EMD-6025
Conformational Spectrum of Multidrug ABC Transporters Revealed by Single Particle Electron Microscopy
EMD-6025
Single-particle30.0 Å
Deposition: 07/08/2014Map released: 04/02/2015
Last modified: 16/09/2015
Sample Organism:
Escherichia coli
Sample: MsbA stabilised in amphiphilic environment - inward-facing 4.5 nm opening
Deposition Authors: Moeller A
,
Chang Lee S,
Tao H,
Speir S,
Chang G,
Urbatsch IL,
Potter CS,
Carragher B,
Zhang Q
Sample: MsbA stabilised in amphiphilic environment - inward-facing 4.5 nm opening
Deposition Authors: Moeller A
,
Chang Lee S,
Tao H,
Speir S,
Chang G,
Urbatsch IL,
Potter CS,
Carragher B,
Zhang Q
Distinct Conformational Spectrum of Homologous Multidrug ABC Transporters
Moeller A ,
Chang Lee S,
Tao H,
Speir S,
Chang G,
Urbatsch IL,
Potter CS,
Carragher B,
Zhang Q
(2015) Structure , 23 , 450 - 460
,
Chang Lee S,
Tao H,
Speir S,
Chang G,
Urbatsch IL,
Potter CS,
Carragher B,
Zhang Q
(2015) Structure , 23 , 450 - 460
Abstract:
ATP-binding cassette (ABC) exporters are ubiquitously found in all kingdoms of life and their members play significant roles in mediating drug pharmacokinetics and multidrug resistance in the clinic. Significant questions and controversies remain regarding the relevance of their conformations observed in X-ray structures, their structural dynamics, and mechanism of transport. Here, we used single particle electron microscopy (EM) to delineate the entire conformational spectrum of two homologous ABC exporters (bacterial MsbA and mammalian P-glycoprotein) and the influence of nucleotide and substrate binding. Newly developed amphiphiles in complex with lipids that support high protein stability and activity enabled EM visualization of individual complexes in a membrane-mimicking environment. The data provide a comprehensive view of the conformational flexibility of these ABC exporters under various states and demonstrate not only similarities but striking differences between their mechanistic and energetic regulation of conformational changes.
ATP-binding cassette (ABC) exporters are ubiquitously found in all kingdoms of life and their members play significant roles in mediating drug pharmacokinetics and multidrug resistance in the clinic. Significant questions and controversies remain regarding the relevance of their conformations observed in X-ray structures, their structural dynamics, and mechanism of transport. Here, we used single particle electron microscopy (EM) to delineate the entire conformational spectrum of two homologous ABC exporters (bacterial MsbA and mammalian P-glycoprotein) and the influence of nucleotide and substrate binding. Newly developed amphiphiles in complex with lipids that support high protein stability and activity enabled EM visualization of individual complexes in a membrane-mimicking environment. The data provide a comprehensive view of the conformational flexibility of these ABC exporters under various states and demonstrate not only similarities but striking differences between their mechanistic and energetic regulation of conformational changes.