造血细胞表达的内皮型一氧化氮合酶保护肝脏免受胰岛素抵抗。
Hematopoietic Cell-Expressed Endothelial Nitric Oxide Protects the Liver From Insulin Resistance.
机构信息
From the Department of Medicine, University of Washington, Seattle (B.P.D., R.M., T.K., S.A.G., T.V., T.W., K.D.O., K.E.B., A.C., F.K.).
Ben May Department for Cancer Research, University of Chicago, IL (L.B.).
出版信息
Arterioscler Thromb Vasc Biol. 2020 Mar;40(3):670-681. doi: 10.1161/ATVBAHA.119.313648. Epub 2020 Jan 30.
OBJECTIVE
Mice genetically deficient in endothelial nitric oxide synthase (Nos3) have fasting hyperinsulinemia and hepatic insulin resistance, indicating the importance of Nos3 (nitric oxide synthase) in maintaining metabolic homeostasis. Although the current paradigm holds that these metabolic effects are derived specifically from the expression of Nos3 in the endothelium, it has been established that bone marrow-derived cells also express Nos3. The aim of this study was to investigate whether bone marrow-derived cell Nos3 is important in maintaining metabolic homeostasis. Approach and Results: To test the hypothesis that bone marrow-derived cell Nos3 contributes to metabolic homeostasis, we generated chimeric male mice deficient or competent for Nos3 expression in circulating blood cells. These mice were placed on a low-fat diet for 5 weeks, a time period which is known to induce hepatic insulin resistance in global Nos3-deficient mice but not in wild-type C57Bl/6 mice. Surprisingly, we found that the absence of Nos3 in the bone marrow-derived component is associated with hepatic insulin resistance and that restoration of Nos3 in the bone marrow-derived component in global Nos3-deficient mice is sufficient to restore hepatic insulin sensitivity. Furthermore, we found that overexpression of Nos3 in bone marrow-derived component in wild-type mice attenuates the development of hepatic insulin resistance during high-fat feeding. Finally, compared with wild-type macrophages, the loss of macrophage Nos3 is associated with increased inflammatory responses to lipopolysaccharides and reduced anti-inflammatory responses to IL-4, a macrophage phenotype associated with the development of hepatic and systemic insulin resistance.
CONCLUSIONS
These results would suggest that the metabolic and hepatic consequences of high-fat feeding are mediated by loss of Nos3/nitric oxide actions in bone marrow-derived cells, not in endothelial cells.
目的
内皮型一氧化氮合酶(NOS3)基因缺失的小鼠表现为空腹高胰岛素血症和肝胰岛素抵抗,这表明 NOS3(一氧化氮合酶)在维持代谢稳态中的重要性。尽管目前的观点认为这些代谢效应是特定来源于内皮细胞中 NOS3 的表达,但已证实骨髓来源的细胞也表达 NOS3。本研究旨在探讨骨髓来源的细胞 NOS3 是否对维持代谢稳态具有重要作用。
方法和结果
为了验证骨髓来源的细胞 NOS3 有助于维持代谢稳态的假说,我们构建了骨髓细胞中 NOS3 表达缺失或功能正常的嵌合雄性小鼠。这些小鼠被置于低脂饮食 5 周,该时间段已知会诱导全身性 NOS3 缺失的小鼠发生肝胰岛素抵抗,但不会诱导野生型 C57Bl/6 小鼠发生肝胰岛素抵抗。令人惊讶的是,我们发现骨髓来源细胞中 NOS3 的缺失与肝胰岛素抵抗有关,并且在全身性 NOS3 缺失的小鼠中,将 NOS3 恢复到骨髓来源细胞中足以恢复肝胰岛素敏感性。此外,我们发现,在野生型小鼠中,骨髓来源细胞中 NOS3 的过表达可减轻高脂肪喂养期间肝胰岛素抵抗的发生。最后,与野生型巨噬细胞相比,巨噬细胞 NOS3 的缺失与对脂多糖的炎症反应增加以及对 IL-4 的抗炎反应减少有关,这种巨噬细胞表型与肝和全身胰岛素抵抗的发展有关。
结论
这些结果表明,高脂肪喂养的代谢和肝脏后果是通过骨髓来源细胞中 NOS3/一氧化氮作用的丧失介导的,而不是通过内皮细胞中 NOS3/一氧化氮作用的丧失介导的。
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