HIV Infections Clinical Trial
Official title:
The Detection of Drug-Resistant HIV-1 in Taiwan
To assess the HIV resistance rate to variable antiretroviral agents in Taiwan, especially in patients with treatment failure, and to know the correlation between the drug resistance pattern and the HIV subtype, we will enroll a total of 150~200 HIV-1-infected subjects to perform genotypic resistance testing and try to establish facility of phenotypic resistance testing.
Drug-resistant HIV strains may develop during antiretroviral therapy, and transmission of
drug-resistant virus has been documented to be possible. The emergence of drug resistance in
HIV has been associated with suboptimal virologic response to antiretroviral therapy [1].
The likelihood that a patient will acquire drug-resistant virus is related to the prevalence
of drug resistance in the population with specific high-risk behaviors. In the western
countries, studies suggest that the prevalence of viral resistance to at least one
antiretroviral drug ranges from 6% to 16% in treatment-naïve patients, and among them, about
3% to 5% with reduced susceptibility to more than one class [2-4]. However, there is no data
addressing the prevalence of drug resistance in various populations in Taiwan currently.
Drug resistance can be measured using either genotypic or phenotypic resistance assays.
Genotypic assays detect mutations that cause dug resistance; phenotypic assays are drug
susceptibility assays that measuring the in vitro ability of the virus to grow in the
presence of serial dilutions of the inhibitors (that is, antiretroviral drugs). Because of
its more rapid turnaround time and less expensiveness, a genotypic assay is generally
preferred to phenotypic assay [5]. Genotypic resistance assay has been available in three
AIDS centers in Taiwan. However, the methods used for genotypic assay are different in the
three centers, and these data have not been gathered and analyzed to know the epidemiology
of HIV resistance in Taiwan, thus the interpretation and application of the results from
genotypic resistance assay for selection of antiretrovirals are quite questionable in
Taiwan.
Furthermore, though the genotypic assay is less straightforward, several conditions exist to
cause the discordance between genotype and phenotype, and the discordance may result in the
difficulty in phenotype prediction from genotype [6]. Thus, phenotypic assay may help
interpretation of resistance testing results and provide a guide to decide the optimal
regimen. With the availability of newer classes of antiretrovirals in the near future,
currently commercially available phenotypic testing using the recombinant viruses with
insertion of reverse transcriptase and protease gene sequences may not be enough. A new
phenotypic assay that can measure the virus ability to grow in the different concentrations
of NRTIs, NNRTIs, PIs, entry inhibitors, CCR5 inhibitors and integrase inhibitors will be
needed.
It has been known that HIV-1 load in plasma is strongly correlated with disease progression,
response to antiviral treatment, and transmission from mother to child. The plasma viral RNA
is more representative of the replicating virus pool at any time point than the
cell-associated proviral DNA. In order to study the relationship of the complete HIV-1
genome to phenotypic resistance, we choose to focus on plasma virions. However, for those
patients whose plasma viral load is not high enough to conduct this analysis, we will
instead of using patients' proviral DNA from infected PBMC for phenotypic resistance
analysis. Two strategies will be used to amplify viral genome. The first one will be
amplification of a nearly full-length viral genome. If this strategy does not work, the
second strategy will be to amplify two fragments of viral genome and to assemble these two
fragments by unique restriction enzymes.
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Observational Model: Cohort, Time Perspective: Cross-Sectional
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