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Adenosine triphosphate -competitive kinase inhibitor

The synthesis of the two diastereoisomers of P -l-(2-nitrophenyl)ethyl adenosine S -lri-phosphate (91) has been achieved using resolved (R)- and (5)-l-(2-nilroidienyl)ethanol. The alcohols were converted to (R)- and (5)-l-(2-nitrophenyl)ethyl phosphates by phosphitylation with N,)V-diisopropyl-fi(s-(2-cyanoethyl)phosphoramidite (92) and subsequent oxidation with 3-chlorobenzoic acid. Each of the monophosphates was activated with carbonyidiimidazole and condensed with adenosine diphosphate to give the desired triphosphate. These ATP analogues can be used for the rapid release (by flash photolysis) of ATP in biological systems. The 8-azido-3 -0-anthraniloyl derivatives of 2 -dADP (93) and 2 -dATP (94) have been prepared in seven steps from 8-azido-2 -deoxyadenosine. These compounds are of interest as fluorescent and photoactivatable probes for the nucleotide binding site of kinases and cyclases. In particular, (94) was shown to be a competitive inhibitor of Bordetella pertussis adenylate cyclase and the observed K- (74 pM) was close to tiiat predicted from the K- value of 3 -0-anthraniloyl-2 -dATP. ... [Pg.228]


See other pages where Adenosine triphosphate -competitive kinase inhibitor is mentioned: [Pg.20]    [Pg.17]    [Pg.208]    [Pg.168]    [Pg.701]    [Pg.212]    [Pg.2375]    [Pg.411]    [Pg.139]    [Pg.123]    [Pg.180]    [Pg.423]    [Pg.487]    [Pg.150]    [Pg.2262]    [Pg.123]    [Pg.171]   
See also in sourсe #XX -- [ Pg.19 ]




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