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Mechanistic characterization of isoform selective inhibitors of mammalian phospholipase D

dc.creatorSelvy, Paige Elizabeth
dc.date.accessioned2020-08-23T15:43:07Z
dc.date.available2013-11-11
dc.date.issued2011-11-11
dc.identifier.urihttps://etd.library.vanderbilt.edu/etd-11072011-164315
dc.identifier.urihttp://hdl.handle.net/1803/14456
dc.description.abstractIncreasing evidence supports an integral role for the lipid second messenger phosphatidic acid (PtdOH) in cell signaling. In addition to altering curvature of biological membranes, PtdOH lies at the intersection between metabolism and signaling pathways and is involved in cell survival as well as proliferation pathways. Phospholipase D (PLD), an evolutionarily conserved phosphodiesterase that hydrolyzes phosphatidylcholine, is involved in generating signal-mediated PtdOH molecular species. Aberrant PLD expression and activity have been implicated in metastatic cancers, neurological disorders, and microbial pathogenesis, making this enzyme a potential therapeutic target for which we recently developed potent and isoform-selective pharmacological inhibitors. Here we define the mechanism of action for these novel small molecule inhibitors. Using backscattering interferometry (BSI), a novel method for measuring protein-small molecule and protein-lipid binding, we demonstrate that these compounds directly interact with PLD to allosterically block interfacial lipid binding and catalytic activity. This unanticipated finding represents a unique mechanism of phospholipase inhibition and a new paradigm for modulation of signaling pathways.
dc.format.mimetypeapplication/pdf
dc.subjectsmall molecule inhibitor
dc.subjectphospholipase D
dc.subjectmechanism
dc.subjectinterfacial kinetics
dc.subjectenzyme kinetics
dc.subjectlipids
dc.titleMechanistic characterization of isoform selective inhibitors of mammalian phospholipase D
dc.typedissertation
dc.contributor.committeeMemberTina M. Iverson
dc.contributor.committeeMemberVsevolod Gurevich
dc.contributor.committeeMemberH. Alex Brown
dc.contributor.committeeMemberEthan Lee
dc.type.materialtext
thesis.degree.namePHD
thesis.degree.leveldissertation
thesis.degree.disciplinePharmacology
thesis.degree.grantorVanderbilt University
local.embargo.terms2013-11-11
local.embargo.lift2013-11-11
dc.contributor.committeeChairCraig W. Lindsley


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