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大鼠脂肪细胞对油酸的摄取和结合确定了细胞脂肪酸摄取的双重途径。

Oleic acid uptake and binding by rat adipocytes define dual pathways for cellular fatty acid uptake.

作者信息

Stump D D, Fan X, Berk P D

机构信息

Division of Liver Disease, Department of Medicine, Mount Sinai School of Medicine, New York, NY 10029, USA.

出版信息

J Lipid Res. 2001 Apr;42(4):509-20.

Abstract

Oleic acid (OA) uptake by rat adipocytes and the proportions of intracellular unesterified [3H]OA and its 3H-labeled esters were determined over 300 s. Uptake was linear for 20;-30 s, with rapid esterification indicating entry into normal metabolic pathways. Initial rates of OA uptake and its binding to plasma membranes were studied over a spectrum of oleic acid:bovine serum albumin (BSA) ratios, and expressed as functions of unbound OA concentrations calculated with both the 1971 OA:BSA association constants of Spector, Fletcher, and Ashbrook and more recent constants (e.g., the 1993 constants of Richieri, Anel, and Kleinfeld), which generate concentrations 10- to 100-fold lower. In either case, uptake was the sum of saturable and linear processes, with > or =90% occurring via the saturable pathway when the OA:BSA molar ratio was within the physiologic range (0.5;-3.0). Within this range, rate constants for saturable transmembrane influx (k(s)), calculated from both sets of constants, were similar (2.9 s(-1)) and were 10- to 30-fold faster than those for nonsaturable uptake (k(ns) = 0.26;-0.10 s(-1), t1/2 = 2.7;-6.6 s, based on the constants of Spector et al. and Richieri et al., respectively). The rate of oleic acid flip-flop into rat adipocytes (k(ff) = 0.16 +/- 0.02 s(-1), t1/2 = 4.3 +/- 0.5 s), computed from published data, was similar to k(ns). Thus, OA uptake occurs by both a saturable mechanism and passive flip-flop. This conclusion is independent of the OA:BSA association constants used to analyze the experimental measurements.

摘要

在300秒内测定了大鼠脂肪细胞对油酸(OA)的摄取以及细胞内未酯化的[3H]OA及其3H标记酯的比例。摄取在20 - 30秒内呈线性,快速酯化表明进入正常代谢途径。在一系列油酸与牛血清白蛋白(BSA)比例下研究了OA摄取及其与质膜结合的初始速率,并表示为根据Spector、Fletcher和Ashbrook 1971年的OA:BSA缔合常数以及更新的常数(例如Richieri、Anel和Kleinfeld 1993年的常数)计算的未结合OA浓度的函数,这些常数产生的浓度低10至100倍。在任何一种情况下,摄取都是可饱和过程和线性过程的总和,当OA:BSA摩尔比在生理范围内(0.5 - 3.0)时,≥90%通过可饱和途径发生。在此范围内,根据两组常数计算的可饱和跨膜流入速率常数(k(s))相似(2.9 s(-1)),比非可饱和摄取速率常数(k(ns) = 0.26 - 0.10 s(-1),t1/2 = 2.7 - 6.6 s,分别基于Spector等人和Richieri等人的常数)快10至30倍。根据已发表的数据计算,油酸翻转进入大鼠脂肪细胞的速率(k(ff) = 0.16 ± 0.02 s(-1),t1/2 = 4.3 ± 0.5 s)与k(ns)相似。因此,OA摄取通过可饱和机制和被动翻转两种方式发生。这一结论与用于分析实验测量的OA:BSA缔合常数无关。

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