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与短链饱和脂肪酸不同,硬脂酸在培养的大鼠肝细胞中用于三酰甘油合成和β-氧化的利用率很低。

Stearic acid unlike shorter-chain saturated fatty acids is poorly utilized for triacylglycerol synthesis and beta-oxidation in cultured rat hepatocytes.

作者信息

Pai T, Yeh Y Y

机构信息

Department of Nutrition, Pennsylvania State University, University Park, 16802, USA.

出版信息

Lipids. 1996 Feb;31(2):159-64. doi: 10.1007/BF02522615.

Abstract

Utilization of stearate as compared to various saturated fatty acids for cholesterol and lipid synthesis and beta-oxidation was determined in primary culture of rat hepatocytes. At 0.5 mmol/L in the medium, stearate (18:0) adequately solubilized by albumin was less inhibitory to cholesterol synthesis from [2-14C] acetate than myristate (14:0) and palmitate (16:0) (68% vs. 91 and 88% inhibition, respectively). The rate of incorporation into cholesterol from [1-14C] stearate (3.0 +/- 0.6 nmol/mg protein/4 h) was 37-, 1.8-, and 7.8-fold of that from myristate, palmitate, and oleate, respectively. Conversely, the rate of [1-14C] stearate incorporation into total glycerolipids was 88-90% lower than that of labeled palmitate, myristate, and oleate. The rate of [1-14C] stearate incorporation into triacylglycerol (3.6 +/- 0.4 nmol/mg protein/4 h) was 6-8% of that from myristate, palmitate, oleate, and linoleate. The rate of stearate incorporation into phospholipids was the lowest among tested fatty acids, whereas the rate of mono- and diacylglycerol synthesis was the highest with stearate treatment. The rate of beta-oxidation as measured by CO2 and acid soluble metabolite production was also the lowest with [1-14C] stearate treatment at 22.7 nmol/mg protein/4 h, which was 35-40% of those from other [1-14C] labeled fatty acids. A greater proportion of stearate than other fatty acids taken up by the hepatocytes remained free and was not metabolized. Clearly, stearate as compared to shorter-chain saturated fatty acids was less efficiently oxidized and esterified to triacylglycerol in cultured rat hepatocytes.

摘要

在大鼠肝细胞原代培养中,测定了硬脂酸与各种饱和脂肪酸相比用于胆固醇和脂质合成及β-氧化的情况。在培养基中浓度为0.5 mmol/L时,由白蛋白充分溶解的硬脂酸(18:0)对[2-14C]乙酸盐合成胆固醇的抑制作用小于肉豆蔻酸(14:0)和棕榈酸(16:0)(分别为68%抑制率,而肉豆蔻酸和棕榈酸的抑制率分别为91%和88%)。[1-14C]硬脂酸掺入胆固醇的速率(3.0±0.6 nmol/mg蛋白质/4小时)分别是肉豆蔻酸、棕榈酸和油酸的37倍、1.8倍和7.8倍。相反,[1-14C]硬脂酸掺入总甘油脂质的速率比标记的棕榈酸、肉豆蔻酸和油酸低88 - 90%。[1-14C]硬脂酸掺入三酰甘油的速率(3.6±0.4 nmol/mg蛋白质/4小时)是肉豆蔻酸、棕榈酸、油酸和亚油酸的6 - 8%。硬脂酸掺入磷脂的速率在测试的脂肪酸中最低,而单酰甘油和二酰甘油合成的速率在硬脂酸处理时最高。以二氧化碳和酸溶性代谢产物产生量衡量的β-氧化速率在[1-14C]硬脂酸处理时也最低,为22.7 nmol/mg蛋白质/4小时,是其他[1-14C]标记脂肪酸的35 - 40%。肝细胞摄取的硬脂酸比其他脂肪酸有更大比例保持游离状态且未被代谢。显然,与短链饱和脂肪酸相比,硬脂酸在培养的大鼠肝细胞中氧化和酯化生成三酰甘油的效率较低。

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