首页> 外文期刊>Journal of immunotherapy >Cytotoxicity of antiosteosarcoma recombinant immunotoxins composed of TP-3 Fv fragments and a truncated Pseudomonas exotoxin A.
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Cytotoxicity of antiosteosarcoma recombinant immunotoxins composed of TP-3 Fv fragments and a truncated Pseudomonas exotoxin A.

机译:由TP-3 Fv片段和截短的假单胞菌外毒素A组成的抗骨肉瘤重组免疫毒素的细胞毒性。

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Regrowth of drug-resistant tumor cells is responsible for approximately half of an unselected osteosarcoma population still dying of the disease despite aggressive combination therapy. Two monoclonal antibodies, TP-1 (immunoglobulin 2a) and TP-3 (immunoglobulin 2b) are available, which specifically recognize an antigen on osteosarcoma cells. In this work, we have fused the variable (V) genes of TP-3 to a truncated fragment of Pseudomonas exotoxin A, referred to as PE38. Two immunotoxins were made that differed in the Fv portion: TP-3(scFv)-PE38, which contains a peptide linker, and TP-3(dsFv)-PE38, which contains a disulfide bond for stabilization of the association between the V domains. Recombinant TP-3 immunotoxins were expressed in Escherichia coli and purified from inclusion bodies. We describe the design and expression of these immunotoxins, and their properties with regard to antigen binding, stability, and cytotoxicity. Toxicity studies were done in mice. We found that the immunotoxins exhibited very similar in vitro properties, whereas in vivo TP-3(dsFv)-PE38 was much better tolerated than TP-3(scFv)-PE38.
机译:尽管积极的联合疗法,抗药性肿瘤细胞的再生还是导致仍死于疾病的未选择的骨肉瘤人口的大约一半。有两种单克隆抗体TP-1(免疫球蛋白2a)和TP-3(免疫球蛋白2b)可以特异性识别骨肉瘤细胞上的抗原。在这项工作中,我们已经将TP-3的可变(V)基因融合到假单胞菌外毒素A的截短片段上,称为PE38。制备了两种在Fv部分有所不同的免疫毒素:TP-3(scFv)-PE38和TP-3(dsFv)-PE38,其中TP-3(scFv)-PE38包含一个肽接头,该二硫键用于稳定V结构域之间的结合。重组TP-3免疫毒素在大肠杆菌中表达,并从包涵体中纯化。我们描述了这些免疫毒素的设计和表达,以及它们在抗原结合,稳定性和细胞毒性方面的特性。在小鼠中进行了毒性研究。我们发现免疫毒素表现出非常相似的体外特性,而体内TP-3(dsFv)-PE38的耐受性比TP-3(scFv)-PE38更好。

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