Li Qingtian, Chu Mei-Jin, Xu Jianming
Department of Molecular and Cellular Biology, Baylor College of Medicine, One Baylor Plaza, Houston, TX 77030, USA.
Mol Cell Biol. 2007 Dec;27(23):8073-86. doi: 10.1128/MCB.00451-07. Epub 2007 Oct 1.
Although the LXXLL motif of nuclear receptor (NR) coactivators is essential for interaction with NRs, its role has not been assessed in unbiased animal models. The nuclear receptor coactivator 6 (NCoA6; also AIB3, PRIP, ASC-2, TRBP, RAP250, or NRC) is a coactivator containing an N-terminal LXXLL-1 (L1) and a C-terminal L2. L1 interacts with many NRs, while L2 interacts with the liver X receptor alpha (LXRalpha) and the estrogen receptor alpha (ERalpha). We generated mice in which L2 was mutated into AXXAL (L2m) to disrupt its interaction with LXRalpha and ERalpha. NCoA6(L2m/L2m) mice exhibited normal reproduction, mammary gland morphogenesis, and ERalpha target gene expression. In contrast, when treated with an LXRalpha agonist, lipogenesis and the LXRalpha target gene expression were significantly reduced in NCoA6(L2m/L2m) mice. The induction of Cyp7A1 expression by a high-cholesterol diet was impaired in NCoA6(L2m/L2m) mice, which reduced bile acid synthesis in the liver and excretion in the feces and resulted in cholesterol accumulation in the liver and blood. These results demonstrate that L2 plays a tissue- and NR-specific role: it is required for NCoA6 to mediate LXRalpha-regulated lipogenesis and cholesterol/bile acid homeostasis in the liver but not required for ERalpha function in the mammary gland.
尽管核受体(NR)共激活因子的LXXLL基序对于与NR相互作用至关重要,但其在无偏差动物模型中的作用尚未得到评估。核受体共激活因子6(NCoA6;也称为AIB3、PRIP、ASC-2、TRBP、RAP250或NRC)是一种共激活因子,包含一个N端LXXLL-1(L1)和一个C端L2。L1与许多NR相互作用,而L2与肝脏X受体α(LXRα)和雌激素受体α(ERα)相互作用。我们构建了L2突变为AXXAL(L2m)以破坏其与LXRα和ERα相互作用的小鼠。NCoA6(L2m/L2m)小鼠表现出正常的繁殖、乳腺形态发生和ERα靶基因表达。相比之下,用LXRα激动剂处理时,NCoA6(L2m/L2m)小鼠的脂肪生成和LXRα靶基因表达显著降低。高胆固醇饮食诱导的Cyp7A1表达在NCoA6(L2m/L2m)小鼠中受损,这降低了肝脏中胆汁酸的合成和粪便中的排泄,并导致肝脏和血液中胆固醇积累。这些结果表明L2发挥着组织和NR特异性作用:它是NCoA6介导肝脏中LXRα调节的脂肪生成和胆固醇/胆汁酸稳态所必需的,但不是乳腺中ERα功能所必需的。