TY - JOUR
T1 - Enantioselective construction of nitrogen-substituted quaternary carbon centers adjacent to the carbonyl group in the cyclohexane ring
T2 - first asymmetric synthesis of anesthetic (S)-ketamine with high selectivity
AU - Yokoyama, Reiko
AU - Matsumoto, Satoshi
AU - Nomura, Satoshi
AU - Higaki, Takafumi
AU - Yokoyama, Takeshi
AU - Kiyooka, Syun ichi
N1 - Funding Information:
This work was supported by Grand-in-Aid for Scientific Research (C) of Japan Society for the Promotion of Science. We are grateful to Messrs. Motoo Shiro and Mikio Yamasaki of X-ray Research Laboratory and Application Laboratory, Rigaku Corporation for X-ray crystallographic measurement.
Copyright:
Copyright 2009 Elsevier B.V., All rights reserved.
PY - 2009/7/4
Y1 - 2009/7/4
N2 - Enantioselective construction of nitrogen-substituted quaternary carbon centers adjacent to the carbonyl group in the cyclohexane ring was performed with respect to the asymmetric synthesis of anesthetic (S)-ketamine 1. Diastereoselective nucleophilic 1,2-addition reaction of phenyllithium to α-ketoxime-ether acetal 9 bearing chiral auxiliary on the α-carbonyl function gave benzyloxyamine 11 major in 83% yield with 82% de, which was converted to the corresponding amino ketone 12. However, the reaction of 2-chlorophenyllithium did not work in which this route was unavailable for the synthesis of 1. Then, an alternative strategy directed toward 1, starting with a compound having 2-chlorophenyl groups in advance, was designed in which the chiral quaternary carbon center bearing a nitrogen atom in the ring is created by the enantioselective reduction of the atropisomeric intermediate ketone 18, and the sequential allyl cyanate-to-isocyanate rearrangement with complete 1,3-chirality transfer. The first asymmetric synthesis of 1 with excellent selectivity (>99% ee) was accomplished by a short path according to the strategy.
AB - Enantioselective construction of nitrogen-substituted quaternary carbon centers adjacent to the carbonyl group in the cyclohexane ring was performed with respect to the asymmetric synthesis of anesthetic (S)-ketamine 1. Diastereoselective nucleophilic 1,2-addition reaction of phenyllithium to α-ketoxime-ether acetal 9 bearing chiral auxiliary on the α-carbonyl function gave benzyloxyamine 11 major in 83% yield with 82% de, which was converted to the corresponding amino ketone 12. However, the reaction of 2-chlorophenyllithium did not work in which this route was unavailable for the synthesis of 1. Then, an alternative strategy directed toward 1, starting with a compound having 2-chlorophenyl groups in advance, was designed in which the chiral quaternary carbon center bearing a nitrogen atom in the ring is created by the enantioselective reduction of the atropisomeric intermediate ketone 18, and the sequential allyl cyanate-to-isocyanate rearrangement with complete 1,3-chirality transfer. The first asymmetric synthesis of 1 with excellent selectivity (>99% ee) was accomplished by a short path according to the strategy.
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U2 - 10.1016/j.tet.2009.05.004
DO - 10.1016/j.tet.2009.05.004
M3 - Article
AN - SCOPUS:66149114030
SN - 0040-4020
VL - 65
SP - 5181
EP - 5191
JO - Tetrahedron
JF - Tetrahedron
IS - 27
ER -