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马细胞色素c1三个抗原区域中的多个重叠表位。

Multiple overlapping epitopes in the three antigenic regions of horse cytochrome c1.

作者信息

Jemmerson R

出版信息

J Immunol. 1987 Jan 1;138(1):213-9.

PMID:2431055
Abstract

To gain a better understanding of the diversity of epitopes on a protein, the specificities of 103 monoclonal antibodies to a model antigen, horse cytochrome c(cyt c), were analyzed. The antibodies were generated in in vitro monoclonal, secondary antibody responses against horse cyt c coupled to hemocyanin in splenic fragment cultures. For this assay, horse cyt c-primed murine B lymphocytes were transferred to irradiated, hemocyanin-primed recipients. A panel of seven mammalian cyts c differing at one to six residues out of 104 and cyanogen bromide-cleaved fragments of horse cyt c containing residues 1-65, 1-80, and 66-104 was used to examine the specificities of the antibodies. Twenty-two distinct reactivity patterns were observed, even though the majority of the monoclonal antibodies were found to bind in the three previously identified antigenic regions of the molecule about residues 44-47, 60-62, and 89-92. The results indicate that each of the three antigenic regions consists of multiple overlapping epitopes. Few of the antibodies directed to any given antigenic region bound polypeptide fragments inclusive of the epitope sequences, demonstrating that some antibodies were more conformationally dependent than others. Only 13% of the antibodies bound to cyanogen bromide-cleaved polypeptide fragments that together encompassed the entire length of the protein. Considering the large number of antibodies analyzed and the reoccurrence of 13 of the 22 clonotypes in different lymphocyte donors, it is likely that the antibody specificities tabulated herein approach yet do not completely enumerate the total inventory of the horse cyt c-specific B cell repertoire. The remarkable diversity for epitope recognition within antigenic regions observed here is likely to pertain to protein antigens in general, and strongly supports the widely held notion that the entire surface of a protein is potentially antigenic. The restriction of the epitopes of horse cyt c to three antigenic regions where the amino acid sequences of the mammalian cyts c differ probably results from tolerance of the mice to their own cyt c.

摘要

为了更好地理解蛋白质表位的多样性,分析了针对模型抗原马细胞色素c(cyt c)的103种单克隆抗体的特异性。这些抗体是在体外单克隆二级抗体反应中产生的,该反应针对与血蓝蛋白偶联的马cyt c在脾细胞片段培养物中进行。对于该测定,将用马cyt c免疫的小鼠B淋巴细胞转移到经辐照、用血蓝蛋白免疫的受体中。使用一组七种哺乳动物的cyt c,它们在104个残基中有1至6个残基不同,以及马cyt c的溴化氰裂解片段,包含残基1 - 65、1 - 80和66 - 104,来检测抗体的特异性。尽管发现大多数单克隆抗体结合在分子先前确定的三个抗原区域,即约残基44 - 47、60 - 62和89 - 92处,但仍观察到22种不同的反应模式。结果表明,这三个抗原区域中的每一个都由多个重叠表位组成。很少有针对任何给定抗原区域的抗体结合包含表位序列的多肽片段,这表明一些抗体比其他抗体更依赖构象。只有13%的抗体结合到一起涵盖了蛋白质全长的溴化氰裂解多肽片段。考虑到分析的抗体数量众多以及22种克隆型中有13种在不同淋巴细胞供体中再次出现,本文列出的抗体特异性可能接近但并未完全列举出马cyt c特异性B细胞库的全部清单。此处观察到的抗原区域内表位识别的显著多样性可能普遍适用于蛋白质抗原,并有力地支持了广泛持有的观点,即蛋白质的整个表面都可能具有抗原性。马cyt c的表位局限于三个抗原区域,其中哺乳动物cyt c的氨基酸序列不同,这可能是由于小鼠对自身cyt c产生了耐受性。

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