Automated subtyping of HIV-1 genetic sequences for clinical and surveillance purposes : Performance evaluation of the new REGA version 3 and seven other tools

Background: To investigate differences in pathogenesis, diagnosis and resistance pathways between HIV-1 subtypes, an accurate subtyping tool for large datasets is needed. We aimed to evaluate the performance of automated subtyping tools to classify the different subtypes and circulating recombinant...

Full description

Autores:
Tipo de recurso:
Fecha de publicación:
2013
Institución:
Universidad del Rosario
Repositorio:
Repositorio EdocUR - U. Rosario
Idioma:
eng
OAI Identifier:
oai:repository.urosario.edu.co:10336/18729
Acceso en línea:
http://repository.urosario.edu.co/handle/10336/18729
Palabra clave:
Crf
Hiv-1
Phylogenetic Analysis
Sensitivity
Subtypes
Subtyping
Human Immunodeficiency Virus Proteinase
Rna Directed Dna Polymerase
Article
Automation
Cladistics
Computer Program
Controlled Study
Gene Sequence
Human Immunodeficiency Virus 1
Intermethod Comparison
Nonhuman
Phylogeny
Priority Journal
Reproducibility
Sensitivity And Specificity
Statistical Analysis
Structural Gene
Virus Genome
Virus Recombinant
Virus Typing
Human Immunodeficiency Virus 1
Circulating Recombinant Forms
Crf
Crfs
Hiv-1
Lanl
Los Alamos Dataset
Manual Phylogenetic Analysis
Mphy
Nts
Nucleotides
Phylogenetic Analysis
Pr
Protease
Rega Hiv Subtyping Tool Version 2
Rega Hiv Subtyping Tool Version 3
Regav2
Regav3
Reverse Transcriptase
Rt
Sensitivity
Subtypes
Subtyping
Unique Recombinant Forms
Urfs
Cluster Analysis
Computational Biology
Databases, Genetic
Hiv Infections
Hiv-1
Humans
Molecular Typing
Phylogeny
Public Health Surveillance
Reproducibility Of Results
Sensitivity And Specificity
VIH
Patogenicidad
Filogenia
Rights
License
Abierto (Texto Completo)
Description
Summary:Background: To investigate differences in pathogenesis, diagnosis and resistance pathways between HIV-1 subtypes, an accurate subtyping tool for large datasets is needed. We aimed to evaluate the performance of automated subtyping tools to classify the different subtypes and circulating recombinant forms using pol, the most sequenced region in clinical practice. We also present the upgraded version 3 of the Rega HIV subtyping tool (REGAv3). Methodology: HIV-1 pol sequences (PR. +. RT) for 4674 patients retrieved from the Portuguese HIV Drug Resistance Database, and 1872 pol sequences trimmed from full-length genomes retrieved from the Los Alamos database were classified with statistical-based tools such as COMET, jpHMM and STAR; similarity-based tools such as NCBI and Stanford; and phylogenetic-based tools such as REGA version 2 (REGAv2), REGAv3, and SCUEAL. The performance of these tools, for pol, and for PR and RT separately, was compared in terms of reproducibility, sensitivity and specificity with respect to the gold standard which was manual phylogenetic analysis of the pol region. Results: The sensitivity and specificity for subtypes B and C was more than 96% for seven tools, but was variable for other subtypes such as A, D, F and G. With regard to the most common circulating recombinant forms (CRFs), the sensitivity and specificity for CRF01_AE was ~99% with statistical-based tools, with phylogenetic-based tools and with Stanford, one of the similarity based tools. CRF02_AG was correctly identified for more than 96% by COMET, REGAv3, Stanford and STAR. All the tools reached a specificity of more than 97% for most of the subtypes and the two main CRFs (CRF01_AE and CRF02_AG). Other CRFs were identified only by COMET, REGAv2, REGAv3, and SCUEAL and with variable sensitivity. When analyzing sequences for PR and RT separately, the performance for PR was generally lower and variable between the tools. Similarity and statistical-based tools were 100% reproducible, but this was lower for phylogenetic-based tools such as REGA (~99%) and SCUEAL (~96%). Conclusions: REGAv3 had an improved performance for subtype B and CRF02_AG compared to REGAv2 and is now able to also identify all epidemiologically relevant CRFs. In general the best performing tools, in alphabetical order, were COMET, jpHMM, REGAv3, and SCUEAL when analyzing pure subtypes in the pol region, and COMET and REGAv3 when analyzing most of the CRFs. Based on this study, we recommend to confirm subtyping with 2 well performing tools, and be cautious with the interpretation of short sequences. © 2013 The Authors.

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