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8000名人类的血液DNA病毒群落

The blood DNA virome in 8,000 humans.

作者信息

Moustafa Ahmed, Xie Chao, Kirkness Ewen, Biggs William, Wong Emily, Turpaz Yaron, Bloom Kenneth, Delwart Eric, Nelson Karen E, Venter J Craig, Telenti Amalio

机构信息

Human Longevity Inc., San Diego, California, United States of America.

Human Longevity Singapore Pte. Ltd., Singapore.

出版信息

PLoS Pathog. 2017 Mar 22;13(3):e1006292. doi: 10.1371/journal.ppat.1006292. eCollection 2017 Mar.

Abstract

The characterization of the blood virome is important for the safety of blood-derived transfusion products, and for the identification of emerging pathogens. We explored non-human sequence data from whole-genome sequencing of blood from 8,240 individuals, none of whom were ascertained for any infectious disease. Viral sequences were extracted from the pool of sequence reads that did not map to the human reference genome. Analyses sifted through close to 1 Petabyte of sequence data and performed 0.5 trillion similarity searches. With a lower bound for identification of 2 viral genomes/100,000 cells, we mapped sequences to 94 different viruses, including sequences from 19 human DNA viruses, proviruses and RNA viruses (herpesviruses, anelloviruses, papillomaviruses, three polyomaviruses, adenovirus, HIV, HTLV, hepatitis B, hepatitis C, parvovirus B19, and influenza virus) in 42% of the study participants. Of possible relevance to transfusion medicine, we identified Merkel cell polyomavirus in 49 individuals, papillomavirus in blood of 13 individuals, parvovirus B19 in 6 individuals, and the presence of herpesvirus 8 in 3 individuals. The presence of DNA sequences from two RNA viruses was unexpected: Hepatitis C virus is revealing of an integration event, while the influenza virus sequence resulted from immunization with a DNA vaccine. Age, sex and ancestry contributed significantly to the prevalence of infection. The remaining 75 viruses mostly reflect extensive contamination of commercial reagents and from the environment. These technical problems represent a major challenge for the identification of novel human pathogens. Increasing availability of human whole-genome sequences will contribute substantial amounts of data on the composition of the normal and pathogenic human blood virome. Distinguishing contaminants from real human viruses is challenging.

摘要

血液病毒组的特征对于血液来源的输血产品的安全性以及新兴病原体的识别至关重要。我们探索了来自8240名个体血液全基因组测序的非人类序列数据,这些个体均未被确诊患有任何传染病。病毒序列是从未映射到人类参考基因组的序列读取池中提取的。分析筛选了近1PB的序列数据,并进行了50万亿次相似性搜索。以每10万个细胞中鉴定出2个病毒基因组为下限,我们将序列映射到94种不同的病毒,包括来自19种人类DNA病毒、前病毒和RNA病毒(疱疹病毒、环病毒、乳头瘤病毒、三种多瘤病毒、腺病毒、HIV、HTLV、乙型肝炎病毒、丙型肝炎病毒、细小病毒B19和流感病毒)的序列,在42%的研究参与者中发现了这些病毒。与输血医学可能相关的是,我们在49名个体中鉴定出默克尔细胞多瘤病毒,在13名个体的血液中鉴定出乳头瘤病毒,在6名个体中鉴定出细小病毒B19,在3名个体中发现了疱疹病毒8的存在。两种RNA病毒DNA序列的存在出乎意料:丙型肝炎病毒显示出整合事件,而流感病毒序列是由DNA疫苗免疫导致的。年龄、性别和血统对感染率有显著影响。其余75种病毒大多反映了商业试剂和环境的广泛污染。这些技术问题对新型人类病原体的识别构成了重大挑战。人类全基因组序列可用性的增加将为正常和致病性人类血液病毒组的组成提供大量数据。区分污染物和真正的人类病毒具有挑战性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ad0e/5378407/357d4a19ad44/ppat.1006292.g001.jpg

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