Emergence of Protease Inhibitor Resistance–Associated Mutations in Plasma HIV-1 Precedes That in Proviruses of Peripheral Blood Mononuclear Cells by More Than a Year

Bi, Xiuqiong; Gatanaga, Hiroyuki; S, Ida; Tsuchiya, Kiyoto; Matsuoka-Aizawa, Saori; Kimura, Satoshi; Oka, Shinichi

doi:10.1097/00126334-200309010-00001

Cited by 41 publications

(41 citation statements)

References 21 publications

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“…Since all patients in this study initiated HAART very recently and about half of the 11 patients in whom drug resistance mutations were detected still had a viral load of less than 5,000 copies/ml at the time of sampling, they can be considered early treatment failures. Although the number of patients is limited, a correlation between low viral load and a reduced capacity for the detection of resistance mutations in DNA compared to that of resistance mutations in RNA was observed, further strengthening the hypothesis of a relationship between duration of treatment failure and the ability to detect drug resistance in DNA, as was suggested by Bi et al (6).…”

Section: Continued On Facing Pagesupporting

confidence: 64%

“…Some studies reported more mutations in the plasma RNA (6,10,21,24), and others reported more mutations in the cellular DNA (14,34). Most of these discordances may be attributed to differences in the selection of the samples used for the evaluation.…”

Section: Continued On Facing Pagementioning

confidence: 99%

“…Results of published reports in this regard are very inconsistent (6,10,14,21,24,34). The present study aims to investigate both the possibility of DNA sequencing from whole blood cells or from DBS and the usefulness of DNA sequencing for determination of drug resistance in patients from a resource-poor setting with a high level of HIV-1 subtype diversity.…”

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confidence: 99%

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Feasibility of Detecting Human Immunodeficiency Virus Type 1 Drug Resistance in DNA Extracted from Whole Blood or Dried Blood Spots

et al. 2007

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Due to high cost, availability of human immunodeficiency virus type 1 (HIV-1) drug resistance testing in resource-poor settings is still limited. We therefore evaluated the usefulness of viral DNA extracted from either whole blood or dried blood spots (DBS). Samples were collected from 50 patients receiving therapy and 10 therapy-naïve patients. Amplification and sequencing of RNA and DNA was performed using an in-house assay. Protease (PR) and reverse transcriptase (RT) sequences of plasma viral RNA were obtained for 96.6% and 89.7%, respectively, of the 29 patients with a detectable viral load. For cellular viral DNA, useful PR and RT sequences were obtained for 96.6% and 93.1% of the whole-blood-cell samples and for 93.1% and 93.1% of the DBS samples, respectively. For the 31 patients with an undetectable viral load, PR and RT sequences were obtained for 67.7% and 61.3% of the whole-blood-cell DNA preparations and for 54.8% and 58.1% of the DBS DNA preparations, respectively. A good correlation between RNA and DNA sequences was found; most discordances were caused by the detection of mixed amino acids. Of the RT drug-resistant mutations, 13 (38.2%) were seen in RNA only, 6 (17.6%) in DNA only, and 15 (44.1%) in both. Repeated amplification and sequencing of DNA extracts revealed a lack of reproducibility for the detection of drug resistance mutations in a number of samples, indicating a possible founder effect. In conclusion, this study shows the feasibility of genotypic drug resistance testing on whole blood cells or DBS and its possible usefulness for HIV-1 subtyping or examining the overall distribution of drug resistance in a population. For individual patients, RNA sequencing was shown to be superior to DNA sequencing, especially for patients who experienced early treatment failure. The use of DNA extracted from whole blood or DBS for the detection of archived drug resistance mutations deserves further study.Today, more than one million people in low-and middleincome countries have access to antiretroviral treatment (ART). Even though this is only 23% of the estimated 4.6 million human immunodeficiency virus type 1 (HIV-1)-infected individuals who are in need of highly active ART (HAART), it proves that the delivery of ART in resource-poor settings is feasible (41). Experiences from Europe and the United States, however, indicate that the emergence of HIV drug resistance remains an important obstacle to the long-term success of therapy. An adequate follow-up of patients on treatment, in order to identify cases in which therapy has failed, is essential to avoiding accumulation of drug resistance. Efforts to lower the prices for CD4 and viral load testing are being made, and alternative methods for measuring these parameters in resource-poor settings are being developed and evaluated (8,12,17). Unfortunately, genotypic resistance testing remains almost inaccessible due to its high cost, the need for specialized laboratories, and the logistical challenges, such as the requirements for a cold chain to transp...

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confidence: 64%

Section: Continued On Facing Pagementioning

confidence: 99%

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Feasibility of Detecting Human Immunodeficiency Virus Type 1 Drug Resistance in DNA Extracted from Whole Blood or Dried Blood Spots

et al. 2007

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“…Our observation that wild-type proviruses are maintained, despite the emergence of drug resistance mutations in plasma (1,17,34,37,42). In one study, emergence of the M184V mutation was compared in genomic viral RNA and viral DNA; however, there was no attempt to distinguish the emergence of the mutations in the different species of viral DNA (37).…”

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confidence: 99%

In Vivo Evidence for Instability of Episomal Human Immunodeficiency Virus Type 1 cDNA

Sharkey

Triques

Kuritzkes

et al. 2005

J Virol

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“…Since we wished to study all patients (regardless of treatment history), including those with PVL below detection limit, we chose to perform resistance testing by targeting HIV-1 DNA from the PBMC proviral compartment, instead of the most commonly used plasma HIV-1 RNA. Although studies have found that the detection of resistance mutations in the HIV-1 RNA plasma compartment may precede that in PBMC (Kaye et al 1995, Bi et al 2003, it has been shown that HIV DNA recovered from the proviral compartment can reliably be used in drug resistance genotyping (Devereux et al 2000, Sarmati et al 2003, Chew et al 2005, Parisi et al 2007, Vicenti et al 2007). In addition, proviral sequences can be useful to detect archived mutations that can compromise future therapeutic options, such as those selected by previously used regimens (Sarmati et al 2003, SG Parisi et al unpublished observations), and have been found to have greater sensitivity after treatment interruption in treatment experienced patients (Venturi et al 2002).…”

Section: Discussionmentioning

confidence: 99%

Prevalence of HIV type 1 drug resistance mutations in treatment-naïve and experienced patients from resource-limited settings with universal access to antiretroviral therapy: a survey in two small Brazilian cities

Eyer-Silva

Couto-Fernandez

Jesus

et al. 2008

Mem. Inst. Oswaldo Cruz

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Emergence of Protease Inhibitor Resistance–Associated Mutations in Plasma HIV-1 Precedes That in Proviruses of Peripheral Blood Mononuclear Cells by More Than a Year

Cited by 41 publications

References 21 publications

Feasibility of Detecting Human Immunodeficiency Virus Type 1 Drug Resistance in DNA Extracted from Whole Blood or Dried Blood Spots

Feasibility of Detecting Human Immunodeficiency Virus Type 1 Drug Resistance in DNA Extracted from Whole Blood or Dried Blood Spots

In Vivo Evidence for Instability of Episomal Human Immunodeficiency Virus Type 1 cDNA

Prevalence of HIV type 1 drug resistance mutations in treatment-naïve and experienced patients from resource-limited settings with universal access to antiretroviral therapy: a survey in two small Brazilian cities

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