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抗胰岛素血清和抗胰岛素受体血清对大鼠¹²³I-胰岛素代谢的不同作用。

Differing effects of antiinsulin serum and antiinsulin receptor serum on 123I-insulin metabolism in rats.

作者信息

Sodoyez J C, Sodoyez Goffaux F, von Frenckell R, De Vos C J, Treves S, Kahn C R

出版信息

J Clin Invest. 1985 May;75(5):1455-62. doi: 10.1172/JCI111848.

Abstract

Anesthetized rats were treated with saline, antiinsulin receptor serum, or antiinsulin serum, and the biodistribution of high pressure liquid chromatography-purified 123I-Tyr A14-insulin was studied by scintillation scanning. Time activity curves over organs of interest were calibrated by sacrificing the rats at the end of the experiment and directly determining the radioactivity in the blood, liver, and kidneys. Saline-treated rats exhibited normal insulin biodistribution. The highest concentration of 123I-insulin was found in the liver, and reached 30% of total injected dose between 3 and 5 min after injection. After this peak, activity rapidly decreased with a t1/2 of 6 min. Activity of 123I-insulin in kidney showed a more gradual rise and fall and was approximately 15% of injected dose at its maximum. In rats treated with antiinsulin antiserum, insulin biodistribution was markedly altered. Peak liver activity increased with increasing antibody concentration with up to 90% of injected dose appearing in the liver. In addition, there was no clearance of the liver 123I-insulin over 30 min. Autoradiographic studies demonstrated that in contrast to the normal rats in which radioactivity was associated with hepatocytes, in rats passively immunized with anti-insulin serum, 125I-insulin was associated primarily with the Kuppfer cells. In contrast, antibodies to the insulin receptor markedly inhibited 123I-insulin uptake by the liver. Kidney activity increased, reflecting the amount of free 123I-insulin that reached this organ. This is similar to the pattern observed when insulin receptors are saturated with a high concentration of unlabeled insulin. Thus, both insulin antibodies and anti-receptor antibodies alter the distribution of insulin, but with very different patterns. The use of 123I-insulin and scintillation scanning allows one to study specific alterations in insulin distribution in animal models of insulin-resistant states, and should also be useful in human disease states.

摘要

将麻醉后的大鼠分别用生理盐水、抗胰岛素受体血清或抗胰岛素血清进行处理,然后通过闪烁扫描研究高压液相色谱纯化的123I-酪氨酸A14-胰岛素的生物分布。在实验结束时处死大鼠,直接测定血液、肝脏和肾脏中的放射性,以此校准感兴趣器官的时间-活性曲线。用生理盐水处理的大鼠表现出正常的胰岛素生物分布。123I-胰岛素在肝脏中的浓度最高,在注射后3至5分钟内达到注射总剂量的30%。在此峰值之后,活性迅速下降,半衰期为6分钟。123I-胰岛素在肾脏中的活性呈现出更为缓慢的上升和下降,其最大值约为注射剂量的15%。在用抗胰岛素抗血清处理的大鼠中,胰岛素的生物分布明显改变。肝脏的峰值活性随着抗体浓度的增加而升高,肝脏中出现了高达注射剂量90%的放射性。此外,肝脏中的123I-胰岛素在30分钟内没有清除。放射自显影研究表明,与放射性与肝细胞相关的正常大鼠相比,在用抗胰岛素血清被动免疫的大鼠中,125I-胰岛素主要与库普弗细胞相关。相比之下,胰岛素受体抗体显著抑制肝脏对123I-胰岛素的摄取。肾脏活性增加,反映了到达该器官的游离123I-胰岛素的量。这与用高浓度未标记胰岛素使胰岛素受体饱和时观察到的模式相似。因此,胰岛素抗体和抗受体抗体都改变了胰岛素的分布,但模式非常不同。使用123I-胰岛素和闪烁扫描能够研究胰岛素抵抗状态动物模型中胰岛素分布的特定改变,并且在人类疾病状态中也应该是有用的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/588e/425483/66741e913095/jcinvest00140-0074-a.jpg

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