Xu Chu-Pei, Luo Shi-Peng, Wang Ai-E, Huang Pei-Qiang
Department of Chemistry, College of Chemistry and Chemical Engineering, Xiamen University, Xiamen, Fujian 361005, China.
Org Biomol Chem. 2014 May 14;12(18):2859-63. doi: 10.1039/c4ob00314d.
We demonstrated, for the first time, that on the basis of chemistry principles, the hexacyclic peptidyl alkaloid (−)-chaetominine (1) can be synthesized in a straightforward manner from L-Trp. The approach features the efficient generation of molecular complexity via a tandem C3/C14 syn-selective epoxidation (dr = 3:2)–annulative ring-opening reaction and a regioselective epimerization at C14. The successful production of (−)-chaetominine (1) from L-Trp could be helpful for revealing how the configuration of L-tryptophan becomes inverted in the biosynthetic pathway of (−)-chaetominine (1).
我们首次证明,基于化学原理,六环肽基生物碱(-)-链霉胺(1)可以从L-色氨酸直接合成。该方法的特点是通过串联C3/C14顺式选择性环氧化(dr = 3:2)-环化开环反应和C14处的区域选择性差向异构化有效地产生分子复杂性。从L-色氨酸成功制备(-)-链霉胺(1)可能有助于揭示L-色氨酸的构型在(-)-链霉胺(1)的生物合成途径中是如何反转的。
