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丙型肝炎病毒免疫原设计的经验性适应性模型

Empirical fitness models for hepatitis C virus immunogen design.

作者信息

Hart Gregory R, Ferguson Andrew L

机构信息

Department of Physics, University of Illinois at Urbana-Champaign, Urbana, IL 61801, USA.

出版信息

Phys Biol. 2015 Nov 24;12(6):066006. doi: 10.1088/1478-3975/12/6/066006.

DOI:10.1088/1478-3975/12/6/066006
PMID:26599153
Abstract

UNLABELLED

Hepatitis C virus (HCV) afflicts 170 million people worldwide, 2%-3% of the global population, and kills 350 000 each year. Prophylactic vaccination offers the most realistic and cost effective hope of controlling this epidemic in the developing world where expensive drug therapies are not available. Despite 20 years of research, the high mutability of the virus and lack of knowledge of what constitutes effective immune responses have impeded development of an effective vaccine. Coupling data mining of sequence databases with spin glass models from statistical physics, we have developed a computational approach to translate clinical sequence databases into empirical fitness landscapes quantifying the replicative capacity of the virus as a function of its amino acid sequence. These landscapes explicitly connect viral genotype to phenotypic fitness, and reveal vulnerable immunological targets within the viral proteome that can be exploited to rationally design vaccine immunogens. We have recovered the empirical fitness landscape for the HCV RNA-dependent RNA polymerase (protein NS5B) responsible for viral genome replication, and validated the predictions of our model by demonstrating excellent accord with experimental measurements and clinical observations. We have used our landscapes to perform exhaustive in silico screening of 16.8 million T-cell immunogen candidates to identify 86 optimal formulations. By reducing the search space of immunogen candidates by over five orders of magnitude, our approach can offer valuable savings in time, expense, and labor for experimental vaccine development and accelerate the search for a HCV vaccine.

ABBREVIATIONS

HCV-hepatitis C virus, HLA-human leukocyte antigen, CTL-cytotoxic T lymphocyte, NS5B-nonstructural protein 5B, MSA-multiple sequence alignment, PEG-IFN-pegylated interferon.

摘要

未标注

丙型肝炎病毒(HCV)在全球感染了1.7亿人,占全球人口的2%-3%,每年导致35万人死亡。预防性疫苗接种为在无法获得昂贵药物治疗的发展中世界控制这一流行病提供了最现实且具成本效益的希望。尽管经过20年的研究,但该病毒的高变异性以及对有效免疫反应构成因素的缺乏了解阻碍了有效疫苗的研发。通过将序列数据库的数据挖掘与统计物理学中的自旋玻璃模型相结合,我们开发了一种计算方法,将临床序列数据库转化为经验适应度景观,量化病毒作为其氨基酸序列函数的复制能力。这些景观明确地将病毒基因型与表型适应度联系起来,并揭示病毒蛋白质组中可被利用以合理设计疫苗免疫原的易受攻击的免疫靶点。我们已经恢复了负责病毒基因组复制的HCV RNA依赖RNA聚合酶(蛋白质NS5B)的经验适应度景观,并通过证明与实验测量和临床观察的极佳一致性来验证我们模型的预测。我们利用这些景观对1680万个T细胞免疫原候选物进行了详尽的计算机模拟筛选,以确定86种最佳配方。通过将免疫原候选物的搜索空间减少五个以上数量级,我们的方法可为实验性疫苗开发节省宝贵的时间、费用和劳动力,并加速寻找HCV疫苗的进程。

缩写

HCV-丙型肝炎病毒,HLA-人类白细胞抗原,CTL-细胞毒性T淋巴细胞,NS5B-非结构蛋白5B,MSA-多序列比对,PEG-IFN-聚乙二醇化干扰素

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