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Abstract
We designed novel Ca2+-mobilizing purine nucleotides, cyclic ADP-carbocycl-icribose 4, and its inosine congener 5, and C-glycosidic adenophostin A 6. In the synthesis of cADPR analogs, the intramolecular condensation to form the pyrophosphate linkage should be the key step. We developed an efficient method for forming such an intramolecular pyrophosphate linkage by the activation of the phenylthiophosphate group with I2 or AgNO3. Using this method, we achieved to synthesize the target compounds 4 and 5. The synthesis of C-glycosidic analog 6 of adenophostin A was achieved using a temporary silicon-tethered radical coupling reaction for constructing (3′α, 1″α)-C-glycosi-dic structure as the key step.
ACKNOWLEDGEMENT
We are grateful to Ms. T. Iizawa and Drs. M. Takahashi and H. Hotoda, Sankyou Co. Ltd, for the biological evaluation, and to Dr. A. M. Riley and Prof. B. V. L. Potter, University of Bath, for useful discussions.