Iwanaga_1994_Jpn.J.Pharmacol_66_317

Reference

Title : Characterization of acetylcholinesterase-inhibition by itopride - Iwanaga_1994_Jpn.J.Pharmacol_66_317
Author(s) : Iwanaga Y , Kimura T , Miyashita N , Morikawa K , Nagata O , Itoh Z , Kondo Y
Ref : Japanese Journal of Pharmacology , 66 :317 , 1994
Abstract :

Itopride is a gastroprokinetic benzamide derivative. This agent inhibited both electric eel acetylcholinesterase (AChE) and horse serum butyrylcholinesterase (BCHE). The IC50 of itopride with AChE (2.04 +/- 0.27 microM) was, however, 100-fold less than that with BCHE, whereas in the case of neostigmine with AChE (11.3 +/- 3.4 nM), it was 10-fold less. The recovery of AChE activity inhibited by 10(-7) M neostigmine was partial, but that inhibited by up to 3 x 10(-5) M itopride was complete when the reaction mixture was subjected to ultrafiltration. Double reciprocal plots of the experimental data showed that both Km and Vmax were affected by itopride, suggesting that the inhibition is a "mixed" type, although primarily being an uncompetitive one. The inhibitory effect of itopride on cholinesterase (ChE) activity in guinea pig gastrointestine was much weaker than that on pure AChE. However, in the presence of a low dose of diisopropyl fluorophosphate, just enough to inhibit BCHE but not AChE, the IC50s of itopride against ChE activities were found to be about 0.5 microM. In conclusion, itopride exerts reversible and a "mixed" type of inhibition preferably against AChE. The IC50 of itopride for electric eel and guinea pig gastrointestinal AChE inhibition was 200 times and 50 times as large as that of neostigmine, respectively.

PubMedSearch : Iwanaga_1994_Jpn.J.Pharmacol_66_317
PubMedID: 7869618

Related information

Inhibitor Itopride

Citations formats

Iwanaga Y, Kimura T, Miyashita N, Morikawa K, Nagata O, Itoh Z, Kondo Y (1994)
Characterization of acetylcholinesterase-inhibition by itopride
Japanese Journal of Pharmacology 66 :317

Iwanaga Y, Kimura T, Miyashita N, Morikawa K, Nagata O, Itoh Z, Kondo Y (1994)
Japanese Journal of Pharmacology 66 :317