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外文期刊>The biochemical journal
>Mouse white adipocytes and 3T3-L1 cells display an anomalous pattern of carnitine palmitoyltransferase (CPT) I isoform expression during differentiation: Inter-tissue and inter-species expression of CPT I and CPT II enzymes
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Mouse white adipocytes and 3T3-L1 cells display an anomalous pattern of carnitine palmitoyltransferase (CPT) I isoform expression during differentiation: Inter-tissue and inter-species expression of CPT I and CPT II enzymes
pThe outer mitochondrial membrane enzyme carnitine palmitoyltransferase I (CPT I) represents the initial and regulated step in the β-oxidation of fatty acids. It exists in at least two isoforms, denoted L (liver) and M (muscle) types, with very different kinetic properties and sensitivities to malonyl-CoA. Here we have examined the relative expression of the CPT I isoforms in two different models of adipocyte differentiation and in a number of rat tissues. Adipocytes from mice, hamsters and humans were also evaluated. Primary monolayer cultures of undifferentiated rat preadipocytes expressed solely L-CPT I, but significant levels of M-CPT I emerged after only 3 days of differentiation iin iv/iitro/i; in the mature cell M-CPT I predominated. In sharp contrast, the murine 3T3-L1 preadipocyte expressed essentially exclusively L-CPT I, both in the undifferentiated state and throughout the differentiation process iin iv/iitro/i. This was also true of the mature mouse white fat cell. Fully developed adipocytes from the hamster and human behaved similarly to those of the rat. Thus the mouse white fat cell differs fundamentally from those of the other species examined in terms of its choice of a key regulatory enzyme in fatty acid metabolism. In contrast, brown adipose tissue from all three rodents displayed the same isoform profiles, each expressing overwhelmingly M-CPT I. Northern blot analysis of other rat tissues established L-CPT I as the dominant isoform not only in liver but also in kidney, lung, ovary, spleen, brain, intestine and pancreatic islets. In addition to its primacy in skeletal muscle, heart and fat, M-CPT I was also found to dominate in the testis. The same inter-tissue isoform pattern (with the exception of white fat) was found in the mouse. Taken together, the data bring to light an intriguing divergence between white adipocytes of the mouse and other mammalian species. They also raise a cautionary note that should be considered in the choice of animal model used in further studies of fat cell physiology./p
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机译:线粒体外膜酶肉碱棕榈酰转移酶I(CPT I)代表脂肪酸β-氧化的起始步骤和调控步骤。它以至少两种同工型存在,表示为L(肝脏)和M(肌肉)类型,对丙二酰辅酶A的动力学性质和敏感性有很大不同。在这里,我们检查了两种不同的脂肪细胞分化模型和许多大鼠组织中CPT I同工型的相对表达。还评估了小鼠,仓鼠和人类的脂肪细胞。未分化大鼠前脂肪细胞的原代单层培养仅表达L-CPT I,但在 v itro 中仅3天的分化后便出现了显着水平的M-CPTI。在成熟细胞M-CPT中,我占主导地位。与之形成鲜明对比的是,鼠3T3-L1前脂肪细胞在未分化状态和整个 v itro 分化过程中基本上只表达L-CPTI。成熟的小鼠白色脂肪细胞也是如此。来自仓鼠和人的成熟脂肪细胞的行为与大鼠相似。因此,小鼠白脂肪细胞在脂肪酸代谢中关键调节酶的选择方面与其他种类的动物根本不同。相比之下,所有三只啮齿动物的棕色脂肪组织都显示相同的同工型,每个都绝大多数表达M-CPTI。对其他大鼠组织的Northern印迹分析表明,L-CPT I不仅在肝脏中而且在肾脏,肺中都是主要的同工型。 ,卵巢,脾脏,脑,肠和胰岛。除了在骨骼肌,心脏和脂肪中占主导地位,M-CPT I在睾丸中也占主导地位。在小鼠中发现了相同的组织间亚型模式(白色脂肪除外)。综上所述,数据揭示了小鼠的白色脂肪细胞与其他哺乳动物物种之间的有趣差异。他们还提出了一个警告说明,在选择用于进一步研究脂肪细胞生理学的动物模型时应考虑这一点。
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