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卡妥索单抗:临床开发及未来方向。

Catumaxomab: clinical development and future directions.

机构信息

Fresenius Biotech GmbH, Munich, Germany.

出版信息

MAbs. 2010 Mar-Apr;2(2):129-36. doi: 10.4161/mabs.2.2.11221.

DOI:10.4161/mabs.2.2.11221
PMID:20190561
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2840231/
Abstract

Catumaxomab, a monoclonal bispecific trifunctional antibody, was approved in the European Union in April 2009 for the intraperitoneal treatment of patients with malignant ascites. The marketing authorization holder Fresenius Biotech GmbH developed catumaxomab (Removab(®)) together with its partner TRION Pharma GmbH, Germany. It is the first substance worldwide with a regulatory label for the treatment of malignant ascites due to epithelial carcinomas. Since the peritoneum is of mesothelial origin and therefore lacks EpCAM expression, the intraperitoneal administration of catumaxomab is an attractive targeted immunotherapeutic approach. Catumaxomab is able to destroy EpCAM positive tumor cells in the peritoneal cavity known as the main cause of malignant ascites. In addition, catumaxomab is a potential therapeutic option for several primary tumors since the EpCAM molecule is expressed on the majority of epithelial carcinomas. This review focuses on the clinical development of catumaxomab and indicates future directions.

摘要

卡特木单抗是一种单克隆双特异性三功能抗体,于 2009 年 4 月在欧盟获批,用于治疗恶性腹水患者。该药物的上市许可持有人费森尤斯医药保健有限公司(Fresenius Biotech GmbH)与德国的 TRION Pharma GmbH 合作开发了卡特木单抗(Removab(®))。它是全球首个具有治疗上皮性癌所致恶性腹水适应证的监管标签的药物。由于腹膜源于间皮细胞,因此缺乏 EpCAM 表达,因此腹腔内给予卡特木单抗是一种有吸引力的靶向免疫治疗方法。卡特木单抗能够破坏腹腔中 EpCAM 阳性肿瘤细胞,这些细胞是恶性腹水的主要原因。此外,由于 EpCAM 分子在上皮性癌中大多数都有表达,因此卡特木单抗也是几种原发性肿瘤的潜在治疗选择。本文重点介绍了卡特木单抗的临床开发情况,并指出了未来的发展方向。

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