Development of a Generic Stereocontrolled Pathway to Fully Hydroxylated Spirocarbocyclic Nucleosides as a Prelude to RNA Targeting

Ryan E. Hartung; Leo A. Paquette

doi:10.1055/s-2005-918472

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Synthesis 2005(19): 3209-3218
DOI: 10.1055/s-2005-918472

PAPER

Development of a Generic Stereocontrolled Pathway to Fully Hydroxylated Spirocarbocyclic Nucleosides as a Prelude to RNA Targeting

Ryan E. Hartung, Leo A. Paquette*
Evans Chemical Laboratories, The Ohio State University, Columbus, Ohio 43210, USA
Fax: +1(614)2921685; e-Mail: paquette.1@osu.edu;

Further Information

Publication History

Received 12 February 2005
Publication Date:
17 November 2005 (online)

Abstract
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Abstract

Osmylation of the enantiopure conjugated enones 4 and 15 proceeded predominantly or exclusively from the α-face to give the 2′,3′-diols 6 and 16. Ensuing conversion into the acetonide allowed for sequential stereocontrolled reduction with L-Selectride, and esterification with triflic anhydride was utilized to form triflates 11 and 19. The heightened electrophilicity of these intermediates made possible S_N2 displacements with several nucleobases as promoted with potassium hydride in N,N-dimethylformamide at room temperature. Suitable deprotection measures led to the targeted compounds.

Key words

spirocarbocycles - nucleosides - triflate displacements - osmylation - acetonides

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