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The evolution within us

机译:我们内心的进化

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摘要

The B-cell immune response is a remarkable evolutionary system found in jawed vertebrates. B-cell receptors, the membrane-bound form of antibodies, are capable of evolving high affinity to almost any foreign protein. High germline diversity and rapid evolution upon encounter with antigen explain the general adaptability of B-cell populations, but the dynamics of repertoires are less well understood. These dynamics are scientifically and clinically important. After highlighting the remarkable characteristics of naive and experienced B-cell repertoires, especially biased usage of genes encoding the B-cell receptors, we contrast methods of sequence analysis and their attempts to explain patterns of B-cell evolution. These phylogenetic approaches are currently unlinked to explicit models of B-cell competition, which analyse repertoire evolution at the level of phenotype, the affinities and specificities to particular antigenic sites. The models, in turn, suggest how chance, infection history and other factors contribute to different patterns of immunodominance and protection between people. Challenges in rational vaccine design, specifically vaccines to induce broadly neutralizing antibodies to HIV, underscore critical gaps in our understanding of B cells' evolutionary and ecological dynamics.
机译:B细胞免疫反应是在颌骨脊椎动物中发现的非凡进化系统。 B细胞受体是抗体的膜结合形式,能够与几乎所有外源蛋白质发展高度亲和力。高种系多样性和遇到抗原后的快速进化解释了B细胞群体的一般适应性,但对库的动态了解较少。这些动力学在科学和临床上都很重要。在强调了朴素和有经验的B细胞功能的显着特征,特别是偏向使用编码B细胞受体的基因后,我们对比了序列分析方法及其尝试解释B细胞进化模式的尝试。这些系统发育方法目前与B细胞竞争的显式模型无关,后者可在表型水平,对特定抗原位点的亲和力和特异性上分析库的进化。这些模型反过来提示机会,感染史和其他因素如何导致人与人之间免疫支配和保护方式的不同。合理疫苗设计的挑战,特别是诱导广泛中和性HIV抗体的疫苗,在我们对B细胞的进化和生态动力学的理解中突显了重要的差距。

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