Mass spectrometry reveals synergistic effects of nucleotides, lipids, and drugs binding to a multidrug resistance efflux pump
Mass spectrometry reveals synergistic effects of nucleotides, lipids, and drugs binding to a multidrug resistance efflux pump
Multidrug resistance is a serious barrier to successful treatment of many human diseases, including cancer, wherein chemotherapeutics are exported from target cells by membrane-embedded pumps. The most prevalent of these pumps, the ATP-Binding Cassette transporter P-glycoprotein (P-gp), consists of two homologous halves each comprising one nucleotide-binding domain and six transmembrane helices. The transmembrane region encapsulates a hydrophobic cavity, accessed by portals in the membrane, that binds cytotoxic compounds as well as lipids and peptides. Here we use mass spectrometry (MS) to probe the intact P-gp small molecule-bound complex in a detergent micelle. Activation in the gas phase leads to formation of ions, largely devoid of detergent, yet retaining drug molecules as well as charged or zwitterionic lipids. Measuring the rates of lipid binding and calculating apparent KD values shows that up to six negatively charged diacylglycerides bind more favorably than zwitterionic lipids. Similar experiments confirm binding of cardiolipins and show that prior binding of the immunosuppressant and antifungal antibiotic cyclosporin A enhances subsequent binding of cardiolipin. Ion mobility MS reveals that P-gp exists in an equilibrium between different states, readily interconverted by ligand binding. Overall these MS results show how concerted small molecule binding leads to synergistic effects on binding affinities and conformations of a multidrug efflux pump.
9704-9709
Marcoux, J
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Wang, SC
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Politis, A
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Reading, E
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Ma, J
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Biggin, PC
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Zhou, M
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Tao, H
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Zhang, Q
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Chang, G
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Morgner, N
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Robinson, CV
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20 May 2013
Marcoux, J
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Wang, SC
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Politis, A
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Reading, E
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Ma, J
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Biggin, PC
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Zhou, M
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Tao, H
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Zhang, Q
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Chang, G
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Morgner, N
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Robinson, CV
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Marcoux, J, Wang, SC, Politis, A, Reading, E, Ma, J, Biggin, PC, Zhou, M, Tao, H, Zhang, Q, Chang, G, Morgner, N and Robinson, CV
(2013)
Mass spectrometry reveals synergistic effects of nucleotides, lipids, and drugs binding to a multidrug resistance efflux pump.
Nature Protocols, 110 (24), .
(doi:10.1073/pnas.1303888110).
Abstract
Multidrug resistance is a serious barrier to successful treatment of many human diseases, including cancer, wherein chemotherapeutics are exported from target cells by membrane-embedded pumps. The most prevalent of these pumps, the ATP-Binding Cassette transporter P-glycoprotein (P-gp), consists of two homologous halves each comprising one nucleotide-binding domain and six transmembrane helices. The transmembrane region encapsulates a hydrophobic cavity, accessed by portals in the membrane, that binds cytotoxic compounds as well as lipids and peptides. Here we use mass spectrometry (MS) to probe the intact P-gp small molecule-bound complex in a detergent micelle. Activation in the gas phase leads to formation of ions, largely devoid of detergent, yet retaining drug molecules as well as charged or zwitterionic lipids. Measuring the rates of lipid binding and calculating apparent KD values shows that up to six negatively charged diacylglycerides bind more favorably than zwitterionic lipids. Similar experiments confirm binding of cardiolipins and show that prior binding of the immunosuppressant and antifungal antibiotic cyclosporin A enhances subsequent binding of cardiolipin. Ion mobility MS reveals that P-gp exists in an equilibrium between different states, readily interconverted by ligand binding. Overall these MS results show how concerted small molecule binding leads to synergistic effects on binding affinities and conformations of a multidrug efflux pump.
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More information
Published date: 20 May 2013
Additional Information:
We thank Elizabeth Carpenter for helpful discussion and Martin Caffrey for providing diacylglycerol kinase alpha. We also acknowledge funding from European Research Council Integral Membrane Proteins Resolution of Stoichiometry and Structure, the Royal Society, and The Wellcome Trust
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Local EPrints ID: 479661
URI: http://eprints.soton.ac.uk/id/eprint/479661
ISSN: 1754-2189
PURE UUID: 65e4843e-78ff-4553-824c-07d491ee107c
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Date deposited: 26 Jul 2023 16:44
Last modified: 17 Mar 2024 04:19
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Author:
J Marcoux
Author:
SC Wang
Author:
A Politis
Author:
E Reading
Author:
PC Biggin
Author:
M Zhou
Author:
H Tao
Author:
Q Zhang
Author:
G Chang
Author:
N Morgner
Author:
CV Robinson
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