Structured Treatment Interruptions with Tenofovir Monotherapy for Simian Immunodeficiency Virus-infected Newborn Macaques

Overview

Journal J Virol

Publisher American Society for Microbiology

Date 2006 Jun 16

PMID 16775328

Citations 11

Authors

Koen K A Van Rompay

Raman P Singh

Walid Heneine

Jeffrey A Johnson

David C Montefiori

Norbert Bischofberger

Marta L Marthas

Affiliations

Soon will be listed here.

Abstract

We demonstrated previously that prolonged tenofovir treatment of infant macaques, starting early during infection with virulent simian immunodeficiency virus (SIVmac251), can lead to persistently low or undetectable viremia even after the emergence of mutants with reduced in vitro susceptibility to tenofovir as a result of a K65R mutation in reverse transcriptase; this control of viremia was demonstrated to be mediated by the generation of effective antiviral immune responses. To determine whether structured treatment interruptions (STI) can induce similar immunologic control of viremia, eight newborn macaques were infected with highly virulent SIVmac251 and started on a tenofovir STI regimen 5 days later. Treatment was withdrawn permanently at 33 weeks of age. All animals receiving STI fared much better than 22 untreated SIVmac251-infected infant macaques. However, there was a high variability among animals in the viral RNA set point after complete drug withdrawal, and none of the animals was able to achieve long-term immunologic suppression of viremia to persistently low levels. Early immunologic and viral markers in blood (including the detection of the K65R mutation) were not predictive of the viral RNA set point after drug withdrawal. These results, which reflect the complex interactions between drug resistance mutations, viral virulence, and drug- and immune-mediated inhibition of virus replication, highlight the difficulties associated with trying to develop STI regimens with predictable efficacy for clinical practice.

Citing Articles

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

Van Rompay K, Hassounah S, Keele B, Lifson J, Ardeshir A, Watanabe J J Virol. 2018; 93(2).

PMID: 30381490 PMC: 6321921. DOI: 10.1128/JVI.01189-18.

Vazquez-Guillen J, Palacios-Saucedo G, Rivera-Morales L, Garcia-Campos J, Ortiz-Lopez R, Noguera-Julian M PLoS One. 2016; 11(1):e0147591.

PMID: 26807922 PMC: 4725846. DOI: 10.1371/journal.pone.0147591.

Prolonged tenofovir treatment of macaques infected with K65R reverse transcriptase mutants of SIV results in the development of antiviral immune responses that control virus replication after drug withdrawal.

Van Rompay K, Trott K, Jayashankar K, Geng Y, LaBranche C, Johnson J Retrovirology. 2012; 9:57.

PMID: 22805180 PMC: 3419085. DOI: 10.1186/1742-4690-9-57.

SIV-induced impairment of neurovascular repair: a potential role for VEGF.

Ebenezer G, McArthur J, Polydefkis M, Dorsey J, ODonnell R, Hauer P J Neurovirol. 2012; 18(3):222-30.

PMID: 22549763 PMC: 3804009. DOI: 10.1007/s13365-012-0102-5.

A drug evaluation of 1% tenofovir gel and tenofovir disoproxil fumarate tablets for the prevention of HIV infection.

Gengiah T, Baxter C, Mansoor L, Kharsany A, Abdool Karim S Expert Opin Investig Drugs. 2012; 21(5):695-715.

PMID: 22394224 PMC: 3460694. DOI: 10.1517/13543784.2012.667072.

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