Virology Section, Department of Life Sciences, Shiv Nadar University, Gautam Buddha Nagar, Uttar Pradesh, India.
Gastroenterology, Sanjay Gandhi Postgraduate Institute of Medical Sciences, Lucknow, Uttar Pradesh, India.
J Virol. 2020 Jan 17;94(3). doi: 10.1128/JVI.01327-19.
To gain insight into the impact of mutations on the viability of the hepatitis C virus (HCV) genome, we created a set of full-genome mutant libraries, differing from the parent sequence as well as each other, by using a random mutagenesis approach; the proportion of mutations increased across these libraries with declining template amount or dATP concentration. The replication efficiencies of full-genome mutant libraries ranged between 71 and 329 focus-forming units (FFU) per 10 Huh7.5 cells. Mutant libraries with low proportions of mutations demonstrated low replication capabilities, whereas those with high proportions of mutations had their replication capabilities restored. Hepatoma cells transfected with selected mutant libraries, with low (4 mutations per 10,000 bp copied), moderate (33 mutations), and high (66 mutations) proportions of mutations, and their progeny were subjected to serial passage. Predominant virus variants (mutants) from these mutant libraries (Mutant, Mutant, and Mutant, respectively) were evaluated for changes in growth kinetics and particle-to-FFU unit ratio, virus protein expression, and modulation of host cell protein synthesis. Mutant and Mutant variants produced >3.0-log-higher extracellular progeny per ml than the parent, and Mutant produced progeny at a rate 1.0-log lower. More than 80% of the mutations were in a nonstructural part of the mutant genomes, the majority were nonsynonymous, and a moderate to large proportion were in the conserved regions. Our results suggest that the HCV genome has the ability to overcome lethal/deleterious mutations because of the high reproduction rate but highly selects for random, beneficial mutations. Hepatitis C virus (HCV) displays high genetic heterogeneity, which is partly due to the high reproduction and random substitutions during error-prone genome replication. It is difficult to introduce random substitutions because of limitations in inducing mutagenesis from the 5' end to the 3' end of the genome. Our study has overcome this limitation. We synthesized full-length genomes with few to several random mutations in the background of an HCV clone that can recapitulate all steps of the life cycle. Our study provides evidence of the capability of the HCV genome to overcome deleterious mutations and remain viable. Mutants that emerged from the libraries had diverse phenotype profiles compared to the parent, and putative adaptive mutations mapped to segments of the conserved nonstructural genome. We demonstrate the potential utility of our system for the study of sequence variation that ensures the survival and adaptation of HCV.
为了深入了解突变对丙型肝炎病毒 (HCV) 基因组活力的影响,我们使用随机诱变方法创建了一套全基因组突变文库,这些文库与亲本序列以及彼此之间均存在差异;随着模板数量或 dATP 浓度的降低,突变的比例在这些文库中增加。全基因组突变文库的复制效率在每 10 个 Huh7.5 细胞中为 71 至 329 个焦点形成单位 (FFU) 之间。突变比例低的突变文库表现出低的复制能力,而突变比例高的文库则恢复了其复制能力。用低比例(每 10000bp 复制 4 个突变)、中比例(33 个突变)和高比例(66 个突变)突变的选定突变文库转染肝癌细胞,并对其后代进行连续传代。从这些突变文库中选择的突变体文库(分别为突变体、突变体和突变体)中的优势病毒变体(突变体)的生长动力学和颗粒与 FFU 单位比、病毒蛋白表达以及宿主细胞蛋白合成的调节变化进行评估。突变体和突变体变体产生的细胞外子代比亲本高出 >3.0-log,而突变体产生的子代速度低 1.0-log。突变基因组的非结构部分有超过 80%的突变,其中大多数为非同义突变,而且在保守区域中有中等至较大比例的突变。我们的结果表明,由于高复制率,HCV 基因组具有克服致死/有害突变的能力,但高度选择随机有益突变。丙型肝炎病毒 (HCV) 显示出高度的遗传异质性,这部分是由于在易错基因组复制过程中高复制和随机取代。由于在从基因组 5' 端到 3' 端诱导突变方面存在限制,因此难以引入随机取代。我们的研究克服了这一限制。我们合成了全长基因组,在可以重现生命周期所有步骤的 HCV 克隆背景下具有少数到几个随机突变。我们的研究提供了 HCV 基因组克服有害突变并保持活力的能力的证据。与亲本相比,文库中出现的突变体具有不同的表型特征,而假定的适应性突变映射到保守非结构基因组的片段上。我们展示了我们的系统用于研究确保 HCV 存活和适应的序列变异的潜在用途。
