羟醛反应
化学
恶唑
立体中心
维蒂希反应
立体化学
立体选择性
绝对构型
全合成
烷基化
产量(工程)
手性(物理)
对映选择合成
有机化学
催化作用
夸克
物理
量子力学
手征对称破缺
冶金
材料科学
Nambu–Jona Lasinio模型
作者
David A. Evans,Duke M. Fitch,Thomas E. Smith,Victor J. Cee
摘要
The synthesis of phorboxazole B has been accomplished in 27 linear steps and an overall yield of 12.6%. The absolute stereochemistry of the C4−C12, C33−C38, and C13−C19 fragments was established utilizing catalytic asymmetric aldol methodology, while the absolute stereochemistry of the C20−C32 fragment was derived from an auxiliary-based asymmetric aldol reaction. All remaining chirality was incorporated through internal asymmetric induction, with the exception of the C43 stereocenter which was derived from (R)-trityl glycidol. Key fragment couplings include a stereoselective double stereodifferentiating aldol reaction, a metalated oxazole alkylation, an oxazole-stabilized Wittig olefination, and a chelation-controlled addition of the fully elaborated alkenyl metal side chain.
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