Synthese eines 1,2-trans-konfigurierten, äquatorialen Glycosyl-phosphonat-Analogen von D-myo-Inositol-1,4,5-trisphosphat

Synthesis of a 1,2-trans-Configurated, Equatorial Glycosylphosphonate Analogue of D -myo-Inositol 1,4,5-Trisphosphate The diphosphonate analogue 3 of D -myo-inositol 1,4,5-trisphosphate ( 1 ), a 1,2-trans-configurated, equatorial glycosylphosphonate, was synthesized and characterized as its hexasodium salt 3a . In a first approach, the silylated galactal 4 (Scheme 1) was transformed into the oxirane 5 and hence, by treatment with Me₃SiP(OMe)₂, into a mixture of the glycosylphosphonate 6 and its silyl ether 7 . This mixture was desilylated and then treated with acetone and FeCl₃ to yield 8 and 9 (64 and 22%, resp., from 4 ). In a second approach, the acetates 11/12 (Scheme 2) were treated with P(OMe)₃/Me₃SiOTf in MeCN to afford the anomeric glycosylphosphonates 16/17 (1:1, 60%), while the trichloroacetimidate 10 gave mostly the αD -anomer 16 . The αD -anomer 20 was obtained from 12 and P(OPh)₃. The highest yield of a β-D phosphonate was realized by treating 12 with the cyclic phosphite 15 (→ 18/19 , 40% each). The β-D -phosphonate 17 was debenzylated (→ 21 ) and protected to give 8 . Transformation of 8 into the bromide 22 (43%) proved difficult due to the facile demethylation of thephosphonate, and was best followed by treatment of the crude product with CH₂N₂ and 2,2-dimethoxyporpane. Phosphorylation of 22 yielded 41% of the (dimethoxyphosphoryl)phosphate 23 . The conditions of the Arbuzov reaction slowly converted the bromide 23 into the bis(phosphoryl)phosphate 24 (69%), which was then deprotected. The resulting 3 was purified via the ammonium salt and transformed into 3a (72%).