Internalization of [DOTA degrees,125I-Tyr3]Octreotide by somatostatin receptor-positive cells in vitro and in vivo: implications for somatostatin receptor-targeted radio-guided surgery.

L J Hofland, W A Breeman, E P Krenning, M de Jong, M Waaijers, P M van Koetsveld, H R Mäcke, S W Lamberts
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引用次数: 48

Abstract

We compared internalization of three radioiodinated octreotide (OCT) somatostatin (SS) analogs-[125I-Tyr3]OCT, [DTPA degrees, 125I-Tyr3]OCT, and [DOTA degrees,125I-Tyr3]OCT-by somatostatin receptor (SSR)-positive mouse AtT20 pituitary tumor cells and human insulinoma cells. The three SS analogs were internalized in a specific, time-dependent manner. Internalization was significantly inhibited by pertussis toxin (100 microg/l) by 38%, 43%, and 31%, and by an inhibitor of receptor-mediated endocytosis (phenyl arsine oxide; 10 microM) by 98%, 94%, and 92%, respectively. Binding affinities of the three radioligands were comparable (0.2, 0.2, and 0.3 nM, respectively). However, [DOTA degrees,125I-Tyr3]OCT was internalized in a five-fold higher amount in comparison with the two other radioligands. A comparably high uptake of [DOTA degrees, 125I-Tyr3]OCT was found in SSR-positive organs (pituitary, pancreas, and adrenals) in vivo in rats (a ten-fold, five-fold, and eight-fold higher uptake 4 hr post injection, respectively, compared with the two other radioligands). This resulted in very high target-background ratios for [DOTA degrees,125I-Tyr3]OCT 4 hr post injection amounting to 274, 566, and 623 in the pituitary, adrenals, and pancreas, respectively. Both in vivo and in vitro there was a rapid dissociation of radioactivity from the SSR-positive cells. Main conclusions are that: 1) coupling of chelating groups like DTPA or DOTA to the SS analog [Tyr3]OCT does not prevent the internalization of OCT after binding to SSRs; 2) [DOTA degrees, 125I-Tyr3]OCT is internalized in a significantly higher amount by AtT20 and human insulinoma cells and in vivo in rats in SSR-positive organs, in comparison with [DTPA degrees,125I-Tyr3]OCT and [125I-Tyr3]OCT; and 3) the very high target-background ratios in vivo make radioiodinated [DOTA degrees,Tyr3]OCT a very suitable ligand for SSR-targeted radioguided surgery of SSR-positive human neuroendocrine tumors.

体外和体内生长抑素受体阳性细胞对[DOTA度,125I-Tyr3]奥曲肽的内化:对生长抑素受体靶向放射引导手术的影响
我们比较了生长抑素受体(SSR)阳性小鼠AtT20垂体瘤细胞和人胰岛素瘤细胞对三种放射性碘化奥屈肽(OCT)生长抑素(SS)类似物([125I-Tyr3]OCT、[DTPA度,125I-Tyr3]OCT和[DOTA度,125I-Tyr3]OCT的内化作用。三种SS类似物以特定的时间依赖性方式内化。百日咳毒素(100微克/升)对内化的抑制作用分别为38%、43%和31%,受体介导的内吞作用抑制剂(苯基氧化胂;10微米)分别降低98%、94%和92%。三种放射性配体的结合亲和度是相似的(分别为0.2、0.2和0.3 nM)。然而,[DOTA度,125I-Tyr3]OCT的内在化量是其他两种放射配体的五倍。在大鼠体内ssr阳性器官(垂体、胰腺和肾上腺)中发现了相当高的[DOTA度,125I-Tyr3]OCT摄取(注射后4小时分别比其他两种放射性配体高10倍、5倍和8倍)。这导致注射后4小时OCT [DOTA度,125I-Tyr3]的靶本比非常高,分别在垂体、肾上腺和胰腺中达到274、566和623。在体内和体外,放射性都与ssr阳性细胞迅速分离。主要结论是:1)DTPA或DOTA等螯合基团与SS类似物[Tyr3]OCT的偶联并不会阻止与SSRs结合后OCT的内化;2)与[DTPA度,125I-Tyr3]OCT和[125I-Tyr3]OCT相比,[DOTA度,125I-Tyr3]OCT被AtT20和人胰岛素瘤细胞以及ssr阳性器官大鼠体内的内化量明显更高;3)体内非常高的靶本底比使放射碘化OCT [DOTA度,Tyr3]成为ssr阳性人神经内分泌肿瘤靶向放射引导手术的非常合适的配体。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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