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实体瘤的放射免疫疗法:对小鼠和人类的综述

Radioimmunotherapy of solid tumors: a review "of mice and men".

作者信息

Behr T M, Goldenberg D M, Becker W S

机构信息

Department of Nuclear Medicine, Georg-August-University of Göttingen, Germany.

出版信息

Hybridoma. 1997 Feb;16(1):101-7. doi: 10.1089/hyb.1997.16.101.

Abstract

Radioimmunotherapy in lymphoma is crossing the threshold to become a standard mode of treatment. Whereas in solid tumors in preclinical studies, radioimmunotherapy has proven to be superior to conventional chemotherapy, clinical success is still limited. The purpose of this brief review is to analyze recent developments in preclinical as well as clinical radioimmunotherapy of solid, CEA-expressing tumors. Advances in experimental radioimmunotherapy are characterized by the development of metastatic, rather than subcutaneous, tumor models in nude mice, which seem to reflect the actual clinical situation much more accurately. Furthermore, the recent development of strategies to reduce the renal accretion of antibody fragments and peptides enables the use of such smaller molecules for therapy, especially those also labeled with radiometals and other forms of intracellularly retained radionuclides. Recent developments in clinical radioimmunotherapy are characterized by a trend toward the treatment of small-volume and micrometastatic disease, as is the case, e.g., in adjuvant settings. Interestingly, despite dramatic differences in size, weight and percent-of-injected-dose-per-gram uptake values, only small differences between animal models and the actual patient situation exist with respect to activity concentrations (in microCi/gram) in the tumors and tissues. Because the activity concentration over time determines the radiation absorbed dose, and thus biological effects, we postulate that animal models should be able to predict actual clinical scenarios fairly well. These findings could be used as guidelines in the design of future preclinical, as well as clinical, trials.

摘要

淋巴瘤的放射免疫疗法正跨越门槛成为一种标准治疗模式。尽管在临床前研究的实体瘤中,放射免疫疗法已被证明优于传统化疗,但其临床成效仍有限。本简要综述的目的是分析实体性、表达癌胚抗原(CEA)肿瘤的临床前及临床放射免疫疗法的最新进展。实验性放射免疫疗法的进展特点是在裸鼠中建立了转移性而非皮下肿瘤模型,这似乎能更准确地反映实际临床情况。此外,近期减少抗体片段和肽在肾脏蓄积的策略的发展,使得能够使用此类较小分子进行治疗,尤其是那些也用放射性金属和其他形式的细胞内滞留放射性核素标记的分子。临床放射免疫疗法的最新进展特点是倾向于治疗小体积和微转移疾病,例如在辅助治疗环境中。有趣的是,尽管在大小、重量和每克注射剂量摄取值百分比方面存在显著差异,但在肿瘤和组织中的活度浓度(以微居里/克计)方面,动物模型与实际患者情况之间仅存在微小差异。由于活度浓度随时间决定辐射吸收剂量,进而决定生物学效应,我们推测动物模型应该能够较好地预测实际临床情况。这些发现可作为未来临床前及临床试验设计的指导原则。

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