An Aryl Hydrocarbon Receptor Repressor from Xenopus laevis: Function, Expression, and Role in Dioxin Responsiveness during Frog Development

doi:10.1093/toxsci/kfn066

ToxSci Advance Access originally published online on April 2, 2008
Toxicological Sciences 2008 104(1):124-134; doi:10.1093/toxsci/kfn066

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An Aryl Hydrocarbon Receptor Repressor from Xenopus laevis: Function, Expression, and Role in Dioxin Responsiveness during Frog Development

Anna L. Zimmermann, Elizabeth A. King, Emelyne Dengler, Shana R. Scogin and Wade H. Powell¹

Biology Department, Kenyon College, Gambier, Ohio 43022

¹ To whom correspondence should be addressed at Biology Department, Kenyon College, 302A College Park St., Fischman Wing 202, Gambier, OH 43022. Fax: (740) 427-5741. E-mail: powellw{at}kenyon.edu.

Received February 15, 2008; accepted March 14, 2008

Abstract

Xenopus laevis and other frogs are extremely insensitive tothe toxicity of xenobiotic ligands of the aryl hydrocarbon receptor(AHR), including 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD).Premetamorphic life stages are especially insensitive, and theyare reported to be refractory to induction of Cytochrome P4501As,which are readily induced in older animals. The AHR repressor(AHRR) is a member of the AHR gene family. AHRR expression isinduced by TCDD; it then represses AHR in an apparent negativefeedback loop. In this study, we sought to test the hypothesisthat constitutive AHRR expression underlies the lack of TCDDresponsiveness in frog early life stages. We determined thesequence of an AHRR complimentary DNA encoding an 85.3-kDa proteinsharing 52–55% identity with the bHLH/PAS domains of otherAHRRs. In transient transfection assays, X. laevis AHRR inhibitedTCDD-induced reporter gene expression mediated by either X.laevis AHR paralog, AHR1 ${alpha}$ or AHR1β. AHRR messenger RNA wasexpressed at low levels in embryos (Nieuwkoop-Faber stage 33–38;approximately 52 h.p.f.) and was induced approximately twofoldfollowing TCDD exposure (42 ng/g wet weight). In contrast, AHRRexhibited higher constitutive expression and was induced morethan threefold in tadpoles at stage 52–55 (prometamorphic; $~$ 4 weeks postfertilization) and in isolated viscera of stage62 tadpoles (in the metamorphic climax; $~$ 7 weeks postfertilization).Although the magnitude of induction was smaller, the temporalpattern of AHRR expression and inducibility resembled that ofCYP1A6. Thus, attenuated transcriptional activation of AHR targetgenes and low TCDD toxicity in X. laevis embryos cannot be explainedby constitutive, high-level expression of AHRR.

Key Words: dioxin; cytochrome P450; nonmammalian species; aryl hydrocarbon receptor; embryo.

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