Chiral metabolism of propafenone in rat hepatic microsomes treated with two inducers

doi:https://doi.org/10.3748/wjg.v7.i6.830

Chiral metabolism of propafenone in rat hepatic microsomes treated with two inducers

Quan Zhou-2001-01-01-World Journal of Gastroenterology

TL;DRAbstract

CYP1A subfamily(induced by BNF) and CYP3A4 (induced by DEX) have pronounced contribution to propafenone N-desalkylation which exhibited stereoselectivity depending on substrate concentration. The molecular base for this phenomenon is the stereoselectivity in affinity of substrate to the enzyme activity centers instead of at the catalyzing sites.

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CYP1A subfamily(induced by BNF) and CYP3A4 (induced by DEX) have pronounced contribution to propafenone N-desalkylation which exhibited stereoselectivity depending on substrate concentration. The molecular base for this phenomenon is the stereoselectivity in affinity of substrate to the enzyme activity centers instead of at the catalyzing sites.

Keywords

PropafenoneStereoselectivityMicrosomeMetaboliteMetabolismChemistryEnantiomerSubstrate (aquarium)

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