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In Vivo Imaging of Insulin Receptors in Monkeys Using 18F-Labeled Insulin and Positron Emission Tomography

机译:使用18F标签胰岛素和正电子发射断层扫描对猴子体内的胰岛素受体进行体内成像

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摘要

We previously described a prosthetic group methodology for incorporating 18F into peptides and showed that 18F-labeled insulin (18F-insulin) binds to insulin receptors on human cells (IM-9 lymphoblastoid cells) with affinity equal to that of native insulin (). We now report studies using 18F-insulin with positron emission tomography to study binding to insulin receptors in vivo. Positron emission tomography scans were performed in six rhesus monkeys injected with 0.3–1.4 mCi of 18F-insulin (~0.1 nmol, SA 4–11 Ci/μmol). Integrity of the tracer in blood, determined by immunoprecipitation, was 94% of control for the first 5 min and decreased to 31% by 30 min. Specific, saturable uptake of 18F was observed in the liver and kidney. Coinjection of unlabeled insulin (200 U, ~1 nmol) with the 18F-insulin reduced liver and increased kidney uptake of the labeled insulin. Liver radioactivity was decreased by administration of unlabeled insulin at 3 min, but not 5 min, after administration of the tracer, while some kidney radioactivity could be displaced 5 min after injection. Clearance of 18F was predominantly in bile and urine. 18F-insulin is a suitable analogue for studying insulin receptor-ligand interactions in vivo, especially in the liver and kidney.
机译:我们先前描述了将 18 F掺入肽中的修复组方法,并显示了 18 F标记的胰岛素( 18 F-胰岛素)与人体细胞(IM-9淋巴母细胞)上的胰岛素受体,其亲和力等于天然胰岛素()。现在,我们报道了使用 18 F-胰岛素和正电子发射断层扫描技术研究体内结合胰岛素受体的研究。对六只猕猴进行了正电子发射断层扫描,注射了0.3–1.4 mCi的 18 F胰岛素(〜0.1 nmol,SA 4-11 Ci /μmol)。通过免疫沉淀测定,示踪剂在血液中的完整性在开始的5分钟内为对照的94%,到30分钟时降至31%。在肝脏和肾脏中观察到特定的,饱和的 18 F吸收。未标记的胰岛素(200 U,〜1 nmol)与 18 F-胰岛素的共同注射减少了肝脏,增加了肾脏对标记胰岛素的摄取。示踪剂给药后3分钟(而非5分钟)施用未标记的胰岛素可降低肝脏放射性,而注射5分钟后可替代一些肾脏放射性。 18 F的清除主要在胆汁和尿液中进行。 18 F-胰岛素是用于研究体内胰岛素受体-配体相互作用的合适类似物,尤其是在肝脏和肾脏中。

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