Alteration of a Single Amino Acid in Peroxisome Proliferator-Activated Receptor-α (PPARα) Generates a PPARδ Phenotype

Three pharmacologically important nuclear receptors, the peroxisome proliferator-activated receptors (PPARs α,γ , and δ), mediate key transcriptional responses involved in lipid homeostasis. The PPARα and γ subtypes are well conserved from Xenopus to man, but the β/δ subtypes display substantial spe...

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Published inMolecular endocrinology (Baltimore, Md.) Vol. 14; no. 5; pp. 733 - 740
Main Authors Takada, Ichiro, Yu, Ruth T, Xu, H. Eric, Lambert, Millard H, Montana, Valerie G, Kliewer, Steven A, Evans, Ronald M, Umesono, Kazuhiko
Format Journal Article
LanguageEnglish
Published United States Endocrine Society 01.05.2000
Oxford University Press
Subjects
Amino Acid Substitution
Animals
Cell Line
Chickens
Crystallography, X-Ray
DNA, Complementary - genetics
Evolution, Molecular
Haplorhini
Humans
Kidney
Male
Mammals
Methionine - chemistry
Models, Molecular
Mutagenesis, Site-Directed
Peroxisome Proliferators - pharmacology
Phenotype
Protein Conformation
Receptors, Cytoplasmic and Nuclear - chemistry
Receptors, Cytoplasmic and Nuclear - drug effects
Receptors, Cytoplasmic and Nuclear - genetics
Species Specificity
Transcription Factors - chemistry
Transcription Factors - drug effects
Transcription Factors - genetics
Transfection
Valine - chemistry
Xenopus laevis
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Summary:Three pharmacologically important nuclear receptors, the peroxisome proliferator-activated receptors (PPARs α,γ , and δ), mediate key transcriptional responses involved in lipid homeostasis. The PPARα and γ subtypes are well conserved from Xenopus to man, but the β/δ subtypes display substantial species variations in both structure and ligand activation profiles. Characterization of the avian cognates revealed a close relationship between chick (c) α and γ subtypes to their mammalian counterparts, whereas the third chicken subtype was intermediate to Xenopus (x) β and mammalian δ, establishing that β and δ are orthologs. Like xPPARβ, cPPARβ responded efficiently to hypolipidemic compounds that fail to activate the human counterpart. This provided the opportunity to address the pharmacological problem as to how drug selectivity is achieved and the more global evolutionary question as to the minimal changes needed to generate a new class of receptor. X-ray crystallography and chimeric analyses combined with site-directed mutagenesis of avian and mammalian cognates revealed that a Met to Val change at residue 417 was sufficient to switch the human and chick phenotype. These results establish that the genetic drive to evolve a novel and functionally selectable receptor can be modulated by a single amino acid change and suggest how nuclear receptors can accommodate natural variation in species physiology.
ISSN:0888-8809
1944-9917
DOI:10.1210/mend.14.5.0456