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治疗性重组免疫毒素的免疫原性。

Immunogenicity of therapeutic recombinant immunotoxins.

作者信息

Mazor Ronit, Onda Masanori, Pastan Ira

机构信息

Laboratory of Molecular Biology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD, USA.

出版信息

Immunol Rev. 2016 Mar;270(1):152-64. doi: 10.1111/imr.12390.

Abstract

Recombinant immunotoxins (RITs) are chimeric proteins designed to treat cancer. They are made up of an Fv or Fab that targets an antigen on a cancer cell fused to a 38-kDa portion of Pseudomonas exotoxin A (PE38). Because PE38 is a bacterial protein, it is highly immunogenic in patients with solid tumors that have normal immune systems, but much less immunogenic in patients with hematologic malignancies where the immune system is suppressed. RITs have shown efficacy in refractory hairy cell leukemia and in some children with acute lymphoblastic leukemia, but have been much less effective in solid tumors, because neutralizing antibodies develop and prevent additional treatment cycles. In this paper we will (i) review data from clinical trials describing the immunogenicity of PE38 in different patient populations; (ii) review results from clinical trials using different immunosuppressive drugs; and (iii) describe our efforts to make new less-immunogenic RITs by identifying and removing T- and B-cell epitopes to hide the RIT from the immune system.

摘要

重组免疫毒素(RITs)是用于治疗癌症的嵌合蛋白。它们由靶向癌细胞上抗原的Fv或Fab与铜绿假单胞菌外毒素A(PE38)的38 kDa部分融合而成。由于PE38是一种细菌蛋白,在免疫系统正常的实体瘤患者中具有高度免疫原性,但在免疫系统受到抑制的血液系统恶性肿瘤患者中免疫原性要低得多。RITs已在难治性毛细胞白血病和一些急性淋巴细胞白血病儿童中显示出疗效,但在实体瘤中效果要差得多,因为会产生中和抗体并阻止后续治疗周期。在本文中,我们将(i)回顾来自临床试验的数据,这些数据描述了PE38在不同患者群体中的免疫原性;(ii)回顾使用不同免疫抑制药物的临床试验结果;(iii)描述我们通过识别和去除T细胞和B细胞表位以使RIT躲避免疫系统来制备新的低免疫原性RITs的努力。

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