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铟-111标记的嵌合肿瘤坏死治疗(chTNT)-3抗体的基因工程Fab'和F(ab')2构建体的肿瘤靶向特性

Tumor targeting properties of indium-111 labeled genetically engineered Fab' and F(ab')2 constructs of chimeric tumor necrosis treatment (chTNT)-3 antibody.

作者信息

Khawli Leslie A, Alauddin Mian M, Hu Peisheng, Epstein Alan L

机构信息

University of Southern California, Keck School of Medicine, Los Angeles, CA, USA.

出版信息

Cancer Biother Radiopharm. 2003 Dec;18(6):931-40. doi: 10.1089/108497803322702897.

DOI:10.1089/108497803322702897
PMID:14969605
Abstract

Genetic engineering techniques have allowed the construction of Fab' and F(ab')2 constructs of chimeric tumor necrosis treatment antibody (chTNT-3), a chimeric monoclonal antibody (MAb) that targets necrotic regions of solid tumors. The purpose of this study is to evaluate the in vitro and in vivo properties of Fab' and F(ab')2 constructs radiolabeled with indium-111 (111In) using diethylentriamine pentaacetic acid (DTPA) conjugation to develop a clinically useful imaging agent for the detection of necrosis in solid tumors. Optimization of the MAb-to-DTPA ratio showed that a 1:2 ratio gave the best immunoreactivity while providing good radiolabeling efficiency and high specific activity for all three DPTA conjugates. In addition, 111In-labeled Fab' and F(ab')2 conjugates were found to have faster whole body clearance times and better biodistribution profiles compared to parental 111In-labeled chTNT-3 in tumor-bearing mice. Although radiolabeled Fab' and F(ab')2 constructs showed lower tumor uptake than radiolabeled chTNT-3, biodistribution results showed that these constructs had significantly lower uptake in liver, spleen, and other normal organs (except the kidney), and therefore had higher tumor-to-organ ratios. In addition, a comparison of all derivatives showed that the F(ab')2 reagent gave the best results in tumor imaging studies. These results demonstrate that stable, a genetically engineered F(ab')2 construct can be successfully radiolabeled with 111In to produce potential imaging reagents for the imaging and monitoring of tumor necrosis.

摘要

基因工程技术已使得构建嵌合肿瘤坏死治疗抗体(chTNT-3)的Fab'和F(ab')2构建体成为可能,chTNT-3是一种靶向实体瘤坏死区域的嵌合单克隆抗体(MAb)。本研究的目的是评估用二乙三胺五乙酸(DTPA)偶联法用铟-111(111In)进行放射性标记的Fab'和F(ab')2构建体的体外和体内特性,以开发一种临床上有用的成像剂,用于检测实体瘤中的坏死情况。单克隆抗体与DTPA比例的优化表明,1:2的比例能产生最佳的免疫反应性,同时为所有三种DTPA偶联物提供良好的放射性标记效率和高比活性。此外,与荷瘤小鼠体内亲本111In标记的chTNT-3相比,发现111In标记的Fab'和F(ab')2偶联物具有更快的全身清除时间和更好的生物分布情况。尽管放射性标记的Fab'和F(ab')2构建体显示出比放射性标记的chTNT-3更低的肿瘤摄取,但生物分布结果表明,这些构建体在肝脏、脾脏和其他正常器官(肾脏除外)中的摄取显著更低,因此具有更高的肿瘤与器官摄取比。此外,对所有衍生物的比较表明,F(ab')2试剂在肿瘤成像研究中给出了最佳结果。这些结果表明,一种稳定的、基因工程改造的F(ab')2构建体可以成功地用111In进行放射性标记,以产生用于肿瘤坏死成像和监测的潜在成像试剂。

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An overview of translational (radio)pharmaceutical research related to certain oncological and non-oncological applications.
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