放射性标记的单克隆抗体预吸附到肝脏和脾脏组织导致更高的肿瘤与正常组织的比率。

A D van den Abbeele, R A Aaronson, R A Taube, S J Adelstein, A I Kassis
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引用次数: 0

摘要

本研究探讨了背景活性对放射免疫偶联物用于放射免疫诊断和放射免疫治疗的影响。由于肝脏和脾脏是具有优先非特异性摄取的器官,我们将放射性标记(碘化和铟111标记)单克隆抗体暴露在生理温度下的新鲜肝脏和脾脏细胞悬液中,并将其免疫反应性、体内生物分布和肿瘤靶向性与未事先吸附于该悬液的相同放射性标记蛋白进行比较。生物分布研究是在高本底活性条件下进行的,即在注射后不久(1小时)并使用高剂量的蛋白质。放射性标记单克隆抗体的预吸附导致某些正常组织的摄取显著减少,即正常组织和肿瘤组织之间的对比更大,正如两个靶标与非靶标比率(暴露/未暴露抗体)的商数所证明的那样,对于大多数检查的组织来说,其大于1。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Preadsorption of radiolabeled monoclonal antibodies to liver and spleen tissues leads to higher tumor-to-normal-tissue ratios.

This study addresses the impact of background activity on the use of radioimmunoconjugates for radioimmunodiagnosis and radioimmunotherapy. Since the liver and the spleen represent organs with preferential nonspecific uptake, we exposed radiolabeled (iodinated and Indium-111 labeled) preparations of monoclonal antibodies to a suspension of fresh liver and spleen cells at physiological temperature and compared their immunoreactivity, in vivo biodistribution, and tumor targeting to those of the same radiolabeled proteins without prior adsorption to this suspension. The biodistribution studies were performed under conditions of high background activity, i.e., shortly after the injection (1 hour) and using a high dose of the protein. Preadsorption of radiolabeled monoclonal antibodies results in a significant decreased uptake in certain normal tissues, i.e., greater contrast between normal and tumor tissues, as demonstrated by the quotient of the two target-to-nontarget ratios (exposed/unexposed antibody) which was greater than one for most of the tissues examined.

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