Saha Pradip K, Kojima Hideto, Martinez-Botas Javier, Sunehag Agneta L, Chan Lawrence
Division of Diabetes, Endocrinology and Metabolism, Department of Medicine, Baylor College of Medicine, Houston, TX 77030, USA.
J Biol Chem. 2004 Aug 20;279(34):35150-8. doi: 10.1074/jbc.M405499200. Epub 2004 Jun 14.
Targeted disruption of the lipid droplet protein, perilipin, in mice leads to constitutional lipolysis associated with marked reduction in white adipose tissue as a result of unbridled lipolysis. To investigate the metabolic adaptations in response to the constitutive lipolysis, we studied perilipin-null (plin(-/-)) mice in terms of their fatty acid oxidation and glycerol and glucose metabolism homeostasis by using dynamic biochemical testing and clamp and tracer infusion methods. plin(-/-) mice showed increased beta-oxidation in muscle, liver, and adipose tissue resulting from a coordinated regulation of the enzymes and proteins involved in beta-oxidation. The increased beta-oxidation helped remove the extra free fatty acids created by the constitutive lipolysis. An increase in the expression of the transcripts for uncoupling proteins-2 and -3 also accompanied this increase in fatty acid oxidation. Adult plin(-/-) mice had normal plasma glucose but a reduced basal hepatic glucose production (46% that of plin(+/+)). Insulin infusion during low dose hyperinsulinemic-euglycemic clamp further lowered the glucose production in plin(-/-) mice, but plin(-/-) mice also showed a 36% decrease (p < 0.007) in glucose disposal rate during the low dose insulin clamp, indicating peripheral insulin resistance. However, compared with plin(+/+) mice, 14-week-old plin(-/-) mice showed no significant difference in glucose disposal rate during the high dose hyperinsulinemic clamp, whereas 42-week-old plin(-/-) mice displayed significant insulin resistance on high dose hyperinsulinemic clamp. Despite increasing insulin resistance with age, plin(-/-) mice at different ages maintained a normal glucose response during an intraperitoneal glucose tolerance curve, being compensated by the increased beta-oxidation and reduced hepatic glucose production. These experiments uncover the metabolic adaptations associated with the constitutional lipolysis in plin(-/-) mice that allowed the mice to continue to exhibit normal glucose tolerance in the presence of peripheral insulin resistance.
在小鼠中靶向破坏脂滴蛋白围脂滴蛋白会导致持续性脂肪分解,由于不受控制的脂肪分解,白色脂肪组织显著减少。为了研究对持续性脂肪分解的代谢适应性,我们通过动态生化检测、钳夹和示踪剂输注方法,研究了围脂滴蛋白基因敲除(plin(-/-))小鼠的脂肪酸氧化以及甘油和葡萄糖代谢稳态。plin(-/-)小鼠的肌肉、肝脏和脂肪组织中β-氧化增加,这是由参与β-氧化的酶和蛋白质的协同调节所致。增加的β-氧化有助于清除持续性脂肪分解产生的额外游离脂肪酸。解偶联蛋白-2和-3转录本的表达增加也伴随着脂肪酸氧化的增加。成年plin(-/-)小鼠血糖正常,但基础肝葡萄糖生成减少(为plin(+/+)小鼠的46%)。在低剂量高胰岛素-正常血糖钳夹期间输注胰岛素进一步降低了plin(-/-)小鼠的葡萄糖生成,但plin(-/-)小鼠在低剂量胰岛素钳夹期间葡萄糖处置率也降低了36%(p < 0.007),表明存在外周胰岛素抵抗。然而,与plin(+/+)小鼠相比,14周龄的plin(-/-)小鼠在高剂量高胰岛素钳夹期间葡萄糖处置率无显著差异,而42周龄的plin(-/-)小鼠在高剂量高胰岛素钳夹时表现出显著的胰岛素抵抗。尽管随着年龄增长胰岛素抵抗增加,但不同年龄的plin(-/-)小鼠在腹腔葡萄糖耐量曲线期间保持正常的葡萄糖反应,通过增加的β-氧化和减少的肝葡萄糖生成得到补偿。这些实验揭示了plin(-/-)小鼠中与持续性脂肪分解相关的代谢适应性,使小鼠在存在外周胰岛素抵抗的情况下仍能继续表现出正常的葡萄糖耐量。