Structural mechanism for multidrug efflux systems

dc.contributor.advisor Edward W. Yu Su, Chih-chia
dc.contributor.department Biochemistry, Biophysics and Molecular Biology 2018-08-11T14:45:29.000 2020-06-30T02:31:23Z 2020-06-30T02:31:23Z Thu Jan 01 00:00:00 UTC 2009 2013-06-05 2009-01-01
dc.description.abstract <p>Bacteria such as Escherichia coli, Campylobacter jejuni and Neisseria gonorrhoeae have developed various mechanisms to overcome toxic environments that are otherwise unfavorable for their survival. One important strategy that bacteria use to expel toxic compounds, including heavy metal ions, is the expression of membrane efflux transporters that recognize and actively export these toxic compounds out of bacterial cells, thereby allowing them to survive in extremely toxic conditions. Many of these transporters are multiple drug binding proteins which extrude different toxic chemicals and mediate a phenomenon of multidrug resistance (MDR) in bacteria. The expression of these efflux transporters is tightly controlled at the transcriptional level by transcriptional regulators. A number of these transcriptional regulators are also multidrug binding proteins, which recognize and respond to the same set of toxic chemicals that are expelled by the efflux transporters they regulate. The goal of this dissertation is to elucidate the structures and fundamental mechanisms that give rise to multiple drug recognition in these efflux transporters and their regulators. We have determined several x-ray structures of these important proteins, including the E. coli AcrB efflux transporter, C. jejuni CmeR transcriptional regulator and E. coli CusB heavy-metal efflux protein. We also crystallized the N. gonorrhoeae NorM multidrug transporter and collected the x-ray diffraction data of the crystals. To gain further insight into the mechanism of multiple drug recognition, we examined the binding affinities of AcrB and AcrR to different drugs using fluorescence polarization assays. In this thesis, we will summarize the new findings with AcrB, AcrR, CmeR and CusB, and discuss the structure and function of these efflux transporters and regulators.</p>
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dc.identifier archive/
dc.identifier.articleid 1865
dc.identifier.contextkey 2807063
dc.identifier.s3bucket isulib-bepress-aws-west
dc.identifier.submissionpath etd/10840
dc.language.iso en
dc.source.bitstream archive/|||Fri Jan 14 18:29:16 UTC 2022
dc.subject.disciplines Biochemistry, Biophysics, and Structural Biology
dc.subject.keywords membrane fusion protein
dc.subject.keywords membrane protein
dc.subject.keywords Multidrug transporter
dc.title Structural mechanism for multidrug efflux systems
dc.type article
dc.type.genre dissertation
dspace.entity.type Publication
relation.isOrgUnitOfPublication faf0a6cb-16ca-421c-8f48-9fbbd7bc3747 dissertation Doctor of Philosophy
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