Journal of the American Chemical Society p. 7481 - 7486 (1994)
Update date:2022-08-11
Topics:
Gu, Qu-Ming
Sih, Charles J.
Cyclic ADP-ribose (cADPR) is a naturally occurring cyclic nucleotide and a potent mediator of calcium mobilization in many mammalian tissues. Previous studies have shown that cADPR is synthesized from β-NAD+ via the scission of the nicotinamide-ribose linkage and cyclization by forming a new bond between the ribose and the nitrogen of the adenine ring. However, the position and stereochemistry of this newly formed linkage were not unequivocally determined. In this study we have established that cADPR has the anomeric carbon of the ribose attached onto the N1-nitrogen of the adenine nucleus via a β-N-glycosyl linkage. The structural assignment was made by correlating cADPR to N1-(5'-phosphoribosyl)AMP, a known intermediate of histidine biosynthesis. This was achieved by cleaving the pyrophosphate bond of cADPR under conditions (DMSO/tert-butoxide) not perturbing the integrity of the C-N glycosyl bond. Furthermore, cADPR was successfully synthesized by cyclization of N1-(5'-phosphoribosyl)ATP catalyzed by NAD+ pyrophosphorylase in an organic solvent-aqueous medium.
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