一种通过添加二硫键来提高稳定性的重组免疫毒素,其免疫原性降低。
A recombinant immunotoxin engineered for increased stability by adding a disulfide bond has decreased immunogenicity.
机构信息
Laboratory of Molecular Biology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, 37 Convent Drive, Bethesda, MD 20892-4264, USA.
出版信息
Protein Eng Des Sel. 2012 Jan;25(1):1-6. doi: 10.1093/protein/gzr053. Epub 2011 Nov 17.
Abstract
Recombinant immunotoxins (RITs) are anti-cancer agents that combine the Fv of an antibody against cancer cells with a protein toxin from bacteria or plants. Since RITs contain a non-human protein, immunogenicity can be an obstacle in their development. In this study, we have explored the hypothesis that increasing stability can reduce the immunogenicity of a RIT using HA22-LR, which is composed of an anti-CD22 Fv fused to domain III of Pseudomonas exotoxin A. We introduced a disulfide bond into domain III by identifying and mutating two structurally adjacent residues to cysteines at sites suggested by computer modeling. This RIT, HA22-LR-DB, displays a remarkable increase in thermal stability and an enhanced resistance to trypsin degradation. In addition, HA22-LR-DB retains cytotoxic and anti-tumor activity, while exhibiting significantly lower immunogenicity in mice. This study demonstrates that it is possible to design mutations in a protein molecule that will increase the stability of the protein and thereby reduce its immunogenicity.
摘要
重组免疫毒素(RIT)是一种抗癌药物,它将针对癌细胞的抗体 Fv 与来自细菌或植物的蛋白毒素结合在一起。由于 RIT 含有非人类蛋白,因此免疫原性可能是其发展的一个障碍。在这项研究中,我们通过引入二硫键来探索假设,即通过增加稳定性可以降低 RIT 的免疫原性,所使用的 RIT 是由抗 CD22 Fv 与假单胞菌外毒素 A 的结构域 III 融合而成的。我们通过识别和突变两个结构上相邻的残基,将其突变为计算机建模提示的半胱氨酸,从而在结构域 III 中引入了二硫键。这种 RIT,HA22-LR-DB,显示出热稳定性的显著提高和对胰蛋白酶降解的增强抗性。此外,HA22-LR-DB 保留了细胞毒性和抗肿瘤活性,同时在小鼠中表现出明显较低的免疫原性。这项研究表明,有可能对蛋白分子进行设计突变,从而增加蛋白的稳定性,从而降低其免疫原性。
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