Increasing nerve agent treatment efficacy by P-glycoprotein inhibition

Marloes J A Joosen; Stefanie M Vester; Jouk Hamelink; Steven D Klaassen; Roland M van den Berg

doi:10.1016/j.cbi.2016.06.012

Increasing nerve agent treatment efficacy by P-glycoprotein inhibition

Chem Biol Interact. 2016 Nov 25;259(Pt B):115-121. doi: 10.1016/j.cbi.2016.06.012. Epub 2016 Jun 7.

Authors

Marloes J A Joosen¹, Stefanie M Vester², Jouk Hamelink², Steven D Klaassen², Roland M van den Berg²

Affiliations

¹ TNO, CBRN Protection, P.O. Box 45, 2280 AA Rijswijk, The Netherlands. Electronic address: Marloes.joosen@tno.nl.
² TNO, CBRN Protection, P.O. Box 45, 2280 AA Rijswijk, The Netherlands.

PMID: 27287416
DOI: 10.1016/j.cbi.2016.06.012

Abstract

One of the shortcomings of current treatment of nerve agent poisoning is that not all drugs effectively penetrate the blood-brain barrier (BBB), whereas most nerve agents easily do. P-glycoprotein (Pgp) efflux transporters at the BBB may contribute to this aspect. It was previously shown that Pgp inhibition by tariquidar enhanced the efficacy of nerve agent treatment when administered as a pretreatment. In the present study soman-induced seizures were also substantially prevented when the animals were intravenously treated with tariquidar post-poisoning, in addition to HI-6 and atropine. In these animals, approximately twice as much AChE activity was present in their brain as compared to control rats. The finding that tariquidar did not affect distribution of soman to the brain indicates that the potentiating effects were a result of interactions of Pgp inhibition with drug distribution. In line with this, atropine appeared to be a substrate for Pgp in in vitro studies in a MDR1/MDCK cell model. This indicates that tariquidar might induce brain region specific effects on atropine distribution, which could contribute to the therapeutic efficacy increase found. Furthermore, the therapeutic enhancement by tariquidar was compared to that of the less specific and less potent Pgp inhibitor cyclosporine A. This compound appeared to induce a protective effect similar to tariquidar. In conclusion, treatment with a Pgp inhibitor resulted in enhanced therapeutic efficacy of HI-6 and atropine in a soman-induced seizure model in the rat. The mechanism underlying these effects should be further investigated. To that end, the potentiating effect of nerve agent treatment should be addressed against a broader range of nerve agents, for oximes and atropine separately, and for those at lower doses. In particular when efficacy against more nerve agents is shown, a Pgp inhibitor such as tariquidar might be a valid addition to nerve agent antidotes.

Keywords: Atropine; Oxime; Seizures; Soman; Tariquidar; p-Glycoprotein.

MeSH terms

ATP Binding Cassette Transporter, Subfamily B / antagonists & inhibitors
ATP Binding Cassette Transporter, Subfamily B / genetics
ATP Binding Cassette Transporter, Subfamily B / metabolism*
Acetylcholinesterase / blood
Acetylcholinesterase / metabolism
Animals
Atropine / metabolism
Atropine / therapeutic use
Blood-Brain Barrier / drug effects
Blood-Brain Barrier / metabolism
Brain / enzymology
Brain / metabolism
Dogs
Madin Darby Canine Kidney Cells
Male
Nerve Agents / poisoning*
Oximes / metabolism
Oximes / therapeutic use
Pyridinium Compounds / metabolism
Pyridinium Compounds / therapeutic use
Quinolines / pharmacology
Quinolines / therapeutic use
Rats
Rats, Wistar
Seizures / chemically induced
Seizures / drug therapy
Seizures / metabolism
Soman / toxicity
Substrate Specificity

Substances

ATP Binding Cassette Transporter, Subfamily B
Nerve Agents
Oximes
Pyridinium Compounds
Quinolines
Atropine
Soman
Acetylcholinesterase
asoxime chloride
tariquidar