We have identified and characterized a new orphan member of the nuclear hormone receptor superfamily, called MB67, which is predominantly expressed in liver. MB67 binds and transactivates the retinoic acid response elements that control expression of the retinoic acid receptor P2 and alcohol dehydrogenase 3 genes, both of which consist of a direct repeat hexamers related to the consensus AGGTCA, separated by 5 bp. MB67 binds these elements as a heterodimer with the 9-cis-retinoic acid receptor, RXR. However, MB67 does not bind or activate other retinoic acid response elements with alternative hexamer arrangements or any of several other wild-type and synthetic hormone response elements examined. The transactivation of retinoic acid response elements by MB67 is weaker than that conferred by the retinoic acid receptors but does not require the presence of all-trans retinoic acid, 9-cis-retinoic acid, or any exogenously added ligand. We propose that MB67 plays an important role in the complex network of proteins that govern response to retinoic acid and its metabolites.The nuclear hormone receptor superfamily is a large group of related transcription factors which includes members that bind a diverse array of ligands, including steroids, thyroid hormone (T3), all-trans retinoic acid (RA), 9-cis-retinoic acid (9-cis-RA), and vitamin D (reviewed in references 4,8,19,23,35). In mammals, approximately a dozen genes encode these conventional receptors. An even larger number of genes encode proteins known as orphan receptors (recently compiled in references 1 and 32). These orphans are structurally and functionally related to the conventional receptors but do not bind known ligands.The biological roles of the orphans are generally unknown. Some information is available for a limited number which were initially characterized prior to their identification as superfamily members. HNF-4, for example, was originally identified as a liver-specific basic transcription factor, with binding sites in several genes (59). Similarly, SF-I was identified as a factor associated with activation of expression of several steroidogenic enzymes (31). However, the majority of the orphans were isolated simply by cross-hybridization with probes derived from conventional receptors, and their functions remain largely undefined. By analogy with the conventional receptors, it has generally been thought that most of the orphans will eventually be demonstrated to be ligand-dependent transcriptional activators. However, recent results demonstrate that several, including 30,59), , and NGFI-B/Nur77 (13,48,70)
