ISSN:
1573-4978
Keywords:
retinoic acid (RA)
;
retinoic acid receptor (RAR)
;
retinoid X receptor (RXR)
;
retinoic acid responsive element (RARE)
;
normal human keratinocytes (NHK)
Source:
Springer Online Journal Archives 1860-2000
Topics:
Biology
Notes:
Abstract The diversity of isoforms of retinoic acid (RA) receptors (RARs) and of DNA sequences of retinoic acid-responsive elements (RAREs) suggests the existence of selectivities in the RAR/RARE recognition or in the subsequent gene modulation. Such selectivities might be particularly important for RAREs involved in positive feedback, eg. the RARβ RARE. In the present work we found that in several epithelial cell lines, reporter constructs containing the RARβ RARE linked to the HSV-tk promoter were transactivated in the presence of RA by endogenous RARs and co-transfected RARα1 and RARβ2 isoforms, but not by RARγ1. On the contrary, this latter isoform behaved towards the RARβ RARE as an inhibitor of the transactivation produced by endogenous RARs and by cotransfected RARα1 and RARβ2. RARγ1 also behaved as an antagonist of the transactivation produced by cotransfected RXRα. The natural RARβ gene promoter or RARβ RARE tk constructs were not activated by the endogenous receptors of normal human keratinocytes (NHK), which are known to contain predominantly RARγ1. It was, however, possible to activate to a certain extent RARβ RARE-reporter constructs in NHK by co-transfecting RARα1, RARβ2 or RXRα. The antagonist behavior of RARγ1 towards the RARβ RARE may explain why in certain cell types such as keratinocytes, RARβ is neither expressed nor induced by RA.
Type of Medium:
Electronic Resource
URL:
http://dx.doi.org/10.1007/BF01006398
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