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      Quantitative evaluation of the antiretroviral efficacy of dolutegravir

      research-article
      1 , 1 , 2 ,
      JCI Insight
      American Society for Clinical Investigation

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          Abstract

          The second-generation HIV-1 integrase strand transfer inhibitor (InSTI) dolutegravir (DTG) has had a major impact on the treatment of HIV-1 infection. Here we describe important but previously undetermined pharmacodynamic parameters for DTG. We show that the dose-response curve slope, which indicates cooperativity and is a major determinant of antiviral activity, is higher for DTG than for first-generation InSTIs. This steepness does not reflect inhibition of multiple steps in the HIV-1 life cycle, as is the case for allosteric integrase inhibitors and HIV-1 protease inhibitors. We also show that degree of independence, a metric of interaction favorability between antiretroviral drugs, is high for DTG and nucleoside reverse transcriptase inhibitors. Finally, we demonstrate poor selective advantage for HIV-1 bearing InSTI resistance mutations. Selective advantage, which incorporates both the magnitude of resistance conferred by a mutation and its fitness cost, explains the high genetic barrier to DTG resistance. Together, these parameters provide an explanation for the remarkable clinical success of DTG.

          Abstract

          Quantification of the pharmacodynamic parameters describing the HIV integrase inhibitor dolutegravir helps to explain the remarkable clinical success of this antiretroviral drug.

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          Author and article information

          Contributors
          Journal
          JCI Insight
          JCI Insight
          JCI Insight
          JCI Insight
          American Society for Clinical Investigation
          2379-3708
          17 November 2016
          17 November 2016
          17 November 2016
          : 1
          : 19
          : e90033
          Affiliations
          [1 ]Department of Medicine, Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.
          [2 ]Howard Hughes Medical Institute, Baltimore, Maryland, USA.
          Author notes
          Address correspondence to: Robert F Siliciano, 733 North Broadway, MRB Room 879, Baltimore, Maryland 21205, USA. Phone: 410.955.2958; E-mail: rsiliciano@ 123456jhu.edu .
          Article
          PMC5111505 PMC5111505 5111505 90033
          10.1172/jci.insight.90033
          5111505
          27882352
          52ece67f-1fbc-42f8-a983-c4549777eeba
          Copyright © 2016, American Society for Clinical Investigation
          History
          : 8 August 2016
          : 18 October 2016
          Categories
          Research Article

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