Synthesis and properties of second-generation 2-5A-antisense chimeras with enhanced resistance to exonucleases.

In order to stabilize 2-5A-antisense chimeras to exonucleases, we have synthesized chimeric oligonucleotides in which the last phosphodiester bond at the 3‘-terminus of the antisense domain was inverted from the usual 3‘,5‘-linkage to a 3‘,3‘-linkage. The preparation of such analogues was accomplished through standard phosphoramidite chemistry with the use of a controlled pore glass solid support with a nucleoside attached through its 5‘-hydroxyl, thereby permitting elongation at the 3‘-hydroxyl. The structures of such terminally inverted linkage chimeras of the general formula pA4-[pBu]2-(pdNn3‘-3‘dN) were corroborated by a combination of snake venom phosphodiesterase digestion in the presence or absence of bacterial alkaline phosphatase. Most characteristically, the presence of the 3‘-terminal-inverted phosphodiester linkage produced an unnatural dinucleotide of general composition dN3‘p3‘dM. These structures could be confirmed by independent synthesis and fast atom bombardment mass spectroscopy (FAB). ...