Sequential C–H Arylation and Enantioselective Hydrogenation Enables Ideal Asymmetric Entry to the Indenopiperidine Core of an 11β-HSD-1 Inhibitor

Xudong Wei,Bo Qu,Xingzhong Zeng,Jolaine Savoie,Keith R. Fandrick,Jean-Nicolas Desrosiers,Sergei Tcyrulnikov,Maurice A. Marsini,Frederic G. Buono,Zhibin Li,Bing-Shiou Yang,Wenjun Tang,Nizar Haddad,Osvaldo Gutierrez,Jun Wang,Heewon Lee,Shengli Ma,Scot Campbell,Jon C. Lorenz,Matthias Eckhardt,Frank Himmelsbach,Stefan Peters,Nitinchandra D. Patel,Zhulin Tan,Nathan K. Yee,Jinhua J. Song,Frank Roschangar,Marisa C. Kozlowski,Chris H. Senanayake

Sequential C–H Arylation and Enantioselective Hydrogenation Enables Ideal Asymmetric Entry to the Indenopiperidine Core of an 11β-HSD-1 Inhibitor

2016

A concise asymmetric synthesis of an 11β-HSD-1 inhibitor has been achieved using inexpensive starting materials with excellent step-economy at low catalyst loadings. The catalytic enantioselective total synthesis of 1 was accomplished in 7 steps and 38% overall yield aided by the development of an innovative, sequential strategy involving Pd-catalyzed pyridinium C–H arylation and Ir-catalyzed asymmetric hydrogenation of the resulting fused tricyclic indenopyridinium salt highlighted by the use of a unique P,N-ligand (MeO-BoQPhos) with 1000 ppm of [Ir(COD)Cl]2.

Keywords:

Total synthesis
Enantioselective synthesis
Organic chemistry
Catalysis
Tricyclic
Inorganic chemistry
Pyridinium
Chemistry
Asymmetric hydrogenation
Iridium
Stereoisomerism
Palladium

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