Dominant negative retinoid X receptor beta inhibits retinoic acid-responsive gene regulation in embryonal carcinoma cells.

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Mol Cell Biol. 1994 January; 14(1): 360-372

Dominant negative retinoid X receptor beta inhibits retinoic acid-responsive gene regulation in embryonal carcinoma cells.

S Minucci, D J Zand, A Dey, M S Marks, T Nagata, J F Grippo and K Ozato

Laboratory of Molecular Growth Regulation, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892.

ABSTRACT

Retinoid X receptors (RXRs) heterodimerize with multiple nuclearhormone receptors and are thought to exert pleiotropic functions.To address the role of RXRs in retinoic acid- (RA) mediatedgene regulation, we designed a dominant negative RXR beta. Thismutated receptor, termed DBD-, lacked the DNA binding domainbut retained the ability to dimerize with partner receptors,resulting in formation of nonfunctional dimers. DBD- was transfectedinto P19 murine embryonal carcinoma (EC) cells, in which reporterscontaining the RA-responsive elements (RAREs) were activatedby RA through the activity of endogenous RXR-RA receptor (RAR)heterodimers. We found that DBD- had a dominant negative activityon the RARE reporter activity in these cells. P19 clones stablyexpressing DBD- were established; these clones also failed toactivate RARE-driven reporters in response to RA. Further, thesecells were defective in RA-induced mRNA expression of Hox-1.3and RAR beta, as well as in RA-induced down-regulation of Oct3mRNA. Gel mobility shift assays demonstrated that RA treatmentof control P19 cells induces RARE-binding activity, of whichRXR beta is a major component. However, the RA-induced bindingactivity was greatly reduced in cells expressing DBD-. By genomicfootprinting, we show that RA treatment induces in vivo occupancyof the RARE in the endogenous RAR beta gene in control P19 cellsbut that this occupancy is not observed with the DBD- cells.These data provide evidence that the dominant negative activityof DBD- is caused by the lack of receptor binding to targetDNA. Finally, we show that in F9 EC cells expression of DBD-leads to inhibition of the growth arrest that accompanies RA-induceddifferentiation. Taken together, these results demonstrate thatRXR beta and partner receptors play a central role in RA-mediatedgene regulation and in the control of growth and differentiationin EC cells.

Mol Cell Biol. 1994 January; 14(1): 360-372

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