Gerona-Navarro G, Bonache M A, Herranz R, García-López M T, González-Muñiz R
Instituto de Química Médica (CSIC), Juan de la Cierva 3, 28006 Madrid, Spain.
J Org Chem. 2001 May 18;66(10):3538-47. doi: 10.1021/jo015559b.
A systematic study on the base-assisted intramolecular alkylation of N-benzyl-N-chloroacetyl amino acid derivatives is described. This study resulted in the first concise and versatile route to the preparation of 3-unsubstituted 4-alkyl-4-carboxy-2-azetidinones, to be included into the scarce family of beta-lactams with quaternary centers at the C(4) position. Particularly noteworthy is that the intramolecular N(alpha)-C(alpha)-cyclization of Phe and Leu derivatives afforded the corresponding beta-lactam derivatives with moderate enantioselectivity (up to 56%). It is suggested that, in these particular cases, the cyclization reaction proceeds by way of planar enolate intermediates, which possess dynamic chirality. The described sequence of reactions, that is compatible with commonly used protecting moieties for the alpha-carboxy group, cannot be applied to dipeptides, since the cyclization to the six-membered 2,5-diketopiperazine ring occurs preferentially.
本文描述了对N-苄基-N-氯乙酰基氨基酸衍生物的碱辅助分子内烷基化反应的系统研究。该研究首次提供了一种简洁通用的方法来制备3-未取代的4-烷基-4-羧基-2-氮杂环丁酮,这类化合物属于在C(4)位带有季碳中心的稀缺β-内酰胺家族。特别值得注意的是,苯丙氨酸和亮氨酸衍生物的分子内N(α)-C(α)-环化反应以中等对映选择性(高达56%)得到了相应的β-内酰胺衍生物。研究表明,在这些特定情况下,环化反应通过具有动态手性的平面烯醇盐中间体进行。所描述的反应序列与α-羧基常用的保护基团兼容,但不能应用于二肽,因为二肽优先环化形成六元的2,5-二酮哌嗪环。
