Dolutegravir Monotherapy of Simian Immunodeficiency Virus-Infected Macaques Selects for Several Patterns of Resistance Mutations with Variable Virological Outcomes

Rompay, Koen K. A. Van; Hassounah, Said; Keele, Brandon F.; Lifson, Jeffrey D.; Ardeshir, Amir; Watanabe, Jennifer; Pham, Hanh Thi; Chertova, Elena; Sowder, Raymond C.; Balzarini, Jan; Mésplède, Thibault; Wainberg, Mark A.

doi:10.1128/jvi.01189-18

Cited by 12 publications

(14 citation statements)

References 49 publications

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“…In agreement with this hypothesis, all insertions reported to date also contained the small amino acid glycine (G), which could contribute to loop flexibility. Importantly, in our study, insertions could be found in circulating strains as well as proviruses, indicating that both replicative capacity and integration were conserved [5]. The replicative competence of retroviruses carrying integrase insertions is now confirmed by Le Hingrat et al's report of evolution from 2 to 5 amino acid insertions in 1 patient [1].…”

Section: Insertion As a Resistance Mechanism Against Integrase Inhibisupporting

confidence: 74%

“…The insertion consisted of 5 amino acids after position 232 in the integrase of SIVmac251, and could not be introduced in either SIVmac239 or HIV-1 without severely impairing fitness [4]. More recently, we also reported the frequent emergence of various 5 or 6 amino acid insertions in the SIVmac251 integrase in rhesus macaques treated with dolutegravir monotherapy [5]. Integrase insertions in this setting were heterogeneous in sequence, but all contained 2 positively charged amino acids, and all were found in the immediate vicinity of arginine (R) 231, a residue that was shown by cryogenic electron microscopy (cryo-EM) to be the only one outside of integrase catalytic domain to interact with host target DNA strongly [6].…”

Section: Insertion As a Resistance Mechanism Against Integrase Inhibimentioning

confidence: 99%

“…The G625R mutation identified by Das et al is yet neither a validated nor a candidate marker for artemisinin partial resistance [4]. In vitro resistance assessed by ring-stage survival assay (RSA) 0-3h is defined by persistence of a parasite survival rate >1% [2] (and not 10% as used in a previous version of the article and in another publication of this study [5].…”

Section: Lack Of Convincing Evidence Of Artemisinin Resistance In Indiamentioning

confidence: 99%

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Insertion as a Resistance Mechanism Against Integrase Inhibitors in Several Retroviruses

Pham

Hassounah

Keele

et al. 2019

Clinical Infectious Diseases

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Section: Insertion As a Resistance Mechanism Against Integrase Inhibisupporting

confidence: 74%

Section: Insertion As a Resistance Mechanism Against Integrase Inhibimentioning

confidence: 99%

Section: Lack Of Convincing Evidence Of Artemisinin Resistance In Indiamentioning

confidence: 99%

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Insertion as a Resistance Mechanism Against Integrase Inhibitors in Several Retroviruses

Pham

Hassounah

Keele

et al. 2019

Clinical Infectious Diseases

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“…However, to our knowledge, we present a unique instance of de novo selection of Env mutations that confer resistance to DTG in vitro. Ongoing studies should determine whether the Env mutations described here confer resistance to other classes of ARVs, and whether mutations in Env can contribute to escape from ARV therapy in infected individuals (86). The results of this work will provide fundamental insights into mechanisms of drug resistance and viral spread in vivo.…”

Section: Discussionmentioning

confidence: 88%

Mutations in the HIV-1 envelope glycoprotein can broadly rescue blocks at multiple steps in the virus replication cycle

Duyne

Kuo

Pham

et al. 2019

Proc. Natl. Acad. Sci. U.S.A.

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The p6 domain of HIV-1 Gag contains highly conserved peptide motifs that recruit host machinery to sites of virus assembly, thereby promoting particle release from the infected cell. We previously reported that mutations in the YPXnL motif of p6, which binds the host protein Alix, severely impair HIV-1 replication. Propagation of the p6–Alix binding site mutants in the Jurkat T cell line led to the emergence of viral revertants containing compensatory mutations not in Gag but in Vpu and the envelope (Env) glycoprotein subunits gp120 and gp41. The Env compensatory mutants replicate in Jurkat T cells and primary human peripheral blood mononuclear cells, despite exhibiting severe defects in cell-free particle infectivity and Env-mediated fusogenicity. Remarkably, the Env compensatory mutants can also rescue a replication-delayed integrase (IN) mutant, and exhibit reduced sensitivity to the IN inhibitor Dolutegravir (DTG), demonstrating that they confer a global replication advantage. In addition, confirming the ability of Env mutants to confer escape from DTG, we performed de novo selection for DTG resistance and observed resistance mutations in Env. These results identify amino acid substitutions in Env that confer broad escape from defects in virus replication imposed by either mutations in the HIV-1 genome or by an antiretroviral inhibitor. We attribute this phenotype to the ability of the Env mutants to mediate highly efficient cell-to-cell transmission, resulting in an increase in the multiplicity of infection. These findings have broad implications for our understanding of Env function and the evolution of HIV-1 drug resistance.

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“…These antiretroviral drugs were administered in a formulation of a 3-drug cocktail dissolved in the vehicle kleptose following previously published doses for each drug. Each milliliter of formulation contained the reverse transcriptase inhibitors PMPA (20 mg/mL) (50-52) and FTC (30 mg/mL) (53) and the integrase inhibitor DTG (2.5 mg/mL) (54,55).…”

Section: Methodsmentioning

confidence: 99%

Antiretroviral therapy does not reduce tuberculosis reactivation in a tuberculosis-HIV coinfection model

Ganatra¹,

Bucşan²,

Álvarez³

et al. 2020

Journal of Clinical Investigation

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While the advent of combination antiretroviral therapy (ART) has significantly improved survival, tuberculosis (TB) remains the leading cause of death in the HIV-infected population. We used Mycobacterium tuberculosis/simian immunodeficiency virus-coinfected (M. tuberculosis/SIV-coinfected) macaques to model M. tuberculosis/HIV coinfection and study the impact of ART on TB reactivation due to HIV infection. Although ART significantly reduced viral loads and increased CD4 + T cell counts in blood and bronchoalveolar lavage (BAL) samples, it did not reduce the relative risk of SIV-induced TB reactivation in ART-treated macaques in the early phase of treatment. CD4 + T cells were poorly restored specifically in the lung interstitium, despite their significant restoration in the alveolar compartment of the lung as well as in the periphery. IDO1 induction in myeloid cells in the inducible bronchus-associated lymphoid tissue (iBALT) likely contributed to dysregulated T cell homing and impaired lung immunity. Thus, although ART was indispensable for controlling viral replication, restoring CD4 + T cells, and preventing opportunistic infection, it appeared inadequate in reversing the clinical signs of TB reactivation during the relatively short duration of ART administered in this study. This finding warrants the modeling of concurrent treatment of TB and HIV to potentially reduce the risk of reactivation of TB due to HIV to inform treatment strategies in patients with M. tuberculosis/HIV coinfection.

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Dolutegravir Monotherapy of Simian Immunodeficiency Virus-Infected Macaques Selects for Several Patterns of Resistance Mutations with Variable Virological Outcomes

Cited by 12 publications

References 49 publications

Insertion as a Resistance Mechanism Against Integrase Inhibitors in Several Retroviruses

Insertion as a Resistance Mechanism Against Integrase Inhibitors in Several Retroviruses

Mutations in the HIV-1 envelope glycoprotein can broadly rescue blocks at multiple steps in the virus replication cycle

Antiretroviral therapy does not reduce tuberculosis reactivation in a tuberculosis-HIV coinfection model

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