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Chimeric human antibody molecules: mouse antigen-binding domains with human constant region domains.

机译:嵌合人类抗体分子:具有人类恒定区结构域的小鼠抗原结合结构域。

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摘要

We have created mouse-human antibody molecules of defined antigen-binding specificity by taking the variable region genes of a mouse antibody-producing myeloma cell line with known antigen-binding specificity and joining them to human immunoglobulin constant region genes using recombinant DNA techniques. Chimeric genes were constructed that utilized the rearranged and expressed antigen-binding variable region exons from the myeloma cell line S107, which produces an IgA (kappa) anti-phosphocholine antibody. The heavy chain variable region exon was joined to human IgG1 or IgG2 heavy chain constant region genes, and the light chain variable region exon from the same myeloma was joined to the human kappa light chain gene. These genes were transfected into mouse myeloma cell lines, generating transformed cells that produce chimeric mouse-human IgG (kappa) or IgG (kappa) anti-phosphocholine antibodies. The transformed cell lines remained tumorigenic in mice and the chimeric molecules were present in the ascitic fluids and sera of tumor-bearing mice.
机译:我们通过采用具有已知抗原结合特异性的小鼠抗体生产性骨髓瘤细胞系的可变区基因,并使用重组DNA技术将它们与人免疫球蛋白恒定区基因连接,来创建具有定义的抗原结合特异性的小鼠人抗体分子。构建利用来自骨髓瘤细胞系S107的重排和表达的抗原结合可变区外显子的嵌合基因,该外显子产生IgA(κ)抗磷酸胆碱抗体。重链可变区外显子与人IgG1或IgG2重链恒定区基因连接,来自同一骨髓瘤的轻链可变区外显子与人κ轻链基因连接。这些基因被转染到小鼠骨髓瘤细胞系中,产生转化的细胞,产生嵌合的小鼠-人IgG(κ)或IgG(kappa)抗磷酸胆碱抗体。转化的细胞系在小鼠中仍然具有致瘤性,并且嵌合分子存在于荷瘤小鼠的腹水和血清中。

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