Center for Cancer Research, National Cancer, Institute-Frederick, Frederick, MD 21702-1201, USA.
FASEB J. 2012 Jan;26(1):309-23. doi: 10.1096/fj.11-190892. Epub 2011 Oct 11.
Obesity is a major health concern that contributes to the development of diabetes, hyperlipidemia, coronary artery disease, and cancer. Id proteins are helix-loop-helix transcription factors that regulate the proliferation and differentiation of cells from multiple tissues, including adipocytes. We screened mouse tissues for the expression of Id1 and found that Id1 protein is highly expressed in brown adipose tissue (BAT) and white adipose tissue (WAT), suggesting a role for Id1 in adipogenesis and cell metabolism. Id1(-/-) mice are viable but show a significant reduction in fat mass (P<0.005) over the life of the animal that was not due to decreased number of adipocytes. Analysis of Id1(-/-) mice revealed higher energy expenditure, increased lipolysis, and fatty acid oxidation, resulting in reduced triglyceride accumulation in WAT compared to Id1(+/+) mice. Serum levels of triglycerides (193.9±32.2 vs. 86.5±33.8, P<0.0005), cholesterol (189.4±33.8 vs. 110.6±8.23, P<0.0005) and leptin (1263±835 vs. 222±260, P<0.005) were significantly lower in aged Id1(-/-) mice compared to Id1(+/+) mice. Id1-deficient mice have higher resting (P<0.005) and total (P<0.05) O(2) consumption and lower respiratory exchange ratio (P<0.005), confirming that Id1(-/-) mice use a higher proportion of lipid as an energy source for the increased energy expenditure. The expression of PGC1α and UCP1 were 2- to 3-fold up-regulated in Id1(-/-) BAT, suggesting that loss of Id1 increases thermogenesis. As a consequence of higher energy expenditure and reduced fat mass, Id1(-/-) mice displayed enhanced insulin sensitivity. Id1 deficiency protected mice against age- and high-fat-diet-induced adiposity, insulin resistance, and hepatosteatosis. Our findings suggest that Id1 plays a critical role in the regulation of energy homeostasis and could be a potential target in the treatment of insulin resistance and fatty liver disease.
肥胖是一个主要的健康问题,它会导致糖尿病、高血脂、冠心病和癌症的发生。Id 蛋白是螺旋-环-螺旋转录因子,可调节多种组织(包括脂肪细胞)的细胞增殖和分化。我们筛选了小鼠组织中 Id1 的表达情况,发现 Id1 蛋白在棕色脂肪组织 (BAT) 和白色脂肪组织 (WAT) 中高度表达,提示 Id1 在脂肪生成和细胞代谢中发挥作用。Id1(-/-) 小鼠能够存活,但在整个动物生命周期中,脂肪量显著减少(P<0.005),这不是由于脂肪细胞数量减少所致。对 Id1(-/-) 小鼠的分析表明,能量消耗更高,脂肪分解和脂肪酸氧化增加,导致 WAT 中甘油三酯的积累减少。与 Id1(+/+) 小鼠相比,Id1(-/-) 小鼠的血清甘油三酯水平(193.9±32.2 与 86.5±33.8,P<0.0005)、胆固醇(189.4±33.8 与 110.6±8.23,P<0.0005)和瘦素(1263±835 与 222±260,P<0.005)水平显著降低。与 Id1(+/+) 小鼠相比,老龄 Id1(-/-) 小鼠的静止(P<0.005)和总(P<0.05)耗氧量以及呼吸交换率(P<0.005)均升高,证实 Id1(-/-) 小鼠使用更高比例的脂质作为能量来源以满足增加的能量消耗。Id1(-/-) BAT 中 PGC1α 和 UCP1 的表达上调 2-3 倍,提示 Id1 缺失增加了产热。由于能量消耗增加和脂肪量减少,Id1(-/-) 小鼠表现出胰岛素敏感性增强。Id1 缺乏可防止小鼠因年龄增长和高脂肪饮食引起的肥胖、胰岛素抵抗和肝脂肪变性。我们的研究结果表明,Id1 在调节能量平衡中发挥关键作用,可能成为治疗胰岛素抵抗和脂肪肝疾病的潜在靶点。
