A large number of physiological processes in the adult liver are regulated by nuclear receptors that require heterodimerization with retinoid X receptors (RXRs). In this study, we have used cre-mediated recombination to disrupt the mouse RXR␣ gene specifically in hepatocytes. Although such mice are viable, molecular and biochemical parameters indicate that every one of the examined metabolic pathways in the liver (mediated by RXR heterodimerization with PPAR␣, CAR, PXR, LXR, and FXR) is compromised in the absence of RXR␣. These data demonstrate the presence of a complex circuitry in which RXR␣ is integrated into a number of diverse physiological pathways as a common regulatory component of cholesterol, fatty acid, bile acid, steroid, and xenobiotic metabolism and homeostasis.Members of the nuclear receptor family regulate a broad range of developmental and physiological processes by binding to DNA response elements and regulating transcriptional activation (7). The retinoid X receptors (RXRs) are unique among the nuclear receptors in that they bind DNA as a homodimer and are required as a heterodimeric partner for a number of additional nuclear receptors to bind DNA (19). The latter receptors, termed the class II nuclear receptor subfamily, include many which are established or implicated as important regulators of gene expression in the liver (reviewed below). There are three RXR genes (18), coding for RXR␣, -, and -␥, all of which are able to heterodimerize with any of the class II receptors, although there appear to be preferences for distinct RXR subtypes by partner receptors in vivo (6).The physiological processes that are regulated by the class II receptors in the liver are diverse. LXR␣ is activated by oxycholesterol and promotes cholesterol metabolism (22). FXR (also known as RIP14) is part of an interrelated process, in that FXR is activated by bile acids (the end product of cholesterol metabolism) (17,21,34), which serve to inhibit cholesterol catabolism. CAR is involved in phenobarbital induction of the cytochrome P450 2B10 (Cyp2B10) gene (9), which encodes a drug-and xenobiotic-metabolic enzyme. Interestingly, CAR has constitutively activity, but becomes inactive in response to the steroid androstane (8). PXR is activated by a wide spectrum of steroids, and induces the Cyp3A gene (Cyp3A1 in mice; Cyp3A4 in humans) which encodes a broad-spectrum oxidase that is responsible for steroid degradation and for the catabolism of numerous pharmaceutical compounds (2, 11). PPAR␣ is activated by leukotriene B4 and by synthetic peroxisome proliferators, such as fibrates, and controls the expression of several genes which are related to fatty acid metabolism and processing (28). Although not discussed further in the context of this study, other class II nuclear receptors, including the retinoic acid and thyroid hormone receptors, are also likely to be important regulators of liver metabolism.In the adult liver, RXR␣ is the most abundant of the three RXRs (18), suggesting that it might have a prominent role in...
