Development of a cyclosporin A derivative with excellent anti-hepatitis C virus potency |
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| Authors: | Jiping Fu Christopher Becker Li Cao Michael Capparelli Regis Denay Roger Fujimoto Yu Gai Zhaobo Gao Christian Guenat Subramanian Karur Hongyong Kim Weikuan Li Xiaolin Li Wei Li Thomas Lochmann Amy Lu Peichao Lu Alexandre Luneau Fabrice Gallou |
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| Institution: | 1. Novartis Institutes for BioMedical Research, 5300 Chiron way, Emeryville, CA 94608, United States;2. Novartis Institutes for BioMedical Research, Novartis Campus, CH-4056 Basel, Switzerland;3. Chemical and Analytical Development, CH-4002 Basel, Switzerland;4. Chemical & Analytical Development, Suzhou Novartis Pharma Technology Company Limited, Changshu, Jiangsu 215537, China |
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| Abstract: | Synthetic modification of cyclosporin A at P3-P4 positions led to the discovery of NIM258, a next generation cyclophilin inhibitor with excellent anti-hepatitis C virus potency, with decreased transporter inhibition, and pharmacokinetics suitable for coadministration with other drugs. Herein is disclosed the evolution of the synthetic strategy to from the original medicinal chemistry route, designed for late diversification, to a convergent and robust development synthesis. The chiral centers in the P4 fragment were constructed by an asymmetric chelated Claisen rearrangement in the presence of quinidine as the chiral ligand. Identification of advanced crystalline intermediates enabled practical supply of key intermediates. Finally, macrocyclization was carried out at 10% weight concentration by a general and unconventional “slow release” concept. |
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| Keywords: | Cyclosporin A derivative Hepatitis C virus Cyclophilin inhibitor |
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