Collection of Czechoslovak Chemical Communications - digital archive 

Abstract

Guanine derivatives substituted at N⁷ with 4-R-benzyl groups (R = H, MeO, NO₂) have been evaluated in the regioselective N⁹-alkylation of guanine. Given the capricious removal of (substituted) benzyl groups from guanine derivatives and pent-4-enoylation of guaninium hydrochloride, an improved alternative approach has been elaborated consisting in the pent-4-enoylation and per-O-acetylation of guanosine (8), 4-nitrobenzylation at N⁷ followed by N-glycoside hydrolysis (10), N⁹-alkylation (13) and deprotection with sodium dithionite to afford the peptide nucleic acid building block tert-butyl [N²-(pent-4-enoyl)guanin-9-yl]- acetate (15) in 36% overall yield. This avoids N⁷ regioisomer formation, solubility problems and any chromatographic purification. A remarkable influence of the O- and/or N²-acyl groups on the stability of N-glycosidic bond and reactivity of 2-amino group was observed. The structure of a pyrimidine by-product 12 arising from the imidazole ring-opening of guaninium salt 4d in alkaline medium has been elucidated by 2D NMR.

Keywords: Guanine; Regioselective alkylation; Guanosine; Nucleoside analogues; Nucleosides; Purines; Peptide nucleic acids.

References: 62 live references.