Title : Optimal Pre-treatment for Acute Exposure to the Organophosphate Dicrotophos - Lorke_2017_Curr.Pharm.Des_23_3432 |
Author(s) : Lorke DE , Nurulain SM , Hasan MY , Kuca K , Petroianu GA |
Ref : Curr Pharm Des , 23 :3432 , 2017 |
Abstract :
BACKGROUND: Reversible cholinesterase inhibitors, when given prophylactically before exposure to organophosphates, are able to decrease organophosphate-induced mortality. However, the efficacy of pyridostigmine, the only pre-treatment substance approved by the US Federal Drug Administration, is unsatisfactory. METHODS: In search of a better prophylactic compound, we determined in vivo the protection conferred by five cholinesterase inhibitors (ranitidine, physostigmine, tacrine, K-27 and pyridostigmine), which were administered in equitoxic dosage (1/4 of LD01) 30 minutes before exposure to the organophosphate dicrotophos. Efficacy was measured in rats by Cox analysis calculating the relative risk of death (RR), RR being 1 for the reference group which received dicrotophos and no prophylaxis. RESULTS: K-27 (RR=0.06), physostigmine (RR=0.15), pyridostigmine (RR=0.22) and tacrine (RR=0.28) significantly (p <= 0.05) reduced dicrotophos-induced mortality in comparison to the reference group (dicrotophos without pre-treatment), whereas ranitidine (RR=0.86) had no significant influence. The experimental oxime K-27, when given before dicrotophos exposure, conferred the best in vivo protection. This was significantly (p <= 0.05) more efficacious than pre-treatment with any other tested compound. The differences in efficacy between the second best compound, physostigmine, and the less efficacious substances (tacrine and pyridostigmine) were also statistically significant. CONCLUSION: These data indicate that K-27 can be considered a very efficacious prophylactic agent for organophosphate exposure. |
PubMedSearch : Lorke_2017_Curr.Pharm.Des_23_3432 |
PubMedID: 27799040 |
Lorke DE, Nurulain SM, Hasan MY, Kuca K, Petroianu GA (2017)
Optimal Pre-treatment for Acute Exposure to the Organophosphate Dicrotophos
Curr Pharm Des
23 :3432
Lorke DE, Nurulain SM, Hasan MY, Kuca K, Petroianu GA (2017)
Curr Pharm Des
23 :3432