PPAR Research

Review Article

Mediating Roles of PPARs in the Effects of Environmental Chemicals on Sex Steroids

Table 1

Various kinds of environmental activators of PPARs and their impact on sex steroids.
ChemicalsPPARs subtypeMethodsEffects on sex steroidsExperimental modelReferences
DEHPα, γDocking, transcript profiles, antagonismEnhanced expression of aromatase, altered levels of estradiolRat, endometrial cells, fish[2225]
MEHPα, β/δ, γAntagonism, transcript profilesDecreased expression of aromatase and estradiol productionRat ovarian granulosa cells, rat model, human liposarcoma cells, 3T3-L1 cells[2529]
DEHTαDockingNo significant impactRat model[30]
PFNAα, β/δ, γTranscript profiles, PPRE reporterElevated expression of CYP4AZebrafish, monkey kidney CV-1 cell line[31, 32]
PFOAα, γPPRE reporter, transcript profiles, antagonism, gene silencing/Monkey kidney CV-1 cell line, mice[31, 3336]
PFOSα, γPPRE reporter
transcript profiles, antagonism, gene silencing		/Monkey kidney CV-1 cell line, O. melastigma, mice[31, 33, 3539]
PFDAαPPRE reporter/Monkey kidney CV-1 cell line[31]
PFUnDAαPPRE reporter/monkey kidney CV-1 cell line[31]
TBBPAγPPRE reporterIncreased apelin expression and secretionEpithelial ovarian cancer cell line (OVCAR-3)[40, 41]
TCBPAγPPRE reporterIncreased apelin expression and secretionOVCAR-3[40, 41]
BPAa, β/δ, γTranscript profiles, PPRE reporter, dockingDecreased expression of aromatase and estradiol productionHuman ovarian granulosa cell, mouse embryo fibroblasts, OVCAR-3[4146]
PCB77a, β/δ, γDocking, antagonism//[47]
PCB118a, β/δ, γDocking, antagonism/Cell model, mice model[7, 47]
PCB126αTranscript profilesAltered the secretion of estradiolRat model, mice model[48]
DDTγTranscript profilesEnhanced expression of CYP4AHuman mesenchymal stem cells[49]
2,4-DγTranscript profiles, gene silencingDecreased cholesterol levelsMice leydig cells, mice model[6]
TBTa, β/δ, γPPRE reporterInhibition of gonad developmentJuvenile salmon, cell model[50, 51]
EE2γTranscript profilesBrown trout[11]
/” indicated data is not available as we known; The experimental methods to support the interaction between chemicals and PPARs are depicted as follows, Antagonism: PPARs was antagonized by specific antagonist. Then, the effects elicited by chemicals were re-assessed. If the effects were diminished or enhanced, the mediating roles of PPARs could be confirmed; Transcript profiles: Transcript profiles of PPARs were modulated by chemicals treatment; Docking: Computing methods to predict the structural binding between chemicals and PPARs; PPRE reporter: Reporter system was constructed by transfecting the luciferase reporting plasmid containing PPRE sequence into the cells. Then, the cells were treated with chemicals to determine whether chemicals functioned through activating PPARs; Gene silencing: The expression of PPARs was inhibited by RNAi or gene knockout. Then, the effects elicited by chemicals were re-assessed. If the effects were diminished or enhanced, the mediating roles of PPARs could be confirmed; Abbreviation: di-(2-ethylhexyl) phthalate, DEHP; mono-(2-ethylhexyl) phthalate, MEHP; di(2-ethylhexyl) terephthalate, DEHT; perfluorododecanoic acid, PFDoA; perfluorononanoic acid, PFNA; perfluorooctanoic acid, PFOA; perfluorodecanoic acid, PFDA; perfluoroundecanoic acid, PFUnDA; perfluorooctane sulfonate, PFOS; BPA diglycidyl ether, BADGE; tetrabromobisphenol A, TBBPA; tetrachlorobisphenol A, TCBPA; bisphenol A, BPA; polychlorinated biphenyls, PCB; dichlorodiphenyltrichloroethane, DDT; 2,3,7,8-tetrachlorodibenzo-p-dioxin, TCDD; 2,4-dichlorophenoxyacetic acid, 2,4-D; organotin, TBT; ethinylestradiol, EE2.