肥胖和胰岛素抵抗中肝 X 受体对肝和脂肪的脂生成的相互调节作用。
Reciprocal regulation of hepatic and adipose lipogenesis by liver X receptors in obesity and insulin resistance.
机构信息
Howard Hughes Medical Institute and Department of Pathology and Laboratory Medicine, David Geffen School of Medicine at UCLA, Los Angeles, CA, USA.
出版信息
Cell Metab. 2013 Jul 2;18(1):106-17. doi: 10.1016/j.cmet.2013.04.021.
Abstract
Liver X receptors (LXRs) regulate lipogenesis and inflammation, but their contribution to the metabolic syndrome is unclear. We show that LXRs modulate key aspects of the metabolic syndrome in mice. LXRαβ-deficient-ob/ob (LOKO) mice remain obese but show reduced hepatic steatosis and improved insulin sensitivity compared to ob/ob mice. Impaired hepatic lipogenesis in LOKO mice is accompanied by reciprocal increases in adipose lipid storage, reflecting tissue-selective effects on the SREBP, PPARγ, and ChREBP lipogenic pathways. LXRs are essential for obesity-driven SREBP-1c and ChREBP activity in liver, but not fat. Furthermore, loss of LXRs in obesity promotes adipose PPARγ and ChREBP-β activity, leading to improved insulin sensitivity. LOKO mice also exhibit defects in β cell mass and proliferation despite improved insulin sensitivity. Our data suggest that sterol sensing by LXRs in obesity is critically linked with lipid and glucose homeostasis and provide insight into the complex relationships between LXR and insulin signaling.
摘要
肝 X 受体 (LXRs) 调节脂肪生成和炎症,但它们对代谢综合征的贡献尚不清楚。我们表明,LXRs 在小鼠中调节代谢综合征的关键方面。与 ob/ob 小鼠相比,LXRαβ 缺陷型 ob/ob (LOKO) 小鼠仍然肥胖,但肝脂肪变性减少,胰岛素敏感性提高。LOKO 小鼠的肝脂肪生成受损伴随着脂肪组织脂质储存的相应增加,反映了组织选择性对 SREBP、PPARγ 和 ChREBP 脂肪生成途径的影响。LXRs 对于肥胖驱动的 SREBP-1c 和 ChREBP 活性在肝脏中是必需的,但在脂肪中不是必需的。此外,肥胖中 LXRs 的缺失促进了脂肪组织中 PPARγ 和 ChREBP-β 的活性,从而提高了胰岛素敏感性。尽管胰岛素敏感性改善,LOKO 小鼠的β细胞质量和增殖也存在缺陷。我们的数据表明,肥胖中 LXR 的固醇感应与脂质和葡萄糖稳态密切相关,并为 LXR 和胰岛素信号之间的复杂关系提供了深入了解。
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