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Formation of complexes between 125I-labelled human or bovine somatotropins and binding proteins in vivo in rat liver and kidney.

机译:在大鼠肝脏和肾脏中体内125I标记的人或牛生长激素和结合蛋白之间形成复合物。

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摘要

At 5 min after intravenous injection, both 125I-labelled human somatotropin and 125I-labelled bovine somatotropin were concentrated in rat liver and kidney. When the labelled hormones were administered along with an excess of the corresponding unlabelled hormone, a significant decrease of the uptake was observed in the liver, but not in the kidney. Study of the subcellular distribution of radioiodinated somatotropins in liver revealed that most of the radioactivity was specifically concentrated in the microsomal fraction. In contrast, the kidney fraction that accounted for most of the radioactivity was the 100 000 g supernatant. After solubilization, with 1% (w/v) Triton X-100, of the microsomal fractions obtained from both organs, the radioactive material was analysed by gel filtration on Sepharose CL-6B. By using this approach, it was demonstrated that both 125I-labelled human somatotropin and 125I-labelled bovine somatotropin bind in vivo to proteins present in liver. A small proportion of 125I-labelled human somatotropin was also shown to form complexes with proteins present in kidney. The present results demonstrate that the liver uptake is mainly due to binding of somatotropins to specific proteins, in contrast with the kidney, in which binding to specific sites contributes minimally to the overall uptake.
机译:静脉注射后5分钟,125I标记的人生长激素和125I标记的牛生长激素都集中在大鼠肝脏和肾脏中。当将标记的激素与过量的相应的未标记的激素一起施用时,在肝脏中观察到摄取的显着降低,但在肾脏中没有观察到。肝脏中放射性碘化生长激素的亚细胞分布研究表明,大多数放射性特别集中在微粒体部分。相反,占大部分放射性的肾脏部分是10万克上清液。用从两个器官获得的微粒体级分溶解有1%(w / v)Triton X-100后,通过在Sepharose CL-6B上进行凝胶过滤来分析放射性物质。通过使用这种方法,证明了125I标记的人类生长激素和125I标记的牛生长激素在体内均与肝脏中存在的蛋白质结合。还显示了一小部分125I标记的人类生长激素与肾脏中存在的蛋白质形成复合物。目前的结果表明,肝脏摄取主要是由于生长激素与特定蛋白质的结合,而肾脏与肾脏相反,在肾脏中与特定部位的结合对总摄取的贡献最小。

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