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一种新型靶向 CD44v6 的抗体片段,具有改善的肿瘤与血液比值。

A novel CD44v6 targeting antibody fragment with improved tumor-to-blood ratio.

机构信息

Department of Surgical Sciences, Unit of Otolaryngology and Head and Neck Surgery, Uppsala University, Uppsala, Sweden.

出版信息

Int J Oncol. 2012 May;40(5):1525-32. doi: 10.3892/ijo.2012.1352. Epub 2012 Feb 1.

DOI:10.3892/ijo.2012.1352
PMID:22307465
Abstract

The chimeric monoclonal antibody U36 (cMAb U36) recognizes the CD44v6 antigen. Its potential as a radioimmunotargeting agent, as well as its safety, has been shown in previous studies in head and neck cancer patients. However, intact MAbs have long circulation time in the blood and tumor targeting may also be hampered due to the slow and incomplete diffusion into solid tumors. In comparison, smaller monovalent Fab' and divalent F(ab')2 fragments are expected to exhibit shorter circulating half-lives, better tumor penetration and are thus more likely to yield better imaging results. In this study, novel F(ab')2 and Fab' fragments from cMAb U36 were radiolabeled with 125I and the characteristics of the conjugates in vitro were examined. The biodistribution of the conjugates were then evaluated in nude mice bearing CD44v6-expressing xenograft tumors. Furthermore, the penetration depth and distribution in tumor tissue was assessed by autoradiography in selected tumor samples. The in vitro experiments showed that the conjugates were stable and had intact affinity to CD44v6. The biodistribution study demonstrated superior tumor-to-blood ratio for the novel cMAb U36 fragment 125I-F(ab')2 compared with both the intact MAb and the monovalent fragment form. Autoradiography also revealed better tumor penetration for 125I-F(ab')2. This study demonstrates that the use of antibody fragments may improve radioimmunotargeting and possibly improve the management of head and neck malignancies.

摘要

嵌合单克隆抗体 U36(cMAb U36)识别 CD44v6 抗原。在以前对头颈癌患者的研究中,已经证明了其作为放射性免疫靶向剂的潜力及其安全性。然而,完整的 MAbs 在血液中的循环时间较长,并且由于缓慢且不完全扩散到实体瘤中,肿瘤靶向也可能受到阻碍。相比之下,较小的单价 Fab'和二价 F(ab')2 片段预计具有较短的循环半衰期,更好的肿瘤穿透性,因此更有可能产生更好的成像结果。在这项研究中,新型 F(ab')2 和 Fab'片段从 cMAb U36 被放射性标记 125I,并且检查了体外缀合物的特性。然后在表达 CD44v6 的裸鼠异种移植肿瘤中评估了缀合物的体内分布。此外,通过在选定的肿瘤样本中进行放射自显影评估了在肿瘤组织中的穿透深度和分布。体外实验表明,缀合物是稳定的,并且对 CD44v6 具有完整的亲和力。在体内分布研究中,新型 cMAb U36 片段 125I-F(ab')2 的肿瘤与血液比与完整 MAb 和单价片段形式相比均具有更高的肿瘤与血液比。放射自显影还揭示了 125I-F(ab')2 更好的肿瘤穿透性。这项研究表明,使用抗体片段可能会改善放射性免疫靶向,并可能改善头颈部恶性肿瘤的治疗。

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