Identification of Novel Specific and General Inhibitors of the Three Major Human ATP-Binding Cassette Transporters P-gp,BCRP and MRP2 Among Registered Drugs |
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Authors: | Pär Matsson Jenny M Pedersen Ulf Norinder Christel A S Bergström Per Artursson |
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Institution: | 1.Pharmaceutical Screening and Informatics, Department of Pharmacy,Uppsala University,Uppsala,Sweden;2.AstraZeneca R&D,S?dert?lje,Sweden |
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Abstract: | Purpose To study the inhibition patterns of the three major human ABC transporters P-gp (ABCB1), BCRP (ABCG2) and MRP2 (ABCC2), using
a dataset of 122 structurally diverse drugs.
Methods Inhibition was investigated in cellular and vesicular systems over-expressing single transporters. Computational models discriminating
either single or general inhibitors from non-inhibitors were developed using multivariate statistics.
Results Specific (n = 23) and overlapping (n = 19) inhibitors of the three ABC transporters were identified. GF120918 and Ko143 were verified to specifically inhibit
P-gp/BCRP and BCRP in defined concentration intervals, whereas the MRP inhibitor MK571 was revealed to inhibit all three transporters
within one log unit of concentration. Virtual docking experiments showed that MK571 binds to the ATP catalytic site, which
could contribute to its multi-specific inhibition profile. A computational model predicting general ABC inhibition correctly
classified 80% of both ABC transporter inhibitors and non-inhibitors in an external test set.
Conclusions The inhibitor specificities of P-gp, BCRP and MRP2 were shown to be highly overlapping. General ABC inhibitors were more lipophilic
and aromatic than specific inhibitors and non-inhibitors. The identified specific inhibitors can be used to delineate transport
processes in complex experimental systems, whereas the multi-specific inhibitors are useful in primary ABC transporter screening
in drug discovery settings.
Electronic supplementary material The online version of this article (doi:) contains supplementary material, which is available to authorized users.
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Keywords: | ABC transporters drug transport inhibition structure– activity relationships transport proteins |
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