Zhang Qi, Rinkel Jan, Goldfuss Bernd, Dickschat Jeroen S, Tiefenbacher Konrad
Department of Chemistry, University of Basel, BPR 1096, Postfach 3350, Mattenstrasse 24a, 4002 Basel, Switzerland.
Kekulé-Institute of Organic Chemistry and Biochemistry, University of Bonn, Gerhard-Domagk-Straße 1, 53121 Bonn, Germany.
Nat Catal. 2018 Aug;1(8):609-615. doi: 10.1038/s41929-018-0115-4. Epub 2018 Jul 30.
Terpenes constitute the largest class of natural products and serve as an important source for medicinal treatments. Despite constant progress in chemical synthesis, the construction of complex polycyclic sesqui- and diterpene scaffolds remains challenging. Natural cyclase enzymes, however, are able to form the whole variety of terpene structures from just a handful of linear precursors. Man-made catalysts able to mimic such natural enzymes are lacking. Here, we describe the examples of sesquiterpene cyclisations inside an enzyme-mimicking supramolecular catalyst. This strategy allowed the formation of the tricyclic sesquiterpene isolongifolene in only four steps. The mechanism of the catalysed cyclisation reaction was elucidated using C-labelling studies and DFT calculations.
萜类化合物是最大的天然产物类别,也是药物治疗的重要来源。尽管化学合成不断取得进展,但构建复杂的多环倍半萜和二萜支架仍然具有挑战性。然而,天然环化酶能够仅从少数几种线性前体形成各种各样的萜类结构。目前还缺乏能够模拟这种天然酶的人造催化剂。在此,我们描述了在一种模拟酶的超分子催化剂中进行倍半萜环化反应的实例。该策略仅通过四个步骤就实现了三环倍半萜异长叶烯的合成。通过碳标记研究和密度泛函理论计算阐明了催化环化反应的机理。
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