首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Somatic diversification of S107 from an antiphosphocholine to an anti-DNA autoantibody is due to a single base change in its heavy chain variable region.
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Somatic diversification of S107 from an antiphosphocholine to an anti-DNA autoantibody is due to a single base change in its heavy chain variable region.

机译:S107从抗磷酸胆碱到抗DNA自身抗体的体细胞多样化是由于其重链可变区的单碱基变化。

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摘要

The S107 myeloma cell line expresses the germ-line sequence of the T15 antiphosphocholine (P-Cho) antibody, which is the major antibody made by BALB/c mice in response to P-Cho, either on a variety of bacterial polysaccharides or when attached to a protein carrier. We have previously reported that a somatic mutant of the S107 cell line produces an antibody that has lost the ability to bind P-Cho and has acquired binding for double-stranded DNA. This antibody has a substitution of an alanine for a glutamic acid at residue 35 in the heavy chain variable region. We now show that this amino acid substitution is due to a single A-C transversion, which is the only nucleotide change in the heavy and light chain variable regions. Further, it appears that this change is due to somatic mutation rather than to gene conversion.
机译:S107骨髓瘤细胞系表达T15抗磷酸胆碱(P-Cho)抗体的种系序列,该抗体是BALB / c小鼠针对P-Cho产生的主要抗体,可以在多种细菌多糖上或附着时蛋白质载体。我们以前曾报道过S107细胞系的体细胞突变体产生的抗体失去了结合P-Cho的能力,并获得了对双链DNA的结合。该抗体在重链可变区中的残基35处用谷氨酸取代丙氨酸。现在我们显示该氨基酸取代是由于单个A-C颠换而引起的,这是重链和轻链可变区中唯一的核苷酸变化。此外,似乎这种变化是由于体细胞突变而不是基因转化引起的。

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