Dose-response assessment of tariquidar and elacridar and regional quantification of P-glycoprotein inhibition at the rat blood-brain barrier using (R)-[11C]verapamil PET

Kuntner, Claudia; Bankstahl, Jens P.; Bankstahl, Marion; Stanek, Johann; Wanek, Thomas; Stundner, Gloria; Karch, Rudolf; Brauner, Rebecca; Meier, Martin; Ding, Xiao‐Qi; Müller, Markus; Löscher, Wolfgang; Langer, Oliver

doi:10.1007/s00259-009-1332-5

Cited by 102 publications

(156 citation statements)

References 25 publications

(51 reference statements)

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“…Both clinical and preclinical studies have reported small, but significant, regional differences in increasing concentrations of the P-gp substrate radiotracer (R)-11 Cverapamil after P-gp inhibition (16,34,35). In contrast, effects of tariquidar on Q out and V br were similar in all brain regions studied in the present study (Table 4).…”

Section: Discussioncontrasting

confidence: 50%

“…Tariquidar, 3 (n 5 6) or 15 (n 5 23) mgÁkg 21 , was administered as an infusion over 10 min, starting 20 min before the second scan. The tariquidar doses were based on studies showing that 15 mg/kg results in complete inhibition of P-gp and 3 mg/kg is close to the median effective dose (16). The lower dose of 3 mg/kg can also be used in humans and could potentially allow for the translation of results between preclinical and clinical studies.…”

Section: Pet Experimentsmentioning

confidence: 99%

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Altered GABA_A Receptor Density and Unaltered Blood–Brain Barrier Transport in a Kainate Model of Epilepsy: An In Vivo Study Using ¹¹C-Flumazenil and PET

et al. 2012

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The aim of the present study was to investigate if flumazenil blood-brain barrier transport and binding to the benzodiazepine site on the g-aminobutyric acid A (GABA A ) receptor complex is altered in an experimental model of epilepsy and subsequently to study if changes in P-glycoprotein (P-gp)-mediated efflux of flumazenil at the blood-brain barrier may confound interpretation of 11 C-flumazenil PET in epilepsy. Methods: The transport of flumazenil across the blood-brain barrier and the binding to the benzodiazepine site on the GABA A receptors in 5 different brain regions was studied and compared between controls and kainate-treated rats, a model of temporal lobe epilepsy, with and without tariquidar pretreatment. In total, 29 rats underwent 2 consecutive 11 C-flumazenil PET scans, each one lasting 30 min. The tracer was mixed with different amounts of isotopically unmodified flumazenil (4, 20, 100, or 400 mg) to cover a wide range of receptor occupancies during the scan. Before the second scan, the rats were pretreated with a 3 or 15 mg/kg dose of the P-gp inhibitor tariquidar. The second scan was then obtained according to the same protocol as the first scan. Results: GABA A receptor density, B max , was estimated as 44 6 2 ngÁmL 21 in the hippocampus and as 33 6 2 ngÁmL 21 in the cerebellum, with intermediate values in the occipital cortex, parietal cortex, and caudate putamen. B max was decreased by 12% in kainate-treated rats, compared with controls. The radiotracer equilibrium dissociation constant, K D , was similar in both rat groups and all brain regions and was estimated as 5.9 6 0.9 ngÁmL 21 . There was no difference in flumazenil transport across the blood-brain barrier between control and kainate-treated rats, and the effect of tariquidar treatment was similar in both rat groups. Tariquidar treatment also decreased flumazenil transport out of the brain by 73%, increased the volume of distribution in the brain by 24%, and did not influence B max or K D , compared with baseline . Conclusion: B max was decreased in kainate-treated rats, compared with controls, but no alteration in the bloodbrain barrier transport of flumazenil was observed. P-gp inhibition by tariquidar treatment increased brain concentrations of flumazenil in both groups, but B max estimates were not influenced, suggesting that 11 C-flumazenil scanning is not confounded by alterations in P-gp function.

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Section: Discussioncontrasting

confidence: 50%

Section: Pet Experimentsmentioning

confidence: 99%

Altered GABA_A Receptor Density and Unaltered Blood–Brain Barrier Transport in a Kainate Model of Epilepsy: An In Vivo Study Using ¹¹C-Flumazenil and PET

et al. 2012

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“…The choice of loperamide as a P-gp substrate and its dose was based on its opiate-like behavior, which provides an efficient means with which to ascertain the blockage of the P-gp (Elkiweri et al, 2009). Because the reported ED 50 values for tariquidar and elacridar in rats (Kuntner et al, 2010) were lethal in coadministration with loperamide in our pilot study, the doses of the P-gp modulators were reduced to 0.5 or 1.0 mg/kg.…”

Section: Methodsmentioning

confidence: 99%

Coadministration of P-Glycoprotein Modulators on Loperamide Pharmacokinetics and Brain Distribution

et al. 2014

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The efflux transporter P-glycoprotein, expressed at high levels at the blood-brain barrier, exerts a profound effect on the disposition of various therapeutic compounds in the brain. A rapid and efficient modulation of this efflux transporter could enhance the distribution of its substrates and thereby improve central nervous system pharmacotherapies. This study explored the impact of the intravenous coadministration of two P-glycoprotein modulators, tariquidar and elacridar, on the pharmacokinetics and brain distribution of loperamide, a P-glycoprotein substrate probe, in rats. After 1 hour postdosing, tariquidar and elacridar, both at a dose of 1.0 mg/kg, increased loperamide levels in the brain by 2.3-and 3.5-fold, respectively. However, the concurrent administration of both P-glycoprotein modulators, each at a dose of 0.5 mg/kg, increased loperamide levels in the brain by 5.8-fold and resulted in the most pronounced opioid-induced clinical signs. This phenomenon may be the result of a combined noncompetitive modulation by tariquidar and elacridar. Besides, the simultaneous administration of elacridar and tariquidar did not significantly modify the pharmacokinetic parameters of loperamide. This observation potentially allows the concurrent use of low but therapeutic doses of P-gp modulators to achieve full inhibitory effects.

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“…Elacridar is a third-generation P-gp inhibitor with K i of 1.6 nM for P-gp inhibition and is also a potent Bcrp inhibitor with in vitro EC 90 of 51 to 61 nM (Allen et al, 2002;Sugimoto et al, 2011). Its in vivo mouse and rat plasma IC 50 for inhibition of P-gp at the BBB ranged from 114 to 282 ng/ml, and its IC 50 for inhibition of Bcrp was 790 ng/ml determined in a brain perfusion study (Cutler et al, 2006;Bihorel et al, 2007;Oostendorp et al, 2009;Kuntner et al, 2010;Sugimoto et al, 2011). Thus, with 2-fold as a cutoff value for the effects of elacridar on K p , no change for the K p values of P-gp and/or Bcrp substrates occurs when elacridar plasma concentrations are below 114 ng/ml.…”

Section: Liu Et Almentioning

confidence: 99%

Use of the Cassette-Dosing Approach to Assess Brain Penetration in Drug Discovery

Liu¹,

Ding²,

Deshmukh³

et al. 2012

Drug Metab Dispos

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ABSTRACT:The objective of the present study was to examine the cassette dosing method in determination of brain-to-plasma concentration ratio (area under the concentration-time profiles for plasma/area under the concentration-time profiles for brain, K p ). Eleven model compounds, amprenavir, citalopram, digoxin, elacridar, imatinib, (3S,6S,12aS)-1,2,3,4,6,7,12,12a-octahydro-9-methoxy-6-(2-methylpropyl)-1,4-dioxopyrazino[1,2:1,6]pyrido[3,4-b]indole-3-propanoic acid 1,1-dimethylethyl ester (Ko143), loperamide, prazosin, quinidine, sulfasalazine, and verapamil, were selected to compare their K p determined from discrete dosing in wild-type mice and their K p from cassette dosing in wild-type, Mdr1a/1b(؊/؊), Bcrp1(؊/؊), and Mdr1a/1b(؊/؊)/Bcrp1(؊/؊) mice at 1 to 3 mg/kg. The mice brain and plasma were collected at 0.25, 1, and 3 h and were analyzed using high-performance liquid chromatography-tandem mass spectrometry methods. The K p determined from discrete dosing versus cassette dosing in the wild-type mice were within 2-fold for all the compounds except sulfasalazine and Ko143. The brain concentrations of sulfasalazine and Ko143 and the plasma concentrations of Ko143 were below the lower limit of quantitation. In addition, the K p values estimated by mass spectrometry responses, namely the ratio of compound peak area to internal standard peak area, were within 2-fold of the K p observed from the actual concentrations. Furthermore, the ratios of K p in Mdr1a/1b(؊/؊), Bcrp1(؊/؊), and Mdr1a/1b(؊/؊)/ Bcrp1(؊/؊) mice versus the K p in the wild-type mice from cassette dosing were consistent with the ones reported in the literature where the compounds were dosed discretely. These results demonstrate that drug-drug interactions at the blood-brain barrier are unlikely at a subcutaneous dose of 1 to 3 mg/kg and support the use of the cassette dosing approach to assess brain penetration in drug discovery.

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Dose-response assessment of tariquidar and elacridar and regional quantification of P-glycoprotein inhibition at the rat blood-brain barrier using (R)-[11C]verapamil PET

Cited by 102 publications

References 25 publications

Altered GABA_A Receptor Density and Unaltered Blood–Brain Barrier Transport in a Kainate Model of Epilepsy: An In Vivo Study Using ¹¹C-Flumazenil and PET

Altered GABA_A Receptor Density and Unaltered Blood–Brain Barrier Transport in a Kainate Model of Epilepsy: An In Vivo Study Using ¹¹C-Flumazenil and PET

Coadministration of P-Glycoprotein Modulators on Loperamide Pharmacokinetics and Brain Distribution

Use of the Cassette-Dosing Approach to Assess Brain Penetration in Drug Discovery

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Dose-response assessment of tariquidar and elacridar and regional quantification of P-glycoprotein inhibition at the rat blood-brain barrier using (R)-[11C]verapamil PET

Cited by 102 publications

References 25 publications

Altered GABAA Receptor Density and Unaltered Blood–Brain Barrier Transport in a Kainate Model of Epilepsy: An In Vivo Study Using 11C-Flumazenil and PET

Altered GABAA Receptor Density and Unaltered Blood–Brain Barrier Transport in a Kainate Model of Epilepsy: An In Vivo Study Using 11C-Flumazenil and PET

Coadministration of P-Glycoprotein Modulators on Loperamide Pharmacokinetics and Brain Distribution

Use of the Cassette-Dosing Approach to Assess Brain Penetration in Drug Discovery

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Product

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Altered GABA_A Receptor Density and Unaltered Blood–Brain Barrier Transport in a Kainate Model of Epilepsy: An In Vivo Study Using ¹¹C-Flumazenil and PET

Altered GABA_A Receptor Density and Unaltered Blood–Brain Barrier Transport in a Kainate Model of Epilepsy: An In Vivo Study Using ¹¹C-Flumazenil and PET