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丙型肝炎病毒患者体内种群中重组的证据。

Evidence of recombination in intrapatient populations of hepatitis C virus.

作者信息

Sentandreu Vicente, Jiménez-Hernández Nuria, Torres-Puente Manuela, Bracho María Alma, Valero Ana, Gosalbes María José, Ortega Enrique, Moya Andrés, González-Candelas Fernando

机构信息

Institut Cavanilles de Biodiversitat i Biologia Evolutiva, Universitat de València Valencia, Spain.

出版信息

PLoS One. 2008 Sep 18;3(9):e3239. doi: 10.1371/journal.pone.0003239.

Abstract

Hepatitis C virus (HCV) is a major cause of liver disease worldwide and a potential cause of substantial morbidity and mortality in the future. HCV is characterized by a high level of genetic heterogeneity. Although homologous recombination has been demonstrated in many members of the family Flaviviridae, to which HCV belongs, there are only a few studies reporting recombination on natural populations of HCV, suggesting that these events are rare in vivo. Furthermore, these few studies have focused on recombination between different HCV genotypes/subtypes but there are no reports on the extent of intra-genotype or intra-subtype recombination between viral strains infecting the same patient. Given the important implications of recombination for RNA virus evolution, our aim in this study has been to assess the existence and eventually the frequency of intragenic recombination on HCV. For this, we retrospectively have analyzed two regions of the HCV genome (NS5A and E1-E2) in samples from two different groups: (i) patients infected only with HCV (either treated with interferon plus ribavirin or treatment naïve), and (ii) HCV-HIV co-infected patients (with and without treatment against HIV). The complete data set comprised 17712 sequences from 136 serum samples derived from 111 patients. Recombination analyses were performed using 6 different methods implemented in the program RDP3. Recombination events were considered when detected by at least 3 of the 6 methods used and were identified in 10.7% of the amplified samples, distributed throughout all the groups described and the two genomic regions studied. The resulting recombination events were further verified by detailed phylogenetic analyses. The complete experimental procedure was applied to an artificial mixture of relatively closely viral populations and the ensuing analyses failed to reveal artifactual recombination. From these results we conclude that recombination should be considered as a potentially relevant mechanism generating genetic variation in HCV and with important implications for the treatment of this infection.

摘要

丙型肝炎病毒(HCV)是全球肝脏疾病的主要病因,也是未来导致大量发病和死亡的潜在原因。HCV的特点是基因异质性水平高。尽管在HCV所属的黄病毒科的许多成员中已证实存在同源重组,但关于HCV自然群体中重组的研究仅有少数几篇,这表明这些事件在体内很少见。此外,这少数研究聚焦于不同HCV基因型/亚型之间的重组,但尚无关于感染同一患者的病毒株之间基因型内或亚型内重组程度的报道。鉴于重组对RNA病毒进化具有重要意义,我们在本研究中的目的是评估HCV基因内重组的存在情况以及最终的频率。为此,我们回顾性分析了来自两个不同组样本中HCV基因组的两个区域(NS5A和E1-E2):(i)仅感染HCV的患者(接受过干扰素加利巴韦林治疗或未接受过治疗),以及(ii)HCV-HIV合并感染患者(接受或未接受抗HIV治疗)。完整的数据集包括来自111例患者的136份血清样本中的17712个序列。使用RDP3程序中实现的6种不同方法进行重组分析。当通过所使用的6种方法中的至少3种检测到重组事件时才予以考虑,在10.7%的扩增样本中鉴定出了重组事件,这些样本分布在所有描述的组以及所研究的两个基因组区域中。通过详细的系统发育分析进一步验证了所产生的重组事件。将完整的实验程序应用于相对密切相关的病毒群体的人工混合物,随后的分析未能揭示人为重组。从这些结果我们得出结论,重组应被视为在HCV中产生遗传变异的潜在相关机制,并且对这种感染的治疗具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ddab/2528950/2bf671109bfb/pone.0003239.g001.jpg

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