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RARs and RXRs: evidence for two autonomous transactivation functions (AF‐1 and AF‐2) and heterodimerization in vivo

We have previously reported that the AB regions of retinoic acid receptors (RARs and RXRs) contain a transcriptional activation function capable of modulating the activity of the ligand‐dependent activation function present in the C‐terminal DE regions of these receptors. However, we could not demon...

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Bibliographic Details
Published in:The EMBO journal 1993-06, Vol.12 (6), p.2349-2360
Main Authors: Nagpal, S., Friant, S., Nakshatri, H., Chambon, P.
Format: Article
Language:English
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Summary:We have previously reported that the AB regions of retinoic acid receptors (RARs and RXRs) contain a transcriptional activation function capable of modulating the activity of the ligand‐dependent activation function present in the C‐terminal DE regions of these receptors. However, we could not demonstrate that these AB regions possess an autonomous activation function similar to the AF‐1s found in the AB regions of steroid hormone receptors. Using the mouse CRBPII promoter as a reporter gene, we now report that the AB regions of RAR alpha, beta and gamma, as well as those of RXR alpha and gamma, contain an autonomous, ligand‐independent activation function, AF‐1, which can efficiently synergize with AF‐2s. Moreover, AF‐1s account for the ligand‐independent, constitutive activation of transcription by RXR alpha and gamma. We also show that RARs and RXRs preferentially heterodimerize in solution in cultured cells in vivo, through the dimerization interface present in their E region, irrespective of the presence of all‐trans or 9‐cis retinoic acid. Furthermore, our results indicate that homodimeric interactions are not observed in cultured cells in vivo under conditions where heterodimeric interactions readily occur, which is in agreement with previous observations showing the preferential binding of RAR‐RXR heterodimers to RA response elements in vitro.
ISSN:0261-4189
1460-2075
DOI:10.1002/j.1460-2075.1993.tb05889.x