首页> 外文期刊>British Journal of Cancer >Generation of chimeric bispecific G250/anti-CD3 monoclonal antibody, a tool to combat renal cell carcinoma
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Generation of chimeric bispecific G250/anti-CD3 monoclonal antibody, a tool to combat renal cell carcinoma

机译:嵌合双特异性G250 /抗CD3单克隆抗体的产生,一种抗击肾细胞癌的工具

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摘要

The monoclonal antibody (MAb) G250 binds to a tumour-associated antigen, expressed in renal cell carcinoma (RCC), which has been demonstrated to be a suitable target for antibody-mediated immunotherapy. A bispecific antibody having both G250 and anti-CD3 specificity can cross-link G250 antigen-expressing RCC target cells with T cells and can mediate lysis of such targets. Therapy studies with murine antibodies are limited by immune responses to the antibodies injected (HAMA response), which can be decreased by using chimeric antibodies. We generated a chimeric bispecific G250/anti CD3 MAb by transfecting chimeric genes of heavy and light chains for both the G250 MAb and the anti-CD3 MAb into a myeloma cell line. Cytotoxicity assays revealed that the chimeric bispecific MAb was capable of mediating lysis of RCC cell lines by cloned human CD8+T cells or by IL-2-stimulated peripheral blood lymphocytes (PBLs). Lysis mediated by the MAb was specific for target cells that expressed the G250 antigen and was effective at concentrations as low as 0.01 microgram ml-1. The chimeric bispecific G250/anti-CD3 MAb produced may be an effective adjuvant to the currently used IL-2-based therapy of advanced renal cell arcinoma.
机译:单克隆抗体(MAb)G250与在肾细胞癌(RCC)中表达的肿瘤相关抗原结合,该抗原已被证明是抗体介导的免疫疗法的合适靶标。同时具有G250和抗CD3特异性的双特异性抗体可以使表达G250抗原的RCC靶细胞与T细胞交联,并介导此类靶的裂解。鼠抗体的治疗研究受到对注射抗体的免疫应答(HAMA应答)的限制,使用嵌合抗体可以降低免疫应答。通过将G250 MAb和抗CD3 MAb的重链和轻链嵌合基因转染到骨髓瘤细胞系中,我们产生了嵌合双特异性G250 /抗CD3 MAb。细胞毒性试验表明,嵌合双特异性MAb能够通过克隆的人CD8 + T细胞或IL-2刺激的外周血淋巴细胞(PBL)介导RCC细胞系的裂解。 MAb介导的裂解对表达G250抗原的靶细胞具有特异性,并且在低至0.01微克ml-1的浓度下有效。产生的嵌合双特异性G250 /抗CD3 MAb可能是目前使用的基于IL-2的晚期肾细胞弓形瘤治疗的有效佐剂。

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