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癌胚抗原作为人甲状腺髓样癌放射免疫治疗的靶点:抗体处理、靶向以及用¹³¹I和⁹⁰Y标记单克隆抗体的实验性治疗

Carcinoembryonic antigen as a target for radioimmunotherapy of human medullary thyroid carcinoma: antibody processing, targeting, and experimental therapy with 131I and 90Y labeled MAbs.

作者信息

Stein R, Juweid M, Mattes M J, Goldenberg D M

机构信息

Garden State Cancer Center, Belleville, NJ 07109, USA.

出版信息

Cancer Biother Radiopharm. 1999 Feb;14(1):37-47. doi: 10.1089/cbr.1999.14.37.

DOI:10.1089/cbr.1999.14.37
PMID:10850286
Abstract

The poor prognosis of patients with advanced medullary thyroid carcinoma (MTC) has prompted a search for new treatment modalities. In this report we explore the characteristics of carcinoembyronic antigen (CEA) as a target for radioimmunotherapy (RAIT) of MTC, with respect to antibody processing, targeting, and experimental therapy. In vitro studies showed a high level of CEA expression on the cell surface of the MTC cell line TT. MAbs bound to the cell were predominantly retained for several days, although there was also a significant level of internalization and catabolism. Immunohistology of frozen sections of tumor xenografts demonstrated that approximately half of the cells were darkly stained, however, some cells expressed little or no CEA. In biodistribution studies in nude mice bearing TT tumors, the mean percent injected dose per gram of tumor observed at three days post injection (time of maximum uptake) of 125I-MN-14 was 19.7%. When the MAb was labeled with 88Y, a residualizing label, a much higher accretion, 50.5%, was observed at the time of maximum uptake (7 days). Significant anti-tumor effects were seen at the maximum tolerated doses of 131I- and 90Y-MN-14, compared with relatively rapid tumor growth in untreated animals or those treated with the same dose of control MAbs. Importantly, it was observed that 90Y-MN-14 yielded significantly improved therapeutic efficacy in comparison to 131I-MN-14, which may have important implications for design and conduct of future clinical trials for the treatment of MTC.

摘要

晚期甲状腺髓样癌(MTC)患者预后较差,这促使人们寻找新的治疗方法。在本报告中,我们探讨了癌胚抗原(CEA)作为MTC放射免疫治疗(RAIT)靶点的特性,涉及抗体处理、靶向作用和实验性治疗。体外研究表明,MTC细胞系TT的细胞表面有高水平的CEA表达。与细胞结合的单克隆抗体(MAb)主要保留数天,不过也有相当程度的内化和分解代谢。肿瘤异种移植冻切片的免疫组织学显示,约一半的细胞被染成深色,然而,一些细胞几乎不表达或不表达CEA。在携带TT肿瘤的裸鼠生物分布研究中,注射125I-MN-14后三天(摄取量最大时),每克肿瘤观察到的平均注射剂量百分比为19.7%。当MAb用残留标记物88Y标记时,在摄取量最大时(7天)观察到更高的积聚率,为50.5%。与未治疗动物或用相同剂量对照MAb治疗的动物中相对快速的肿瘤生长相比,在131I-和90Y-MN-14的最大耐受剂量下观察到了显著的抗肿瘤作用。重要的是,观察到与131I-MN-14相比,90Y-MN-14产生了显著提高的治疗效果,这可能对未来MTC治疗临床试验的设计和开展具有重要意义。

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