Total Synthesis of the Dihydrooxepine-Spiroisoxazoline Natural Product Psammaplysin A | Zendy

Jan Paciorek | Zendy; Denis Höfler | Zendy; Kevin Rafael Sokol | Zendy; Klaus Wurst | Zendy; Thomas Magauer | Zendy

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Total Synthesis of the Dihydrooxepine-Spiroisoxazoline Natural Product Psammaplysin A

Author(s) -

Jan Paciorek,

Denis Höfler,

Kevin Rafael Sokol,

Klaus Wurst,

Thomas Magauer

Publication year - 2022

Publication title -

journal of the american chemical society

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 7.115

H-Index - 612

eISSN - 1520-5126

pISSN - 0002-7863

DOI - 10.1021/jacs.2c10010

Subject(s) - chemistry , regioselectivity , total synthesis , natural product , ring (chemistry) , stereochemistry , sequence (biology) , combinatorial chemistry , organic chemistry , catalysis , biochemistry

We report a general synthetic entry to dihydrooxepine-spiroisoxazoline (DOSI) natural products that culminated in the first racemic total synthesis of psammaplysin A. For the synthesis of the unique spirocyclic fragment we employed a strategy that features two key transformations: (1) a diastereoselective Henry reaction/cyclization sequence to access the C7 hydroxylated isoxazoline scaffold in one step and (2) a regioselective Baeyer-Villiger ring expansion to install the fully substituted dihydrooxepine and avoid the risk of a previously observed oxepine-arene oxide rearrangement. The overall synthesis proceeds in 13 steps from an inexpensive starting material.

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