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实体癌的放射免疫疗法:综述

Radioimmunotherapy of solid cancers: A review.

作者信息

Kairemo K J

机构信息

Department of Oncology, Helsinki University Central Hospital, Helsinki, Finland.

出版信息

Acta Oncol. 1996;35(3):343-55. doi: 10.3109/02841869609101651.

DOI:10.3109/02841869609101651
PMID:8679266
Abstract

Depending on radionuclide characteristics, radioimmunotherapy (RIT) relies on radioactivity to destroy cells distant from immunotargeted cells. Therefore, even heterogeneous tumors (for antigen recognition) can be treated, because not all cells have to be targeted. Substantial complete response rates have been reported in patients with non-Hodgkin's lymphoma. Much more modest results have been reported for patients with bulky solid tumors, e.g. adenocarcinomas. The radiation doses delivered by targeting antibodies are generally too low to achieve major therapeutic responses. Dose escalation is limited by myelotoxicity, and higher doses need to be delivered to neoplasms less radiosensitive than lymphomas. Various trials for both systemic and regional RIT have been reported on. Intraperitoneal administration has been applied for colorectal and ovarian carcinomas. Our own results indicate that, e.g., intraperitoneal pseudomyxoma can be treated with RIT. Myelotoxicity can be reduced by anti-antibody-enhancement, 2- and 3-step strategies, bispecific monoclonal antibodies (MAbs), and extracorporeal immunoadsorption. The radionuclide has to be selected properly for each purpose; it can be a beta-emitter, e.g. I-131, Y-90, Re-188, Re-186, Lu-177 or Sm-153, an alpha-emitter At-211 or Bi-212 or an Auger-emitter, e.g. I-125, I-123. One major problem with RIT, besides slow penetration rate into tumor tissue and low tumor-to-normal tissue ratio, is the HAMA response, which can be partly avoided by the use of humanized MAbs and immunosuppression. However, RIT will be, because of all the recent developments, an important form of cancer management.

摘要

根据放射性核素的特性,放射免疫疗法(RIT)依靠放射性来破坏远离免疫靶向细胞的细胞。因此,即使是异质性肿瘤(用于抗原识别)也可以得到治疗,因为并非所有细胞都必须成为靶向目标。据报道,非霍奇金淋巴瘤患者有相当高的完全缓解率。对于体积较大的实体瘤患者,如腺癌患者,所报道的结果则要逊色得多。靶向抗体所输送的辐射剂量通常过低,无法实现显著的治疗反应。剂量递增受到骨髓毒性的限制,需要向比淋巴瘤对辐射敏感性更低的肿瘤输送更高剂量。已经报道了关于全身和局部RIT的各种试验。腹腔内给药已应用于结直肠癌和卵巢癌。我们自己的结果表明,例如,腹腔内黏液性假瘤可用RIT治疗。通过抗抗体增强、两步和三步策略、双特异性单克隆抗体(MAb)和体外免疫吸附可以降低骨髓毒性。必须针对每个目的正确选择放射性核素;它可以是β发射体,如I-131、Y-90、Re-188、Re-186、Lu-177或Sm-153,α发射体At-211或Bi-212,或俄歇电子发射体,如I-125、I-123。除了向肿瘤组织的渗透速度慢和肿瘤与正常组织的比例低之外,RIT的一个主要问题是人抗鼠抗体(HAMA)反应,使用人源化单克隆抗体和免疫抑制可部分避免这种反应。然而,鉴于最近的所有进展,RIT将成为癌症治疗的一种重要形式。

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1
Radioimmunotherapy of solid cancers: A review.实体癌的放射免疫疗法:综述
Acta Oncol. 1996;35(3):343-55. doi: 10.3109/02841869609101651.
2
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Correlation of red marrow radiation dosimetry with myelotoxicity: empirical factors influencing the radiation-induced myelotoxicity of radiolabeled antibodies, fragments and peptides in pre-clinical and clinical settings.红骨髓辐射剂量测定与骨髓毒性的相关性:影响临床前和临床环境中放射性标记抗体、片段和肽辐射诱导骨髓毒性的经验因素。
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Strategies for developing effective radioimmunotherapy for solid tumors.开发实体瘤有效放射免疫疗法的策略。
Clin Cancer Res. 1999 Oct;5(10 Suppl):3219s-3223s.
8
Biodistribution and therapeutic efficacy of (125/131)I-, (186)Re-, (88/90)Y-, or (177)Lu-labeled monoclonal antibody MN-14 to carcinoembryonic antigen in mice with small peritoneal metastases of colorectal origin.(125/131)I-、(186)Re-、(88/90)Y-或(177)Lu标记的抗癌胚抗原单克隆抗体MN-14在结直肠癌源性小腹膜转移小鼠中的生物分布及治疗效果
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Clin Cancer Res. 2003 Dec 1;9(16 Pt 1):5842-52.

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