Peters René, Althaus Martin, Nagy Anne-Laure
F. Hoffmann-La Roche Ltd, Pharmaceuticals Division, Safety and Technical Sciences, Synthesis and Process Research, Grenzacherstr. 124, CH-4070 Basel, Switzerland.
Org Biomol Chem. 2006 Feb 7;4(3):498-509. doi: 10.1039/b514147h. Epub 2005 Dec 22.
A practical, efficient and scalable formal total synthesis of (rac)- and (S)-camptothecin is described, which proceeds via the known DE ring building blocks 19 and (S)-19, respectively. The racemic synthesis starts from diethyl oxalate and uses straightforward carbonyl chemistry in order to generate the pyridone ring system. 19 was formed in 8.4% overall yield over 9 linear steps avoiding any chromatographic purification. The asymmetric version of this approach encompassed a diastereoselective Grignard addition to the enantiomerically pure alpha-ketoester 30 in order to generate the (S)-configured quaternary stereocenter. The auxiliary could be recycled in high yield and was successfully reused multiple times. The final steps paralleled the racemic approach. (S)-19 was thus prepared in 9.4% overall yield (er = 95 : 5) over 10 steps.
本文描述了一种实用、高效且可扩展的(外消旋)-和(S)-喜树碱的形式全合成方法,该方法分别通过已知的DE环结构单元19和(S)-19进行。外消旋合成从草酸二乙酯开始,并使用直接的羰基化学方法来生成吡啶酮环系统。在9个线性步骤中,19的总收率为8.4%,无需任何色谱纯化。该方法的不对称版本包括对映体纯的α-酮酯30进行非对映选择性格氏加成,以生成具有(S)构型的季碳立体中心。助剂可以高收率回收,并成功多次重复使用。最后几步与外消旋方法类似。因此,(S)-19在10步反应中以9.4%的总收率(对映体比例为95:5)制备得到。
