Journal
CHINESE JOURNAL OF CHEMISTRY
Volume 39, Issue 1, Pages 137-142Publisher
WILEY-V C H VERLAG GMBH
DOI: 10.1002/cjoc.202000460
Keywords
Protecting‐ group‐ free; Total synthesis; Spirooxindole; Alkaloid; Asymmetric synthesis
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Funding
- SZSTI [JCYJ20170817110515599, KQTD20150717103157174]
- National Natural Science Foundation of China [21772082, 21971104]
- Guangdong Innovative Program [2019BT02Y335]
- Guangdong Provincial Key Laboratory of Catalysis [2020B121201002]
- Shenzhen Key Laboratory of Small Molecule Drug Discovery and Synthesis [ZDSYS20190902093215877]
- Shenzhen Nobel Prize Scientists Laboratory Project [C17783101]
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This study presents a concise, protecting-group-free total synthesis of cabucine oxindole A, a putative natural spirooxindole alkaloid, and investigates the biological activity of its synthetic intermediates.
Main observation and conclusion Owing to their challenging structures and promising biological profiles, spirooxindole alkaloids have long attracted much attention from the synthetic community. Herein, we wish to describe a concise, protecting-group-free total synthesis of cabucine oxindole A, a putative natural spirooxindole alkaloid and a possible biosynthetic congener of cabucine and palmirine. Key transformations of our approach include a one-step, organocatalytic and enantioselective construction of the spiro[pyrrolidine-3,3'-oxindole] moiety and a Korte rearrangement to furnish the final dihydropyran motif. Biological investigation of 1 and its synthetic intermediates revealed lactone 2 as a mild MOLT-4 and MCF7 cell line inhibitor.
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