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流感感染中和抗体库中祖B细胞多样性与免疫显性。

Immunodominance with progenitor B cell diversity in the neutralizing antibody repertoire to influenza infection.

作者信息

Patera A C, Graham C M, Thomas D B, Smith C A

机构信息

National Institute for Medical Research, Mill Hill, London.

出版信息

Eur J Immunol. 1995 Jul;25(7):1803-9. doi: 10.1002/eji.1830250702.

Abstract

We report striking immunodominance in the neutralizing antibody responses of major histocompatibility complex congenic mice to natural infection with influenza virus (H3N2 subtype), as deduced by sequencing the hemagglutinin (HA) genes of monoclonal antibody (mAb)-selected mutant viruses. A majority of mAb, established from individual BALB/c (H-2d) mice, select mutant viruses containing the same single amino acid substitution in the membrane distal ecto-domain, HA1 198 A-->E, whereas changes at either HA1 158 G-->E or HA1 198 A-->E are selected for by mAb from BALB.K (H-2k) donors. The structural basis for immunodominance, and potential diversity of progenitor B cells, was investigated by sequence analysis of H and L chain gene rearrangements in mAb specific for HA1 158 or HA1 198. No correlation was found between antibody specificity and VH or VL gene usage, and a minimum of three to six progenitor cells contributed to the individual's repertoire for a single antigenic site. However, in a further analysis of the HA1 158-specific antibody response of CBA/Ca (H-2k) donors, there was highly restricted light chain gene usage. Focusing of the immune repertoire to limited regions of the HA molecule during a primary viral infection may be a significant factor in immune pressure for antigenic variation, particularly since there is no evident restriction in the antibody response to immunization.

摘要

通过对单克隆抗体(mAb)筛选的突变病毒的血凝素(HA)基因进行测序,我们发现主要组织相容性复合体同基因小鼠对流感病毒(H3N2亚型)自然感染的中和抗体反应中存在显著的免疫显性。从个体BALB/c(H-2d)小鼠中建立的大多数mAb选择了在膜远端胞外结构域HA1 198处含有相同单氨基酸取代(A→E)的突变病毒,而来自BALB.K(H-2k)供体的mAb选择了HA1 158处(G→E)或HA1 198处(A→E)的变化。通过对HA1 158或HA1 198特异性mAb的H链和L链基因重排进行序列分析,研究了免疫显性的结构基础以及祖B细胞的潜在多样性。未发现抗体特异性与VH或VL基因使用之间的相关性,并且至少三到六个祖细胞对个体针对单个抗原位点的抗体库有贡献。然而,在对CBA/Ca(H-2k)供体的HA1 158特异性抗体反应的进一步分析中,轻链基因的使用受到高度限制。在原发性病毒感染期间,免疫库聚焦于HA分子的有限区域可能是抗原变异免疫压力的一个重要因素,特别是因为对免疫接种的抗体反应没有明显的限制。

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