Subtype-associated differences in HIV-1 reverse transcription affect the viral replication

Iordanskiy, Sergey; Waltke, Mackenzie; Feng, Yanjun; Wood, Charles

doi:10.1186/1742-4690-7-85

Cited by 29 publications

(29 citation statements)

References 73 publications

(94 reference statements)

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“…We observed a strong inhibitory effect of PPYaT on cultured T cells infected with HIV-1 subtype B, but less so with HIV subtype C. Previously, subtype C was shown to exhibit slower replication due to a different enzymatic activity of its reverse transcriptase (45). Thus, iron chelators may not be efficient against all HIV subtypes, and whether they have an effect on other HIV subtypes remains to be determined.…”

Section: Discussionmentioning

confidence: 66%

Phenyl-1-Pyridin-2yl-Ethanone-Based Iron Chelators Increase IκB-α Expression, Modulate CDK2 and CDK9 Activities, and Inhibit HIV-1 Transcription

Kumari

Iordanskiy

Kovalskyy

et al. 2014

Antimicrob Agents Chemother

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dHIV-1 transcription is activated by the Tat protein, which recruits CDK9/cyclin T1 to the HIV-1 promoter. CDK9 is phosphorylated by CDK2, which facilitates formation of the high-molecular-weight positive transcription elongation factor b (P-TEFb) complex. We previously showed that chelation of intracellular iron inhibits CDK2 and CDK9 activities and suppresses HIV-1 transcription, but the mechanism of the inhibition was not understood. In the present study, we tested a set of novel iron chelators for the ability to inhibit HIV-1 transcription and elucidated their mechanism of action. Novel phenyl-1-pyridin-2yl-ethanone (

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Section: Discussionmentioning

confidence: 66%

Phenyl-1-Pyridin-2yl-Ethanone-Based Iron Chelators Increase IκB-α Expression, Modulate CDK2 and CDK9 Activities, and Inhibit HIV-1 Transcription

Kumari

Iordanskiy

Kovalskyy

et al. 2014

Antimicrob Agents Chemother

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“…A recent study by Iordanskiy et al (18) found that differences in the replicative fitness of subtype B and C RTs is linked to the polymerase and the RNase H domain of RT. These findings cannot explain why some NNRTI resistance mutations are nonfunctional in the MJ4 background RT, since the RNase H and connective domains remained constant in all clones tested regardless of RT genotype.…”

Section: Discussionmentioning

confidence: 99%

Replicative Fitness Costs of Nonnucleoside Reverse Transcriptase Inhibitor Drug Resistance Mutations on HIV Subtype C

Armstrong

Lee

Essex

2011

Antimicrob Agents Chemother

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Single-dose nevirapine (NVP) is quite effective in preventing transmission of the human immunodeficiency virus (HIV) from mother to child; however, many women develop resistance to NVP in this setting. Comparing outcomes of clinical studies reveals an increased amount of resistance in subtype C relative to that in other subtypes. This study investigates how nonnucleoside reverse transcriptase inhibitor (NNRTI) drug resistance mutations of subtype C affect replication capacity. The 103N, 106A, 106M, 181C, 188C, 188L, and 190A drug resistance mutations were placed in a reverse transcriptase (RT) that matches the consensus subtype C sequence as well as the HXB2 RT, as a subtype B reference. The replicative fitness of each mutant was compared with that of the wild type in a head-to-head competition assay. The 106A mutant of subtype C would not grow in the competition assay, making it the weakest virus tested. The effect of the 106M mutation was weaker than those of the 181C and 188C mutations in the consensus C RT, but in subtype B, this difference was not seen. To see if the 106A mutation in a different subtype C background would have a different replicative profile, the same NNRTI resistance mutations were added to the MJ4 RT, a reference subtype C molecular clone. In the context of MJ4 RT, the 106A mutant was not the only mutant that showed poor replicative fitness; the 106M, 188C, and 190A mutants also failed to replicate. These results suggest that NNRTIs may be a cost-effective alternative for salvage therapy if deleterious mutations are present in a subtype C setting.The emergence of drug-resistant mutants is common among HIV-infected patients undergoing antiviral therapy. Clinically, the standard practice is to drop the antiviral to which the resistance has developed from the treatment regimen in such drug failure cases. However, a notable exception to this is the continuing use of lamivudine (3TC) as a salvage regimen because the 184V mutation linked to 3TC treatment has decreased replication ability relative to that of the wild type (WT) in subtype B (7). Mechanistically, Back et al. (2) found that the 184V mutant is less processive than wild-type RT under conditions of limiting deoxynucleoside triphosphates (dNTPs), and in primary lymphoid cells, the mutant is less fit than wildtype virus. These studies were extended further in vivo by Paredes et al. (35), who looked at multidrug-resistant virus from patients who were ending 3TC treatment. They used an allele-specific PCR assay to track the reversion of the M184V sequence and found that there was a fitness cost of 4 to 8% for the 184V mutation compared to that of the viral sequence that grew without 3TC drug pressure. Taken together, these studies illustrate how clinical management of HIV-infected patients can benefit from the study of the fitness cost of HIV drugresistant mutants.The use of antiretroviral drugs is increasing in the developing world. In particular, the use of single-dose nevirapine (NVP) has been shown to be an effective means of mitigat...

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“…Over half of the global HIV population is infected with subtype C, 4,29,30 which is dangerously uncontrolled in Africa and India. Subtypes A and B follow, then CRF_AG and CRF_AE, the latter predominantly found in Asia.…”

Section: Hawke Et Almentioning

confidence: 99%

HIV Non-B Subtype Distribution: Emerging Trends and Risk Factors for Imported and Local Infections Newly Diagnosed in South Australia

Hawke

Waddell

Gordon

et al. 2013

AIDS Research and Human Retroviruses

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(2000)(2001)(2002)(2003) to 64% (2007-2010) ( p = 0.007) and correspondingly the proportion of subtype B declined from 85% to 68% ( p = 0.002). Non-B infections were predominantly (83%) heterosexual contacts, mostly acquired overseas (74%). The majority (68%) of non-B patients were born outside of Australia. There was a nonsignificant increase from 1.6% to 4.2% in the proportion of locally transmitted non-B cases (p = 0.3). Three non-B subtypes and two circulating recombinant forms (CRFs) were identified: CRF_AE (n = 41), C (n = 36), CRF_AG (n = 13), A (n = 9), and D (n = 2). There has been a substantial increase over the past decade in diagnosed non-B infections, primarily through cases acquired overseas.

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Subtype-associated differences in HIV-1 reverse transcription affect the viral replication

Cited by 29 publications

References 73 publications

Phenyl-1-Pyridin-2yl-Ethanone-Based Iron Chelators Increase IκB-α Expression, Modulate CDK2 and CDK9 Activities, and Inhibit HIV-1 Transcription

Phenyl-1-Pyridin-2yl-Ethanone-Based Iron Chelators Increase IκB-α Expression, Modulate CDK2 and CDK9 Activities, and Inhibit HIV-1 Transcription

Replicative Fitness Costs of Nonnucleoside Reverse Transcriptase Inhibitor Drug Resistance Mutations on HIV Subtype C

HIV Non-B Subtype Distribution: Emerging Trends and Risk Factors for Imported and Local Infections Newly Diagnosed in South Australia

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