TY - JOUR

T1 - Total Synthesis of (-)-Antroalbocin A Enabled by a Strain Release-Controlled Photochemical 1,3-Acyl Shift

AU - Siekmeyer, Björn

AU - Lübken, Dennis

AU - Bajerke, Kevin

AU - Bernhardt, Bastian

AU - Schreiner, Peter R.

AU - Kalesse, Markus

PY - 2022/8/12

Y1 - 2022/8/12

N2 - The first bioinspired, enantioselective, and protecting group free total synthesis of the antibacterial sesquiterpenoid (-)-antroalbocin A (1) has been achieved in 12 steps (5.4% overall yield) from dimedone. An organocatalytic Robinson annulation gave rapid access to the tricyclic enone (19) as starting material for the photochemical domino process of deconjugation and sigmatropic 1,3-acyl shift. Computational data of this process indicate that the 1,3-acyl shift benefits from the highly strained 1,3-enone 8. The transformation of 8 to its bridged isomer 5 is exergonic and, therefore, enables an increased conversion compared to unstrained substrates.

AB - The first bioinspired, enantioselective, and protecting group free total synthesis of the antibacterial sesquiterpenoid (-)-antroalbocin A (1) has been achieved in 12 steps (5.4% overall yield) from dimedone. An organocatalytic Robinson annulation gave rapid access to the tricyclic enone (19) as starting material for the photochemical domino process of deconjugation and sigmatropic 1,3-acyl shift. Computational data of this process indicate that the 1,3-acyl shift benefits from the highly strained 1,3-enone 8. The transformation of 8 to its bridged isomer 5 is exergonic and, therefore, enables an increased conversion compared to unstrained substrates.

UR - http://www.scopus.com/inward/record.url?scp=85135999138&partnerID=8YFLogxK

U2 - 10.26434/chemrxiv-2021-3pd4x

DO - 10.26434/chemrxiv-2021-3pd4x

M3 - Article

C2 - 35912985

AN - SCOPUS:85135999138

VL - 24

SP - 5812

EP - 5816

JO - Organic letters

JF - Organic letters

SN - 1523-7060

IS - 31

ER -