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首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Saturable transport of insulin from plasma into the central nervous system of dogs in vivo. A mechanism for regulated insulin delivery to the brain.
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Saturable transport of insulin from plasma into the central nervous system of dogs in vivo. A mechanism for regulated insulin delivery to the brain.

机译:体内胰岛素从血浆到血浆中枢神经系统的饱和运输。一种调节胰岛素向大脑输送的机制。

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By acting in the central nervous system, circulating insulin may regulate food intake and body weight. We have previously shown that the kinetics of insulin uptake from plasma into cerebrospinal fluid (CSF) can best be explained by passage through an intermediate compartment. To determine if transport kinetics into this compartment were consistent with an insulin receptor-mediated transport process, we subjected overnight fasted, anesthetized dogs to euglycemic intravenous insulin infusions for 90 min over a wide range of plasma insulin levels (69-5,064 microU/ml) (n = 10). Plasma and CSF samples were collected over 8 h for determination of immunoreactive insulin levels, and the kinetics of insulin uptake from plasma into CSF were analyzed using a compartmental model with three components (plasma-->intermediate compartment-->CSF). By sampling frequently during rapid changes of plasma and CSF insulin levels, we were able to precisely estimate three parameters (average standard deviation 14%) characterizing the uptake of insulin from plasma, through the intermediate compartment and into CSF (k1k2); insulin entry into CSF and insulin clearance from the intermediate compartment (k2 + k3); and insulin clearance from CSF (k4). At physiologic plasma insulin levels (80 +/- 7.4 microU/ml), k1k2 was determined to be 10.7 x 10(-6) +/- 1.3 x 10(-6) min-2. With increasing plasma levels, however, k1k2 decreased progressively, being reduced sevenfold at supraphysiologic levels (5,064 microU/ml). The apparent KM of this saturation curve was 742 microU/ml (approximately 5 nM). In contrast, the rate constants for insulin removal from the intermediate compartment and from CSF did not vary with plasma insulin (k2 + k3 = 0.011 +/- 0.0019 min-1 and k4 = 0.046 +/- 0.021 min-1). We conclude that delivery of plasma insulin into the central nervous system is saturable, and is likely facilitated by an insulin-receptor mediated transport process.
机译:通过作用于中枢神经系统,循环中的胰岛素可以调节食物的摄入量和体重。先前我们已经表明,胰岛素从血浆中摄取到脑脊液(CSF)中的动力学可以最好地通过中间隔室来解释。为了确定进入该腔室的运输动力学是否与胰岛素受体介导的运输过程一致,我们对禁食,麻醉的犬进行了整夜的正常血糖静脉内胰岛素输注,历时90分钟,血浆胰岛素水平较高(69-5,064 microU / ml) (n = 10)。在8小时内收集血浆和CSF样品以测定免疫反应性胰岛素水平,并使用具有三种成分的血浆模型(血浆->中级腔室-> CSF)分析血浆从血浆吸收到CSF中的动力学。通过在血浆和CSF胰岛素水平快速变化期间进行频繁采样,我们能够精确估计三个参数(平均标准偏差14%),这些参数表征了胰岛素从血浆,通过中间腔室并进入CSF(k1k2)的吸收。胰岛素进入脑脊液和胰岛素从中间腔室清除(k2 + k3);和从CSF中清除胰岛素(k4)。在生理血浆胰岛素水平(80 +/- 7.4 microU / ml)下,k1k2被确定为10.7 x 10(-6)+/- 1.3 x 10(-6)min-2。但是,随着血浆水平的升高,k1k2逐渐降低,在超生理水平(5,064 microU / ml)下降低了7倍。该饱和度曲线的表观KM为742 microU / ml(约5 nM)。相反,从中隔室和CSF去除胰岛素的速率常数不随血浆胰岛素而变化(k2 + k3 = 0.011 +/- 0.0019 min-1和k4 = 0.046 +/- 0.021 min-1)。我们得出结论,血浆胰岛素到中枢神经系统的传递是可饱和的,并且可能由胰岛素受体介导的转运过程促进。

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