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基因工程改造的泛癌单克隆抗体CC49的四价单链Fv:改善的生物分布及治疗应用潜力

Genetically engineered tetravalent single-chain Fv of the pancarcinoma monoclonal antibody CC49: improved biodistribution and potential for therapeutic application.

作者信息

Goel A, Colcher D, Baranowska-Kortylewicz J, Augustine S, Booth B J, Pavlinkova G, Batra S K

机构信息

Department of Biochemistry, University of Nebraska Medical Center, Omaha 68198-4525, USA.

出版信息

Cancer Res. 2000 Dec 15;60(24):6964-71.

PMID:11156397
Abstract

Failure of radiolabeled monoclonal antibodies (MAbs) in the treatment of solid tumors, for the most part, is a result of undesirable pharmacokinetics that lead to significant radiation exposure of normal tissues and an inadequate delivery of radiation doses to tumors. Using genetic engineering, antitumor MAbs can be optimized for desirable clinical applications. In the present study, we report the generation of a tetravalent single-chain Fv [[sc(Fv)2]2] of the murine MAb CC49 that recognizes the tumor-associated glycoprotein, TAG-72. [Sc(Fv)2]2 was expressed as a secreted soluble protein in Pichia pastoris under the regulation of alcohol oxidase 1 promoter. The in vitro binding properties of the tetravalent construct were analyzed by solid-phase RIA and surface plasmon resonance studies using BIAcore. The binding affinity constant (K(A)) for the [sc(Fv)2]2 and CC49 IgG were similar, i.e., 1.02 x 10(8) M(-1) and 1.14 x 10(8) M(-1), respectively, and were 4-fold higher than its divalent scFv [sc(Fv)2; 2.75 x 10(7) M(-1)]. At 6 h postadministration, the percentage of injected dose accumulated/g of LS-174T colon carcinoma xenografts was 21.3+/-1.3, 9.8+/-1.3, and 17.3+/-1.1 for radioiodinated [sc(Fv)2]2, sc(Fv)2, and IgG, respectively. Pharmacokinetic analysis of blood clearance studies showed the elimination half-life for [sc(Fv)2]2, sc(Fv)2, and IgG as 170, 80, and 330 min, respectively. The gain in avidity resulting from multivalency along with an improved biological half-life makes the tetravalent construct an important reagent for cancer therapy and diagnosis in MAb-based radiopharmaceuticals.

摘要

放射性标记的单克隆抗体(MAb)在实体瘤治疗中大多失败,这主要是由于不理想的药代动力学,导致正常组织受到显著辐射暴露,且肿瘤接受的辐射剂量不足。利用基因工程,抗肿瘤单克隆抗体可针对理想的临床应用进行优化。在本研究中,我们报告了鼠源单克隆抗体CC49的四价单链Fv [[sc(Fv)2]2] 的产生,该抗体识别肿瘤相关糖蛋白TAG-72。[Sc(Fv)2]2在甲醇氧化酶1启动子的调控下,作为分泌性可溶性蛋白在毕赤酵母中表达。通过固相放射免疫分析和使用BIAcore的表面等离子体共振研究,分析了四价构建体的体外结合特性。[sc(Fv)2]2和CC49 IgG的结合亲和常数(K(A))相似,分别为1.02×10(8) M(-1)和1.14×10(8) M(-1),比其二价单链Fv [sc(Fv)2;2.75×10(7) M(-1)]高4倍。给药后6小时,放射性碘化的[sc(Fv)2]2、sc(Fv)2和IgG在LS-174T结肠癌异种移植瘤中每克积累的注射剂量百分比分别为21.3±1.3、9.8±1.3和17.3±1.1。血液清除研究的药代动力学分析表明,[sc(Fv)2]2、sc(Fv)2和IgG的消除半衰期分别为170、80和330分钟。多价性带来的亲和力增加以及生物学半衰期的改善,使得四价构建体成为基于单克隆抗体的放射性药物用于癌症治疗和诊断的重要试剂。

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