SCD), a concept that guides the expansion of saturated drug-like scaffolds through regiochemical and stereochemical variation, we describe the synthesis of a collection of methyl-substituted morpholine acetic acid esters starting from enantiomerically pure amino acids and amino alcohols. In total, 24 diverse substituted morpholines were produced that vary systematically in regiochemistry and stereochemistry (relative and absolute). These diverse C-substituted morpholines can be directly applied in fragment screening or incorporated as building blocks in medicinal chemistry and library synthesis.
吗啡啉杂环是许多生物活性化合物和 FDA 批准药物中的结构单元,但更复杂的 C 功能化吗啡啉衍生物的生成仍在很大程度上未被探索。使用系统化学多样性 (SCD),这一概念通过区域化学和立体化学变化指导饱和类似药物支架的扩展,我们描述了从对映体纯氨基酸和氨基醇开始的一系列甲基取代吗啡啉乙酸酯的合成。总共产生了 24 种不同取代的吗啡啉,它们在区域化学和立体化学(相对和绝对)上系统地变化。这些不同的 C 取代吗啡啉可以直接应用于片段筛选,也可以作为药物化学和文库合成中的构建块。
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