Somatic Hypermutation in T-Independent and T-Dependent Immune Responses toHaemophilus influenzaeType b Polysaccharide

Elisabeth E. Adderson, Penelope G. Shackelford, William L. Carroll
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引用次数: 12

Abstract

Secondary immune responses to T-independent antigens are characterized by little or no affinity maturation, a phenomenon attributed to limited somatic hypermutation. In the human immune response toHaemophilus influenzaetype b capsular polysaccharide, however, there are numerous differences between rearranged heavy chain variable region gene segments and candidate germline genes, irrespective of antigen presentation in a T-independent or T-dependent form. To determine the characteristics of somatic hypermutation in this response, we analyzed rearranged heavy chain variable region segments and associated 3′ untranslated JH4–JH5 introns from monoclonal anti-Hib PS antibodies. Mutation of untranslated introns and heavy chain variable segments in both T-independent and T-dependent responses resembles that described in murine and unselected human immune responses. Although mutation is frequent in both T-independent and T-dependent anti-Hib PS responses, there is little evidence of antigen-driven selection, suggesting that ongoing pressure to conserve the variable segment germline configuration limits affinity maturation in this immune response.

对流感嗜血杆菌b型多糖的t独立和t依赖免疫反应的体细胞超突变
对t非依赖性抗原的二次免疫反应的特征是很少或没有亲和成熟,这一现象归因于有限的体细胞超突变。然而,在人类对流感嗜血杆菌b型荚膜多糖的免疫应答中,重排的重链可变区基因片段和候选种系基因之间存在许多差异,无论抗原呈递是t依赖型还是t依赖型。为了确定这种反应中体细胞超突变的特征,我们分析了来自单克隆抗hib PS抗体的重排重链可变区片段和相关的3 '未翻译的JH4-JH5内含子。非翻译内含子和重链可变片段在t独立和t依赖反应中的突变类似于在小鼠和未选择的人类免疫反应中所描述的。尽管突变在t非依赖性和t依赖性抗hib PS反应中都很常见,但很少有证据表明抗原驱动选择,这表明持续的保护可变片段种系结构的压力限制了这种免疫反应的亲和成熟。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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