Abstract
The biological activity of the mouse orphan receptor Tr2-ll and its truncated isoform on a DR5-type retinoic acid response element (RARE) has been examined. An alternatively spliced variant of Tr2-l 1 has been identified and designated as Tr2-l 1-L As a result of alternative splicing, Tr2-ll-t mRNA encodes a truncated receptor with the complete ligandbinding domain deleted Protein expression of T12-11 and Tr2-ll-t transcripts has been confirmed using a prokaryotic expression system. Tr2-l 1 is able to repress RA induction of an RARE-tK-luc reporter, but has no effect on the tK promoter used in this reporter. In contrast to Tr211, Tr2-ll-t exerts a dramatic stimulatory effect on RA induction of the same RARE-tK-luc reporter. Gel-shift experiments provide evidence for an interaction of Tr2-ll with DNA fragments containing this RARE. Opposite roles of Tr2-ll and Tr2-ll-t on RA signaling pathways have been suggested.
Original language | English (US) |
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Pages (from-to) | A444 |
Journal | FASEB Journal |
Volume | 10 |
Issue number | 3 |
State | Published - Dec 1 1996 |