Overview of Nomenclature of Nuclear Receptors

Nuclear receptor pharmacology has, to a certain extent, led the way, compared with other receptor systems, in the appreciation that ligands may exert very diverse pharmacology, based on their individual chemical structure and the allosteric changes induced in the receptor/accessory protein complex....

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Bibliographic Details
Published inPharmacological reviews Vol. 58; no. 4; pp. 685 - 704
Main Authors Germain, Pierre, Staels, Bart, Dacquet, Catherine, Spedding, Michael, Laudet, Vincent
Format Journal Article
LanguageEnglish
Published United States American Society for Pharmacology and Experimental Therapeutics 01.12.2006
Subjects
Animals
Binding Sites
Binding Sites - genetics
Biochemistry, Molecular Biology
Gene Expression Regulation
Humans
Life Sciences
Ligands
Molecular biology
Receptors, Cytoplasmic and Nuclear
Receptors, Cytoplasmic and Nuclear - classification
Receptors, Cytoplasmic and Nuclear - genetics
Receptors, Cytoplasmic and Nuclear - physiology
Terminology
Terminology as Topic
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Summary:Nuclear receptor pharmacology has, to a certain extent, led the way, compared with other receptor systems, in the appreciation that ligands may exert very diverse pharmacology, based on their individual chemical structure and the allosteric changes induced in the receptor/accessory protein complex. This can lead to very selective pharmacological effects, which may not necessarily be predicted from the experience with other agonists/partial agonists/antagonists. If this is the case, then drug discovery may be back to drug-specific pharmacology (where each drug may have an original profile), rather than specific-drug pharmacology (where agents specific for a receptor have a distinct profile). As functional selectivity is indeed a crucial mechanism to be considered when going through the drug discovery development process, then initial screens using reconstituted systems may not show the appropriate pharmacology, simply because the required stoichiometry of corepressors and coactivators may not be present to select the best compounds; therefore, multiple effector systems are necessary to screen for differential activation, and, even then, screening with in vivo pathophysiological models may ultimately be required for the selection process—a massive but necessary task for pharmacologists. Thus, the characterization of nuclear receptors and their associated proteins and the ligands that interact with them will remain a challenge to pharmacologists.
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ISSN:0031-6997
1521-0081
DOI:10.1124/pr.58.4.2