Specific capture and whole-genome sequencing of viruses from clinical samples

Specific capture and whole-genome sequencing of viruses from clinical samples

Whole genome sequencing of viruses directly from clinical samples is integral for understanding the genetics of host-virus interactions. Here, we report the use of sample sparing target enrichment (by hybridisation) for viral nucleic acid separation and deep-sequencing of herpesvirus genomes directl...

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Veröffentlicht in:PloS one 2011-11, Vol.6 (11), p.e27805-e27805
Hauptverfasser: Depledge, Daniel P, Palser, Anne L, Watson, Simon J, Lai, Imogen Yi-Chun, Gray, Eleanor R, Grant, Paul, Kanda, Ravinder K, Leproust, Emily, Kellam, Paul, Breuer, Judith
Format: Artikel
Sprache:eng
Schlagworte:
Acquired immune deficiency syndrome
AIDS
Amino acids
Bioinformatics
Biology
Cell Line, Tumor
Cerebrospinal fluid
Chicken pox
College campuses
Deoxyribonucleic acid
DNA
DNA sequencing
DNA, Viral - chemistry
DNA, Viral - genetics
Drug therapy
Gene sequencing
Genetic aspects
Genetics
Genome, Viral - genetics
Genomes
Genomics
Herpesviridae - classification
Herpesviridae - genetics
Herpesviridae Infections - blood
Herpesviridae Infections - cerebrospinal fluid
Herpesviridae Infections - virology
Herpesvirus 3, Human - genetics
Herpesvirus 4, Human - genetics
Herpesvirus 8, Human - genetics
HIV
Human immunodeficiency virus
Humans
Infections
Lymphoma
Methods
Mutation
Nucleic acids
Pathogenesis
Polymerase Chain Reaction
Population
Population studies
Reproducibility of Results
Saliva
Saliva - virology
Sequence Analysis, DNA - methods
Species Specificity
Tumor cell lines
Tumors
Vaccines
Viruses
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Zusammenfassung:Whole genome sequencing of viruses directly from clinical samples is integral for understanding the genetics of host-virus interactions. Here, we report the use of sample sparing target enrichment (by hybridisation) for viral nucleic acid separation and deep-sequencing of herpesvirus genomes directly from a range of clinical samples including saliva, blood, virus vesicles, cerebrospinal fluid, and tumour cell lines. We demonstrate the effectiveness of the method by deep-sequencing 13 highly cell-associated human herpesvirus genomes and generating full length genome alignments at high read depth. Moreover, we show the specificity of the method enables the study of viral population structures and their diversity within a range of clinical samples types.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0027805