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Basic Characteristics of Mutations
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Mutation Site
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M204V |
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Mutation Site Sentence
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Among hypermutated UDPS sequence reads, the G → A mutations M204I (7.6%) and A181T (2.9%) were the most common drug-resistance mutations, followed by M204V (0.03%), S202G (0.03%), M250V (0.02%), V173L (0.01%) and T184I (0.01%), which are not caused by G → A substitutions. |
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Mutation Level
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Amino acid level |
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Mutation Type
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Nonsynonymous substitution |
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Gene/Protein/Region
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RT |
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Standardized Encoding Gene
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P
|
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Genotype/Subtype
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- |
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Viral Reference
|
-
|
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Functional Impact and Mechanisms
|
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Disease
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Hepatitis B Virus Infection
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Immune
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- |
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Target Gene
|
-
|
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Clinical and Epidemiological Correlations
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Clinical Information
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- |
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Treatment
|
- |
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Location
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- |
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Literature Information
|
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PMID
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20937597
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Title
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A classification model for G-to-A hypermutation in hepatitis B virus ultra-deep pyrosequencing reads
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Author
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Reuman EC,Margeridon-Thermet S,Caudill HB,Liu T,Borroto-Esoda K,Svarovskaia ES,Holmes SP,Shafer RW
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Journal
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Bioinformatics (Oxford, England)
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Journal Info
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2010 Dec 1;26(23):2929-32
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Abstract
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MOTIVATION: G --> A hypermutation is an innate antiviral defense mechanism, mediated by host enzymes, which leads to the mutational impairment of viruses. Sensitive and specific identification of host-mediated G --> A hypermutation is a novel sequence analysis challenge, particularly for viral deep sequencing studies. For example, two of the most common hepatitis B virus (HBV) reverse transcriptase (RT) drug-resistance mutations, A181T and M204I, arise from G --> A changes and are routinely detected as low-abundance variants in nearly all HBV deep sequencing samples. RESULTS: We developed a classification model using measures of G --> A excess and predicted indicators of lethal mutation and applied this model to 325 920 unique deep sequencing reads from plasma virus samples from 45 drug treatment-naive HBV-infected individuals. The 2.9% of sequence reads that were classified as hypermutated by our model included most of the reads with A181T and/or M204I, indicating the usefulness of this model for distinguishing viral adaptive changes from host-mediated viral editing. AVAILABILITY: Source code and sequence data are available at http://hivdb.stanford.edu/pages/resources.html. CONTACT: ereuman@stanfordalumni.org SUPPLEMENTARY INFORMATION: Supplementary data are available at Bioinformatics online.
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Sequence Data
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SupplementaryDataIandII
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