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Genetic control of B cell function. III. IgVH-controlled polymorphism in the frequencies of B cells that recognize xenogeneic red blood cells.

作者信息

Saizawa K M, Melchers I, Eichmann K

出版信息

Eur J Immunol. 1985 Feb;15(2):124-31. doi: 10.1002/eji.1830150205.

DOI:10.1002/eji.1830150205
PMID:3918870
Abstract

Previous work has shown that the primary IgM plaque-forming cell response of inbred mice to xenogeneic red blood cells (RBC) including sheep, horse and chicken RBC is under the control of two polymorphic genes or sets of genes, one linked to the Igh linkage group and the other of unknown linkage but unlinked to H-2 and a variety of other known genetic markers. Both genes together control B cell function but do not influence the function of T cells and macrophages. Thus, this system permits the study of two polymorphic loci that control B cell responsiveness. In this study we analyze the role of the Igh region in further detail. In bulk cultures and limiting dilution experiments, we confirm its exclusive influence on B cells also when analyzed separately from the background gene, i.e. in Igh-congenic strains. Moreover, we find in the majority of experiments 4-5-fold differences in sheep RBC-specific B cell precursor frequencies among lipopolysaccharide-reactive cells from 3 pairs of Igh-congenic high and low-responder strains. Similar frequency differences exist for horse RBC and chicken RBC-specific B cells but not for B cells with specificity for (4-hydroxy-5-iodo-3-nitrophenyl)acetyl (NIP)-gelatine. These differences are independent of the frequencies of B cells responding to lipopolysaccharide which are shown to be equal between Igh-congenic pairs of strains. Since the differences in RBC-specific B cell frequencies closely resemble the differences in bulk culture responses to the corresponding RBC, we conclude that the role of the Igh linkage group in controlling responsiveness to RBC lies in a selective influence on the B cell repertoire concerning precursor cells for RBC specificity. In addition, we find that the VH part of Igh is responsible for the observed frequency differences, suggesting that VH germ-line genes directly influence the composition of the mature B cell repertoire.

摘要

相似文献

1
Genetic control of B cell function. III. IgVH-controlled polymorphism in the frequencies of B cells that recognize xenogeneic red blood cells.
Eur J Immunol. 1985 Feb;15(2):124-31. doi: 10.1002/eji.1830150205.
2
H-2-linked Ir gene control of VH determinant(s)-specific helper T cells.H-2连锁Ir基因对VH决定簇特异性辅助性T细胞的控制。
J Mol Cell Immunol. 1986;2(5):255-64.
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Genetic control of B cell function. II. Antibody responses of inbred mice to red blood cells are controlled at the B cell level.B细胞功能的遗传控制。II. 近交系小鼠对红细胞的抗体反应在B细胞水平受到控制。
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Frequency analysis of functional immunoglobulin C- and V-gene expression by mitogen-reactive B cells in germfree mice fed chemically defined ultra-filtered "antigen-free" diet.在无菌小鼠中,对喂食化学定义的超滤“无抗原”饮食的丝裂原反应性B细胞的功能性免疫球蛋白C基因和V基因表达进行频率分析。
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The expression of a set of antibody variable regions in lipopolysaccharide-reactive B cells at various stages of ontogeny and its control by anti-idiotypic antibody.一组抗体可变区在个体发育不同阶段的脂多糖反应性B细胞中的表达及其受抗独特型抗体的调控。
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Neonatal and adult primary B cells use the same germ-line VH and V kappa genes in their (T,G)-A-L-specific repertoire.新生儿和成人的原发性B细胞在其(T,G)-A-L特异性库中使用相同的种系VH和Vκ基因。
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Homologies between cell interaction molecules controlled by major histocompatibility complex- and Igh-V-linked genes that T cells use for communication; both molecules undergo "adaptive" differentiation in the thymus.主要组织相容性复合体和免疫球蛋白重链可变区(Igh-V)连锁基因所控制的、T细胞用于通讯的细胞相互作用分子之间的同源性;这两种分子在胸腺中都经历“适应性”分化。
Eur J Immunol. 1983 Apr;13(4):285-91. doi: 10.1002/eji.1830130404.

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