Increasing oxime efficacy by blood-brain barrier modulation

article





Joosen, M.J.A.

Schans, M.J. van der

Dijk, C.G.M. van

Kuijpers, W.C.

Wortelboer, H.M.

Helden, H.P.M. van
One of the shortcomings of current treatment of nerve agent poisoning is that oximes hardly penetrate the blood-brain barrier (BBB), whereas nerve agents easily do. Increasing the concentration of oximes in the brain, would therefore provide an attractive approach to improve medical countermeasures. An explanation for limited penetration might be that oximes are substrates for the active P-glycoprotein (Pgp) efflux transporter located in the BBB.Using quantitative brain microdialysis in rats, the effect of i.v. injected tariquidar, a non-competitive, specific Pgp-inhibitor, on HI-6 levels in blood and brain was investigated. It appeared that tariquidar enhanced HI-6 levels in the brain approximately 2-fold during the first hour after HI-6 administration, whereas plasma levels did not differ between the treatment groups. A subsequent proof-of-concept study in rats showed that soman-induced seizures and convulsions were prevented almost completely when they were, in addition to HI-6 and atropine, pretreated with tariquidar. Moreover, twice as much AChE activity was present in their brains as compared to control rats.These results in rats indicate that modulation of the BBB by a drug like tariquidar, which is non-toxic by itself, is of great value in enhancing the efficacy of oximes. © 2011 Elsevier Ireland Ltd.
Topics




































HI6Nerve agentP-glycoproteinSeizuresTariquidar1 (4 carbamoylpyridinio) 1' (2 hydroxyiminomethylpyridinio)dimethyl etherAcetylcholinesteraseAtropineTariquidarAnimal experimentAnimal modelArticleBlood brain barrierBlood levelBrain blood volumeControlled studyConvulsionDrug effectDrug efficacyDrug intoxicationDrug penetrationMaleMicrodialysisModulationNerve agent poisoningNonhumanPriority journalQuantitative analysisRatSeizureRattus1 (4 carbamoylpyridinio) 1' (2 hydroxyiminomethylpyridinio)dimethyl ether, 34433-31-3Acetylcholinesterase, 9000-81-1Atropine, 51-55-8, 55-48-1Tariquidar, 206873-63-4Tradenames: hi 6, TNO; xr 9576, avaantManufacturers: TNO; avaant
TNO Identifier
435959
Repository link
https://resolver.tno.nl/uuid:13c5876c-1cda-4bf6-9d49-2a09a93cf9c9
DOI
https://dx.doi.org/10.1016/j.toxlet.2011.05.231
ISSN
0378-4274
Source
Toxicology Letters, 206(1), pp. 67-71.
Pages
67-71
Files
To receive the publication files, please send an e-mail request to TNO Repository.