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Development and Evaluation of a Novel Relatively Low-Cost Method to Derive HIV-1 Integration Sites and Proviral Sequences
by
Mullins, James I.
, Hardy, Samantha R.
, McLaughlin, Sherry
, De Meyer, Tim
, Lambrechts, Laurens
, Vandekerckhove, Linos
, Struyve, Tine
, Cole, Basiel
, Termote, Liesbet
, Frenkel, Lisa M.
, Styrchak, Sheila
in
Antiretroviral therapy
/ DNA, Viral - genetics
/ Genomes
/ HIV
/ HIV Infections - drug therapy
/ HIV Infections - virology
/ HIV-1
/ HIV-1 - genetics
/ HIV-1 - physiology
/ Human immunodeficiency virus
/ Humans
/ Infections
/ Integration
/ integration site (IS)
/ multiple displacement amplification (MDA)
/ Nucleic Acid Amplification Techniques - economics
/ Nucleic Acid Amplification Techniques - methods
/ Polymerase chain reaction
/ provirus
/ Proviruses
/ Proviruses - genetics
/ REPLI-g MDA
/ Virus Integration
/ whole-genome amplification (WGA)
2026
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Development and Evaluation of a Novel Relatively Low-Cost Method to Derive HIV-1 Integration Sites and Proviral Sequences
by
Mullins, James I.
, Hardy, Samantha R.
, McLaughlin, Sherry
, De Meyer, Tim
, Lambrechts, Laurens
, Vandekerckhove, Linos
, Struyve, Tine
, Cole, Basiel
, Termote, Liesbet
, Frenkel, Lisa M.
, Styrchak, Sheila
in
Antiretroviral therapy
/ DNA, Viral - genetics
/ Genomes
/ HIV
/ HIV Infections - drug therapy
/ HIV Infections - virology
/ HIV-1
/ HIV-1 - genetics
/ HIV-1 - physiology
/ Human immunodeficiency virus
/ Humans
/ Infections
/ Integration
/ integration site (IS)
/ multiple displacement amplification (MDA)
/ Nucleic Acid Amplification Techniques - economics
/ Nucleic Acid Amplification Techniques - methods
/ Polymerase chain reaction
/ provirus
/ Proviruses
/ Proviruses - genetics
/ REPLI-g MDA
/ Virus Integration
/ whole-genome amplification (WGA)
2026
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Development and Evaluation of a Novel Relatively Low-Cost Method to Derive HIV-1 Integration Sites and Proviral Sequences
by
Mullins, James I.
, Hardy, Samantha R.
, McLaughlin, Sherry
, De Meyer, Tim
, Lambrechts, Laurens
, Vandekerckhove, Linos
, Struyve, Tine
, Cole, Basiel
, Termote, Liesbet
, Frenkel, Lisa M.
, Styrchak, Sheila
in
Antiretroviral therapy
/ DNA, Viral - genetics
/ Genomes
/ HIV
/ HIV Infections - drug therapy
/ HIV Infections - virology
/ HIV-1
/ HIV-1 - genetics
/ HIV-1 - physiology
/ Human immunodeficiency virus
/ Humans
/ Infections
/ Integration
/ integration site (IS)
/ multiple displacement amplification (MDA)
/ Nucleic Acid Amplification Techniques - economics
/ Nucleic Acid Amplification Techniques - methods
/ Polymerase chain reaction
/ provirus
/ Proviruses
/ Proviruses - genetics
/ REPLI-g MDA
/ Virus Integration
/ whole-genome amplification (WGA)
2026
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Development and Evaluation of a Novel Relatively Low-Cost Method to Derive HIV-1 Integration Sites and Proviral Sequences
Journal Article
Development and Evaluation of a Novel Relatively Low-Cost Method to Derive HIV-1 Integration Sites and Proviral Sequences
2026
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Overview
In people taking antiretroviral therapy (ART) for HIV infection, the methods to characterize latent and active HIV reservoirs remain costly and labor-intensive. Our objective was to develop a relatively low-cost technique to amplify and sequence the proviruses that persist during ART along with the site in the human genome where each provirus is integrated. We developed a novel HIV-specific Multiple Displacement Amplification (HIV-MDA) assay that specifically amplifies HIV-1 proviruses and their associated integration site. Upon comparison of our HIV-MDA to an established commercial kit designed to amplify cellular DNA, we found that the HIV-MDA (1) typically yielded a greater number of HIV integration site (HIV IS) sequences per 150,000 cells analyzed; (2) improved rates of proviral DNA amplification; and (3) amplified HIV IS at a fraction of the cost (13.6 times less expensive). Thus, the HIV-MDA method appears to be a more sensitive and cost-effective approach to sequencing HIV IS and the associated proviruses compared to a commercial kit.
Publisher
MDPI AG,Multidisciplinary Digital Publishing Institute (MDPI)
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