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The control of fatty acid and triglyceride synthesis in rat epididymal adipose tissue. Roles of coenzyme A derivatives, citrate and l-glycerol 3-phosphate

机译:大鼠附睾脂肪组织中脂肪酸和甘油三酸酯合成的控制。辅酶A衍生物,柠檬酸盐和1-磷酸3-甘油的作用

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p1. Methods are described for the extraction and assay of acetyl-CoA and of total acid-soluble and total acid-insoluble CoA derivatives in rat epididymal adipose tissue. 2. The concentration ranges of the CoA derivatives in fat pads incubated iin vitro/i under various conditions were: total acid-soluble CoA, 0·20–0·59mm; total acid-insoluble CoA, 0·08–0·23mm; acetyl-CoA, 0·03–0·14mm. 3. An investigation was made of some postulated mechanisms of control of fatty acid and triglyceride synthesis in rat epididymal fat pads incubated iin vitro/i. The concentrations of intermediates of possible regulatory significance were measured at various rates of fatty acid and triglyceride synthesis produced by the addition to the incubation medium (Krebs bicarbonate buffer containing glucose) of insulin, adrenaline, albumin, palmitate or acetate. 4. The whole-tissue concentrations of glucose 6-phosphate, l-glycerol 3-phosphate, citrate, acetyl-CoA, total acid-soluble CoA and total acid-insoluble CoA were assayed after 30 or 60min. incubation. The rates of fatty acid and triglyceride synthesis, calculated from the incorporation of [U?sup14/supC]glucose into fatty acids and glyceride glycerol respectively, and the rates of glucose uptake, lactate plus pyruvate output and glycerol output were measured over a 60min. incubation. 5. The rate of triglyceride synthesis could not be correlated with the concentrations of either l-glycerol 3-phosphate or long-chain fatty acyl-CoA (measured as total acid-insoluble CoA). Factor(s) other than the whole-tissue concentrations of these recognized precursors appear to be involved in the determination of the rate of triglyceride synthesis. 6. No relationship was found between the rate of fatty acid synthesis and the whole-tissue concentrations of the intermediates, citrate or acetyl-CoA, or with the two proposed effectors of acetyl-CoA carboxylase, citrate (as activator) or long-chain fatty acyl-CoA (as inhibitor). The control of fatty acid synthesis appears to reside in additional or alternative factors./p
机译:> 1。描述了在大鼠附睾脂肪组织中提取和测定乙酰辅酶A以及总酸溶性和总酸不溶性CoA衍生物的方法。 2.在不同条件下体外培养的脂肪垫中,CoA衍生物的浓度范围为:总酸溶性CoA,0·20-0·59mm;总酸不溶性CoA,0·08-0·23mm;乙酰-CoA,0·03-0·14mm。 3.研究了在体外培养的大鼠附睾脂肪垫中脂肪酸和甘油三酸酯合成的某些控制机制。通过在胰岛素,肾上腺素,白蛋白,棕榈酸酯或乙酸酯的培养培养基(含葡萄糖的克雷布斯碳酸氢盐缓冲液)中添加各种脂肪酸和甘油三酸酯合成速率,可以测量可能具有调控意义的中间体的浓度。 4.在30或60分钟后,测定6-磷酸葡萄糖,1-磷酸3-甘油,柠檬酸盐,乙酰基-CoA,总酸溶性CoA和总酸不溶性CoA的全组织浓度。孵化。脂肪酸和甘油三酸酯的合成速率,分别是根据将[U?sup14 C]葡萄糖掺入脂肪酸和甘油甘油酯中得出的,以及葡萄糖的摄取速率,乳酸和丙酮酸的输出以及甘油的输出在60分钟内测量。孵化。 5.甘油三酸酯的合成速率与1-甘油3-磷酸酯或长链脂肪酰基-CoA的浓度(以总的酸不溶性CoA测量)不相关。这些公认的前体的全组织浓度以外的因素似乎也参与了甘油三酸酯合成速率的确定。 6.脂肪酸合成速率与中间体柠檬酸盐或乙酰辅酶A的全组织浓度,或与乙酰辅酶A羧化酶,柠檬酸盐(作为激活剂)或长链的两种拟议效应子之间没有发现关系脂肪酰基辅酶A(作为抑制剂)。脂肪酸合成的控制似乎存在于其他或替代因素中。

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