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Breast Cancer Resistance Protein Interacts with Various Compounds in vitro, but Plays a Minor Role in Substrate Efflux at the Blood-Brain Barrier. Drug metabolism and disposition: the biological fate of chemicals [Drug Metab Dispos] Journal article

 
Zhao R, Raub TJ, Sawada GA, Kasper SC, Bacon JA, Bridges AS, Pollack GM 
Breast Cancer Resistance Protein Interacts with Various Compounds in vitro, but Plays a Minor Role in Substrate Efflux at the Blood-Brain Barrier. [JOURNAL ARTICLE]
Drug Metab Dispos 2009 Mar 9.


Expression of breast cancer resistance protein (Bcrp) at the blood-brain barrier (BBB) has been revealed recently. In order to investigate comprehensively the potential role of Bcrp at the murine BBB, a chemically-diverse set of model compounds (cimetidine, alfuzosin, dipyridamole and LY2228820) was evaluated utilizing a multiexperimental design. Bcrp1 stably-transfected MDCKII cell monolayer transport studies demonstrated that each compound had affinity for Bcrp, and that polarized transport by Bcrp was abolished completely by the Bcrp inhibitor chrysin. However, none of the compounds differed in brain uptake between Bcrp wild type and knockout mice under either an in situ brain perfusion or a 24-hr subcutaneous osmotic minipump continuous infusion experimental paradigm. In addition, alfuzosin and dipyridamole were shown to undergo transport by P-gp in an MDCKII-MDR1 cell monolayer model. Alfuzosin brain uptake was four-fold higher in mdr1a(-/-) mice than in mdr1a(+/+) mice in in situ and in vivo studies, demonstrating for the first time that it undergoes P-gp-mediated efflux at the BBB. In contrast, P-gp had no effect on dipyridamole brain penetration in situ or in vivo. In fact, in situ BBB permeability of these solutes appeared to be primarily dependent on their lipophilicity in the absence of efflux transport, and in situ brain uptake clearance correlated with the intrinsic transcellular passive permeability from in vitro transport and cellular accumulation studies. In summary, Bcrp mediates in vitro transport of various compounds, but appears to play a minimal role at the BBB in vivo.



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