Human native kappa opioid receptor functions not predicted by recombinant receptors: {Implications} for drug design.

Broad, John; Maurel, Damien; Kung, Victor W. S.; Hicks, Gareth A.; Schemann, Michael; Barnes, Michael R.; Kenakin, Terrence P.; Granier, Sebastien; Sanger, Gareth J.

doi:10.1038/srep30797

Lehrstuhl für Humanbiologie (Prof. Schemann)

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Title:: Human native kappa opioid receptor functions not predicted by recombinant receptors: {Implications} for drug design.
Document type:: Zeitschriftenaufsatz
Author(s):: Broad, John; Maurel, Damien; Kung, Victor W. S.; Hicks, Gareth A.; Schemann, Michael; Barnes, Michael R.; Kenakin, Terrence P.; Granier, Sebastien; Sanger, Gareth J.
Abstract:: If activation of recombinant G protein-coupled receptors in host cells (by drugs or other ligands) has predictive value, similar data must be obtained with native receptors naturally expressed in tissues. Using mouse and human recombinant kappa opioid receptors transfected into a host cell, two selectively-acting compounds (ICI204448, asimadoline) equi-effectively activated both receptors, assessed by measuring two different cell signalling pathways which were equally affected without evidence of bias. In mouse intestine, naturally expressing kappa receptors within its nervous system, both compounds also equi-effectively activated the receptor, inhibiting nerve-mediated muscle contraction. However, whereas ICI204448 acted similarly in human intestine, where kappa receptors are again expressed within its nervous system, asimadoline was inhibitory only at very high concentrations; instead, low concentrations of asimadoline reduced the activity of ICI204448. This demonstration of species-dependence in activation of native, not recombinant kappa receptors may be explained by different mouse/human receptor structures affecting receptor expression and/or interactions with intracellular signalling pathways in native environments, to reveal differences in intrinsic efficacy between receptor agonists. These results have profound implications in drug design for kappa and perhaps other receptors, in terms of recombinant-to-native receptor translation, species-dependency and possibly, a need to use human, therapeutically-relevant, not surrogate tissues. «
If activation of recombinant G protein-coupled receptors in host cells (by drugs or other ligands) has predictive value, similar data must be obtained with native receptors naturally expressed in tissues. Using mouse and human recombinant kappa opioid receptors transfected into a host cell, two selectively-acting compounds (ICI204448, asimadoline) equi-effectively activated both receptors, assessed by measuring two different cell signalling pathways which were equally affected without evidence... »
Journal title:: Scientific reports
Year:: 2016
Journal volume:: 6
Month:: aug
Pages contribution:: 30797
Language:: eng
Fulltext / DOI:: doi:10.1038/srep30797
Print-ISSN:: 2045-2322 2045-2322
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mediaTUM Gesamtbestand Einrichtungen Schools TUM School of Life Sciences Departments Molecular Life Sciences Lehrstuhl für Humanbiologie (N.N.)

mediaTUM Gesamtbestand Hochschulbibliographie 2016 Fakultäten Wissenschaftszentrum Weihenstephan Lehrstuhl für Humanbiologie (Prof. Schemann)