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在注射吸毒人群中丙型肝炎病毒的宿主内进化动态。

Intra-host evolutionary dynamics of the hepatitis C virus among people who inject drugs.

机构信息

British Columbia Centre for Excellence in HIV/AIDS, Vancouver, BC, Canada.

British Columbia Centre for Disease Control, Vancouver, BC, Canada.

出版信息

Sci Rep. 2021 May 11;11(1):9986. doi: 10.1038/s41598-021-88132-8.

Abstract

Most individuals chronically infected with hepatitis C virus (HCV) are asymptomatic during the initial stages of infection and therefore the precise timing of infection is often unknown. Retrospective estimation of infection duration would improve existing surveillance data and help guide treatment. While intra-host viral diversity quantifications such as Shannon entropy have previously been utilized for estimating duration of infection, these studies characterize the viral population from only a relatively short segment of the HCV genome. In this study intra-host diversities were examined across the HCV genome in order to identify the region most reflective of time and the degree to which these estimates are influenced by high-risk activities including those associated with HCV acquisition. Shannon diversities were calculated for all regions of HCV from 78 longitudinally sampled individuals with known seroconversion timeframes. While the region of the HCV genome most accurately reflecting time resided within the NS3 gene, the gene region with the highest capacity to differentiate acute from chronic infections was identified within the NS5b region. Multivariate models predicting duration of infection from viral diversity significantly improved upon incorporation of variables associated with recent public, unsupervised drug use. These results could assist the development of strategic population treatment guidelines for high-risk individuals infected with HCV and offer insights into variables associated with a likelihood of transmission.

摘要

大多数慢性丙型肝炎病毒(HCV)感染者在感染的初始阶段无症状,因此感染的确切时间往往未知。回顾性估计感染持续时间将改善现有监测数据,并有助于指导治疗。虽然宿主内病毒多样性定量分析,如香农熵,以前曾用于估计感染持续时间,但这些研究仅对 HCV 基因组的相对较短片段进行病毒种群特征描述。在这项研究中,对 HCV 基因组中的宿主内多样性进行了检查,以确定最能反映时间的区域,以及这些估计受高风险活动(包括与 HCV 获得相关的活动)影响的程度。对 78 名具有已知血清转化时间框架的纵向采样个体的 HCV 所有区域进行了香农多样性计算。虽然最能准确反映时间的 HCV 基因组区域位于 NS3 基因内,但在 NS5b 区域内确定了具有最高区分急性和慢性感染能力的基因区域。从病毒多样性预测感染持续时间的多元模型显著提高了与最近公共、无人监督药物使用相关变量的纳入。这些结果可能有助于为感染 HCV 的高危人群制定战略人群治疗指南,并提供与传播可能性相关的变量的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1ea9/8113533/adfb010ef5a4/41598_2021_88132_Fig1_HTML.jpg

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