受天然产物启发而合成的四氢吡喃化合物库产生有丝分裂调节剂，可协同靶向 CSE1L 和微管蛋白。

A natural product inspired tetrahydropyran collection yields mitosis modulators that synergistically target CSE1L and tubulin.

机构信息

Max-Planck-Institut für molekulare Physiologie, Abt. Chemische Biologie, Dortmund, Germany.

出版信息

Angew Chem Int Ed Engl. 2013 Jan 2;52(1):410-4. doi: 10.1002/anie.201205728. Epub 2012 Oct 18.

DOI:10.1002/anie.201205728

Abstract

A Prins cyclization between a polymer-bound aldehyde and a homoallylic alcohol served as the key step in the synthesis of tetrahydropyran derivatives. A phenotypic screen led to the identification of compounds that inhibit mitosis (as seen by the accumulation of round cells with condensed DNA and membrane blebs). These compounds were termed tubulexins as they target the CSE1L protein and the vinca alkaloid binding site of tubulin.

摘要

在四氢吡喃衍生物的合成中，聚合物结合的醛和偕丙醇之间的Prins 环化反应是关键步骤。表型筛选导致了抑制有丝分裂的化合物的鉴定（如圆细胞中 DNA 凝聚和细胞膜泡的积累）。这些化合物被称为 tubulexins，因为它们靶向 CSE1L 蛋白和微管蛋白的长春碱结合位点。

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受天然产物启发而合成的四氢吡喃化合物库产生有丝分裂调节剂，可协同靶向 CSE1L 和微管蛋白。

A natural product inspired tetrahydropyran collection yields mitosis modulators that synergistically target CSE1L and tubulin.

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