M A Puchowicz, I R Bederman, B Comte, D Yang, F David, E Stone, K Jabbour, D H Wasserman, H Brunengraber
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引用次数: 34
摘要
通过质量同位素分布分析(MIDA)测量脂肪酸或胆固醇标记的[(13)C]醋酸,假设在所有肝细胞中脂肪生成乙酰辅酶a持续富集。如果醋酸盐被肝脏摄取和释放导致乙酰辅酶a富集的跨肝梯度,情况就不是这样了。神志清醒的狗预先安装了经肝导管,注入葡萄糖和[1,2 -(13)C(2)]醋酸盐。在动脉(17 μ m, 36%)、门静脉(61 μ m, 5%)中测定醋酸盐的稳定浓度和富集程度。4%),肝静脉(17 μ m, 1.0%),并计算混合血进入肝脏(53 μ m, 7.4%)。我们还测量了肠道和肝脏中丙酸和丁酸的平衡。肠道释放的丙酸盐和丁酸盐全部被肝脏吸收。醋酸酯浓度降低三倍,醋酸酯富集降低七倍,这强烈表明脂肪生成乙酰辅酶a的富集在整个肝脏中减少。因此,通过MIDA在体内测量肝脏脂肪生成的分数可能被低估了。
Zonation of acetate labeling across the liver: implications for studies of lipogenesis by MIDA.
Measurement of fractional lipogenesis by mass isotopomer distribution analysis (MIDA) of fatty acids or cholesterol labeled from [(13)C]acetate assumes constant enrichment of lipogenic acetyl-CoA in all hepatocytes. This would not be the case if uptake and release of acetate by the liver resulted in transhepatic gradients of acetyl-CoA enrichment. Conscious dogs, prefitted with transhepatic catheters, were infused with glucose and [1, 2-(13)C(2)]acetate. Stable concentrations and enrichments of acetate were measured in artery (17 microM, 36%), portal vein (61 microM, 5. 4%), and hepatic vein (17 microM, 1.0%) and were computed for mixed blood entering the liver (53 microM, 7.4%). We also measured balances of propionate and butyrate across gut and liver. All gut release of propionate and butyrate is taken up by the liver. The threefold decrease in acetate concentration and the sevenfold decrease in acetate enrichment across the liver strongly suggest that the enrichment of lipogenic acetyl-CoA decreases across the liver. Thus fractional hepatic lipogenesis measured in vivo by MIDA may be underestimated.
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