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使用(R)-2-溴棕榈酸示踪剂在体内评估组织特异性血浆游离脂肪酸利用的新方法的开发与初步评估。

Development and initial evaluation of a novel method for assessing tissue-specific plasma free fatty acid utilization in vivo using (R)-2-bromopalmitate tracer.

作者信息

Oakes N D, Kjellstedt A, Forsberg G B, Clementz T, Camejo G, Furler S M, Kraegen E W, Olwegård-Halvarsson M, Jenkins A B, Ljung B

机构信息

Department of Pharmacology, Astra-Hässle AB, S-431 83 Mölndal, Sweden.

出版信息

J Lipid Res. 1999 Jun;40(6):1155-69.

Abstract

We describe a method for assessing tissue-specific plasma free fatty acid (FFA) utilization in vivo using a non-beta-oxidizable FFA analog, [9,10-3H]-(R)-2-bromopalmitate (3H-R-BrP). Ideally 3H-R-BrP would be transported in plasma, taken up by tissues and activated by the enzyme acyl-CoA synthetase (ACS) like native FFA, but then 3H-labeled metabolites would be trapped. In vitro we found that 2-bromopalmitate and palmitate compete equivalently for the same ligand binding sites on albumin and intestinal fatty acid binding protein, and activation by ACS was stereoselective for the R-isomer. In vivo, oxidative and non-oxidative FFA metabolism was assessed in anesthetized Wistar rats by infusing, over 4 min, a mixture of 3H-R-BrP and [U-14C] palmitate (14C-palmitate). Indices of total FFA utilization (Rf) and incorporation into storage products (Rfs') were defined, based on tissue concentrations of 3H and 14C, respectively, 16 min after the start of tracer infusion. Rf, but not Rfs', was substantially increased in contracting (sciatic nerve stimulated) hindlimb muscles compared with contralateral non-contracting muscles. The contraction-induced increases in R*f were completely prevented by blockade of beta-oxidation with etomoxir. These results verify that 3H-R-BrP traces local total FFA utilization, including oxidative and non-oxidative metabolism. Separate estimates of the rates of loss of 3H activity indicated effective 3H metabolite retention in most tissues over a 16-min period, but appeared less effective in liver and heart. In conclusion, simultaneous use of 3H-R-BrP and [14C]palmitate tracers provides a new useful tool for in vivo studies of tissue-specific FFA transport, utilization and metabolic fate, especially in skeletal muscle and adipose tissue.

摘要

我们描述了一种使用非β-氧化可利用的游离脂肪酸(FFA)类似物[9,10-³H]-(R)-2-溴软脂酸(³H-R-BrP)在体内评估组织特异性血浆游离脂肪酸利用情况的方法。理想情况下,³H-R-BrP会在血浆中运输,被组织摄取并像天然游离脂肪酸一样被酰基辅酶A合成酶(ACS)激活,但随后³H标记的代谢产物会被捕获。在体外,我们发现2-溴软脂酸和软脂酸在白蛋白和肠脂肪酸结合蛋白上竞争相同的配体结合位点,且ACS对R-异构体的激活具有立体选择性。在体内,通过在4分钟内输注³H-R-BrP和[U-¹⁴C]软脂酸(¹⁴C-软脂酸)的混合物,对麻醉的Wistar大鼠的氧化和非氧化游离脂肪酸代谢进行了评估。基于示踪剂输注开始后16分钟时³H和¹⁴C的组织浓度,分别定义了总游离脂肪酸利用率(Rf)和掺入储存产物的指标(Rfs')。与对侧非收缩性肌肉相比,收缩(坐骨神经刺激)的后肢肌肉中的Rf显著增加,但Rfs'没有增加。用依托莫昔芬阻断β-氧化可完全阻止收缩诱导的R*f增加。这些结果证实³H-R-BrP可追踪局部总游离脂肪酸利用情况,包括氧化和非氧化代谢。对³H活性损失率的单独估计表明,在16分钟的时间段内,³H代谢产物在大多数组织中有效保留,但在肝脏和心脏中似乎效果较差。总之,同时使用³H-R-BrP和[¹⁴C]软脂酸示踪剂为体内研究组织特异性游离脂肪酸转运、利用和代谢命运提供了一种新的有用工具,特别是在骨骼肌和脂肪组织中。

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