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Hydrazine and amphetamine binding to amine oxidases: old drugs with new prospects.

Journal of neural transmission (Vienna, Austria : 1996) (2007-04-05)
P Knowles, C Kurtis, J Murray, C Saysell, W Tambyrajah, C Wilmot, M McPherson, S Phillips, D Dooley, D Brown, M Rogers, M Mure
RÉSUMÉ

Tranylcypromine (TCP), an amphetamine, is a reversible inhibitor of copper-containing amine oxidases. We have solved the structure of the complex of TCP with the amine oxidase from E. coli (ECAO) and shown that only the (+)-enantiomer of TCP binds. Kinetic studies on 2-phenylethylamine and TCP binding to wild-type ECAO and mutational variants fully support the model in which binding of the protonated amine is the first step in the catalytic cycle. Hydrazines are irreversible inhibitors of copper-containing amine oxidases. Binding of hydrazines leads to an adduct ("Adduct 1") with a chromophore at 430 nm which converts at higher pH to another adduct ("Adduct 2") with a chromophore at 520 nm. We have determined the structures of Adduct 1 and 2 for 2-hydrazinopyridine reacted with ECAO. It has been found that Adduct 1 corresponds to the hydrazone and azo tautomers whilst Adduct 2 corresponds to the azo tautomer coordinated to the active site copper. The implications of these results in developing more specific drugs are discussed.

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Sigma-Aldrich
2-Hydrazinopyridine, 97%