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Vol. 58, Issue 3, 577-583, September 2000
Medical Research Council Toxicology Unit, University of
Leicester, Leicester, United Kingdom
We describe here the purification and identification of a
previously unrecognized target for organophosphorus compounds. The target, acylpeptide hydrolase, was isolated as a
tritiated-diisopropylfluorophosphate-reactive protein from porcine
brain and purified to homogeneity using a combination of ion-exchange
and gel-filtration chromatography. Biochemical characterization and
internal sequence analysis confirmed identity. Acylpeptide hydrolase
was found to be potently inhibited by the organophosphorus compounds
chlorpyrifosmethyl oxon, dichlorvos, and diisopropylfluorophosphate
(20-min IC50 values of 18.3 ± 2.0, 118.7 ± 9.7, and 22.5 ± 1.2 nM, respectively). The in vitro sensitivity of
acylpeptide hydrolase toward these compounds is between six and ten
times greater than that of acetylcholinesterase (AChE), making it a
target of pharmacological and toxicological significance. We show that,
in vivo, acylpeptide hydrolase is significantly more sensitive than
AChE to inhibition by dichlorvos and that the inhibition is more
prolonged after a single dose of inhibitor. Furthermore, using
dichlorvos as a progressive inhibitor, it was possible to show that
acylpeptide hydrolase is the only enzyme in the brain capable of
hydrolyzing the substrate
N-acetyl-alanyl-p-nitroanilide. A
concentration of 154 ± 27 pmol of acylpeptide hydrolase/gram of
fresh rat brain was also deduced by specific labeling with tritiated-diisopropylfluorophosphate. We also suggest that, by comparison of structure-activity relationships, acylpeptide hydrolase may be the target for the cognitive-enhancing effects of certain organophosphorus compounds. Acylpeptide hydrolase cleaves
N
-acylated amino acids from small
peptides and may be involved in regulation of neuropeptide turnover,
which provides a new and plausible mechanism for its proposed cognitive
enhancement effect.
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