The Handbook of International Advertising Research 2014
DOI: 10.1002/9781118378465.ch5
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Cited by 1 publication
(3 citation statements)
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“…Additionally, the difference in results between in vitro and in vivo assays for orthologues of each SphK isoform 14 is unexpected but provides a pathway to rationalize current experimental results on inhibitor efficacy. 39 Specifically, our investigation aimed to (1) interrogate how variation in key residues in the Sph binding cavities among isoforms and across orthologues affects the binding site shape, volume, and lipophilicity and ( 2) identify intermolecular interactions that can be exploited to improve inhibitors as based on known experimental inhibitor selectivity and molecular docking results.…”
Section: Resultsmentioning
confidence: 99%
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“…Additionally, the difference in results between in vitro and in vivo assays for orthologues of each SphK isoform 14 is unexpected but provides a pathway to rationalize current experimental results on inhibitor efficacy. 39 Specifically, our investigation aimed to (1) interrogate how variation in key residues in the Sph binding cavities among isoforms and across orthologues affects the binding site shape, volume, and lipophilicity and ( 2) identify intermolecular interactions that can be exploited to improve inhibitors as based on known experimental inhibitor selectivity and molecular docking results.…”
Section: Resultsmentioning
confidence: 99%
“…PF-543 is hSphK1 selective (100-fold) with a K i of 4.3 nM in hSphK1, 19 and SLP7111228 is hSphK1 selective inhibitor with a K i of 48 nM. 39 Docking results of PF-543 showed selectivity for hSphK1 when compared to mSphK1 based on our ranking of important interactions and distance measurements (Figure 6). The poses of PF-543 in hSphK2 and mSphK2 do not support selectivity for SphK 2s.…”
Section: Molecular Docking Of Dual and Isoform Selective Inhibitorsmentioning
confidence: 91%
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