Accessing 2-substituted piperidine iminosugars by organometallic addition/intramolecular reductive amination: aldehyde vs. nitrone route
Anno: 2017
Autori: Mirabella S., Fibbi G., Matassini C., Faggi C., Goti A., Cardona F.
Affiliazione autori: Univ Firenze, Dept Chem Ugo Schiff, Via Lastruccia 3-13, I-50019 Sesto Fiorentino, FI, Italy; CNR INO, Via N Carrara 1, Sesto Fiorentino, FI, Italy
Abstract: A dual synthetic strategy to afford 2-substituted trihydroxypiperidines is disclosed. The procedure involved Grignard addition either to a carbohydrate-derived aldehyde or to a nitrone derived thereof, and took advantage of an efficient ring-closure reductive amination strategy in the final cyclization step. An opposite diastereofacial preference was demonstrated in the nucleophilic attack to the two electrophiles, which would finally produce the same piperidine diastereoisomer as the major product. However, use of a suitable Lewis acid in the Grignard addition to the nitrone allowed reversing the selectivity, giving access to 2-substituted piperidines with the opposite configuration at C-2.
Giornale/Rivista: ORGANIC & BIOMOLECULAR CHEMISTRY
Volume: 15 (43) Da Pagina: 9121 A: 9126
Parole chiavi: PHARMACOLOGICAL CHAPERONE THERAPY; LYSOSOMAL BETA-GALACTOSIDASE; NUCLEOPHILIC ADDITIONS; GAUCHER-DISEASE; STORAGE DISORDERS; HIGHLY POTENT; INHIBITORS; DESIGN; G(M1)-GANGLIOSIDOSIS; GLUCOCEREBROSIDASEDOI: 10.1039/c7ob01848gCitazioni: 10dati da “WEB OF SCIENCE” (of Thomson Reuters) aggiornati al: 2024-04-14Riferimenti tratti da Isi Web of Knowledge: (solo abbonati) Link per visualizzare la scheda su IsiWeb: Clicca quiLink per visualizzare la citazioni su IsiWeb: Clicca qui