Imaging the impact of cyclosporin A and dipyridamole on P-glycoprotein (ABCB1) function at the blood-brain barrier: A [(11)C]-N-desmethyl-loperamide PET study in nonhuman primates

Annelaure Damont; Sébastien Goutal; Sylvain Auvity; Héric Valette; Bertrand Kuhnast; Wadad Saba; Nicolas Tournier

doi:10.1016/j.ejps.2016.06.005

Imaging the impact of cyclosporin A and dipyridamole on P-glycoprotein (ABCB1) function at the blood-brain barrier: A [(11)C]-N-desmethyl-loperamide PET study in nonhuman primates

Eur J Pharm Sci. 2016 Aug 25:91:98-104. doi: 10.1016/j.ejps.2016.06.005. Epub 2016 Jun 7.

Authors

Annelaure Damont¹, Sébastien Goutal¹, Sylvain Auvity¹, Héric Valette¹, Bertrand Kuhnast¹, Wadad Saba¹, Nicolas Tournier²

Affiliations

¹ Imagerie Moléculaire In Vivo, IMIV, CEA, Inserm, CNRS, Univ. Paris-Sud, Université Paris Saclay, CEA-SHFJ, Orsay, France.
² Imagerie Moléculaire In Vivo, IMIV, CEA, Inserm, CNRS, Univ. Paris-Sud, Université Paris Saclay, CEA-SHFJ, Orsay, France. Electronic address: nicolas.tournier@cea.fr.

PMID: 27283486
DOI: 10.1016/j.ejps.2016.06.005

Abstract

Cyclosporin A (CsA) and dipyridamole (DPy) are potent inhibitors of the P-glycoprotein (P-gp; ABCB1) in vitro. Their efficacy at inhibiting P-gp at the blood-brain barrier (BBB) is difficult to predict. Efficient and readily available (i.e. marketed) P-gp inhibitors are needed as probes to investigate the role of P-gp at the human BBB. In this study, the P-gp inhibition potency at the BBB of therapeutic doses of CsA or DPy was evaluated in baboons using Positron Emission Tomography (PET) imaging with [(11)C]-N-desmethyl-loperamide ([(11)C]dLop), a radiolabeled P-gp substrate. The preparation of dLop as authentic standard and [(11)C]dLop as radiotracer were revisited so as to improve their production yields. [(11)C]dLop PET imaging was performed in the absence (n=3, baseline condition) and the presence of CsA (15mg/kg/h i.v., n=3). Three animals were injected with i.v. DPy at either 0.56 or 0.96 or 2mg/kg (n=1), corresponding to the usual, maximal and twice the maximal dose in patients, respectively, administered immediately before PET. [(11)C]dLop brain kinetics as well as [(11)C]dLop kinetics and radiometabolites in arterial plasma were measured to calculate [(11)C]dLop area-under the time-activity curve from 10 to 30min in the brain (AUCbrain) and in plasma (AUCplasma). [(11)C]dLop brain uptake was described by AUCR=AUCbrain/AUCplasma. CsA as well as DPy did not measurably influence [(11)C]dLop plasma kinetics and metabolism. Baseline AUCR (0.85±0.29) was significantly enhanced in the presence of CsA (AUCR=10.8±3.6). Injection of pharmacologic dose of DPy did not enhance [(11)C]dLop brain distribution with AUCR being 1.2, 0.9 and 1.1 after administration of 0.56, 0.96 and 2mg/kg DPy doses, respectively. We used [(11)C]dLop PET imaging in baboons, a relevant in vivo model of P-gp function at the BBB, to show the P-gp inhibition potency of therapeutic dose CsA. Despite in vitro P-gp inhibition potency, usual doses DPy are not likely to inhibit P-gp function at the BBB.

Keywords: BBB; Drug-drug interaction; Positron emission tomography; Radiochemistry; Stress-test.

MeSH terms

ATP Binding Cassette Transporter, Subfamily B, Member 1 / antagonists & inhibitors*
ATP Binding Cassette Transporter, Subfamily B, Member 1 / metabolism
Animals
Blood-Brain Barrier / diagnostic imaging
Blood-Brain Barrier / drug effects*
Blood-Brain Barrier / metabolism
Carbon Radioisotopes
Cyclosporine / pharmacokinetics
Cyclosporine / pharmacology*
Dipyridamole / pharmacokinetics
Dipyridamole / pharmacology*
Loperamide / analogs & derivatives
Male
Papio
Positron-Emission Tomography / methods

Substances

ATP Binding Cassette Transporter, Subfamily B, Member 1
Carbon Radioisotopes
N-demethylloperamide
Dipyridamole
Loperamide
Cyclosporine