54596-01-9Relevant academic research and scientific papers
Efficient synthesis of a highly selective NPY-5 receptor antagonist: A drug candidate for the treatment of obesity
Itoh, Takahiro,Kato, Shinji,Nonoyama, Nobuaki,Wada, Toshihiro,Maeda, Kenji,Mase, Toshiaki,Zhao, Matthew M.,Song, Jake Z.,Tschaen, David M.,McNamara, James M.
, p. 822 - 828 (2012/12/22)
A concise and practical synthesis of highly selective NPY-5 receptor antagonist 1 is described. The animopyrazine intermediate 3 was synthesized via either monobromination of aminopyrazine or palladium-catalyzed regioselective debromination of dibromopyrazine followed by an efficient Suzuki-Miyaura coupling. For the preparation of the spirolactone piperidine 2, significantly improved yield was achieved by using a combination of n-BuMgCl and n-BuLi. This protocol also dramatically increased the thermal stability of the aryllithium intermediate and eliminated the requirement for costly cryogenic conditions. The union of the spirolactone piperidine 2 and aminopyrazine 3 via a carbonyl group was accomplished using phenyl chloroformate delivering the target molecule in high yield.
METHOD OF SUBSTITUENT INTRODUCTION THROUGH HALOGEN-METAL EXCHANGE REACTION
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Page/Page column 15, (2010/02/10)
A method of exchanging a halogen atom of a halide, which has a group containing an acidic proton and in which one or more halogen atom(s) is/are substituted on a carbon atom of the carbon-carbon double bond, with a metal atom by halogen-metal-exchange reaction and introducing an electrophilic reagent into the carbon atom to which the metal atom is attached. The above method is an industrially excellent method of introducing a substituent by halogen-metal exchange reaction.
Process for making spiro isobenzofuranone compounds
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, (2008/06/13)
This invention relates to a process for making spiro isobenzofuranone compounds by coupling of an aminopyrazine fragment with a spirolactone piece.
