A Pilot Study of Raltegravir Plus Combination Antiretroviral Therapy in Early Human Immunodeficiency Virus Infection: Challenges and Lessons Learned.

Ann C Collier,James I Mullins,Kenneth Tapia,Joanne D Stekler,Sarah E Holte,Robert W Coombs,Janine Maenza,Tae-Wook Chun,Claire E Stevens,Danielle Murray,J Shawn Justement,Ming Chang

doi:10.1089/biores.2015.0038

Abstract

Availability of integrase strand transfer inhibitors created interest in determining whether their use would decrease persistently infected cell numbers. This study hypothesized that adding raltegravir (RAL) to standard antiretroviral therapy (ART) would decrease human immunodeficiency virus (HIV)-infected CD4+ T cells more than standard combination ART. This was a pilot, randomized study comparing open-label standard triple ART to standard triple ART plus RAL over 96 weeks in ART-naive adults with early HIV infection. The primary objective was to compare quantity and trajectory of HIV DNA. Eighty-two persons were referred. A diverse set of reasons precluded the enrollment of all but 10. Those who enrolled and completed the study had an estimated median duration of HIV infection of 74 days at ART start. The groups had similar baseline characteristics. The RAL group had more rapid first phase plasma HIV RNA decay (0.67 log10 copies/mL/day) than with combination ART (0.34 log10copies/mL/day), p = 0.037. Second phase HIV RNA decay, residual viremia, cell-associated RNA, HIV DNA, CD4+ T-cells with replication-competent virus, and 2LTR circle levels did not differ between groups. Among those with entry plasma HIV RNA levels above the median, 2LTR circles were significantly lower over time than in those with lower entry HIV RNA levels (p = 0.02). Our results suggest homogeneity of responses in cell-associated RNA, HIV DNA, CD4+ T-cells with replication-competent virus, and 2LTR circles with early HIV in both ART groups. The kinetics of 2LTR DNA did not reflect the kinetics of plasma HIV RNA decline following ART initiation.

Highlights

Availability of the first integrase strand transfer inhibitor created interest in determining whether its use would decrease the number of cells persistently infected with human immunodeficiency virus (HIV) type one
Raltegravir (RAL, IsentressÒ) added to standard combination antiretroviral therapy (ART) in persons with chronic HIV decreased latently infected, resting CD4+ T cells and had favorable effects on ileal cell-associated unspliced HIV RNA in CD4+ T cells[1,2]; other studies showed no virologic impact of RAL intensification.[3,4,5,6]
When ART was started during early HIV, our results suggest homogeneity of responses in residual viremia, cell-associated RNA, HIV DNA, and CD4+ T cells with infectious virus

Summary

Introduction

Availability of the first integrase strand transfer inhibitor created interest in determining whether its use would decrease the number of cells persistently infected with human immunodeficiency virus (HIV) type one. Raltegravir (RAL, IsentressÒ) added to standard combination antiretroviral therapy (ART) in persons with chronic HIV decreased latently infected, resting CD4+ T cells and had favorable effects on ileal cell-associated unspliced HIV RNA in CD4+ T cells[1,2]; other studies showed no virologic impact of RAL intensification.[3,4,5,6] No difference in HIV RNA or DNA was seen in randomized studies of 5-drug RAL-containing ART versus three-drug ART in recent HIV infection.[7,8]. Persons who start ART earlier versus later have lower HIV DNA burden.[9,10,11] We performed a pilot study to a Ann C.

Methods

Results

Conclusion