Preliminary safety and efficacy data of brecanavir, a novel HIV-1 protease inhibitor: 24 week data from study HPR10006

doi:10.1093/jac/dkm122

JAC Advance Access originally published online on May 8, 2007
Journal of Antimicrobial Chemotherapy 2007 60(1):170-174; doi:10.1093/jac/dkm122

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© The Author 2007. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org

Preliminary safety and efficacy data of brecanavir, a novel HIV-1 protease inhibitor: 24 week data from study HPR10006

Jacob P. Lalezari¹^,*, Douglas J. Ward², Susan A. Tomkins³ and Harmony P. Garges⁴

¹ Quest Clinical Research, Department of Medicine, University of California at San Francisco, San Francisco, CA, USA ² Dupont Circle Physicians Group, Washington, DC, USA ³ GlaxoSmithKline, Greenford, UK ⁴ GlaxoSmithKline, Research Triangle Park, NC, USA

Received 4 December 2006; returned 2 February 2007; revised 6 April 2007; accepted 8 April 2007

^* Corresponding author. Tel: +1-415-353-0800; Fax: +1-415-353-0801; E-mail: drjay{at}questclinical.com

Background: Brecanavir, a novel protease inhibitor (PI), has sub-nM in vitroantiviral activity against multi-PI-resistant HIV-1 and in vitrois >100-fold more potent than previously marketed PIs andapprox. 10-fold more potent than the recently marketed PI, darunavir.

Methods: HPR10006 is an open label, single-arm, descriptive 48 week study,with 8 and 24 week interim analyses. Thirty-one HIV-1-infectedpatients were enrolled and received brecanavir/ritonavir 300mg/100 mg twice daily, with two nucleoside reverse transcriptaseinhibitors, based on history and genotype.

Results: At baseline, 25/31 had PI-sensitive virus and 6/31 had PI-resistantvirus (median of two primary PI and five secondary PI mutations).Median baseline HIV-1 RNA was 5.0 and 4.2 log₁₀ copies/mL, respectively.Four patients discontinued prior to Week 24. At Week 24, 77%(24/31) had HIV-1 RNA <50 copies/mL regardless of screeninggenotype, including 5/6 patients with PI-resistant virus (6/6had HIV-1 RNA <400 copies/mL). Brecanavir/ritonavir was welltolerated with no serious adverse events or clinically concerningchanges in laboratory parameters. Of 31 patients, 10 (32%) experienceddrug-related Grade 2–4 adverse events [most frequent eventswere fatigue (13%), dyspepsia (10%) and nausea (10%)]. Baselineisolate brecanavir IC₅₀ values for all patients ranged from0.1 to 0.2 nM. Median plasma trough concentration at Week 4was 150 ng/mL. Correcting the IC₅₀ (0.2 nM) value for proteinbinding (6-fold increase in vitro with 50% human serum) givesa corrected inhibitory quotient of 180.

Conclusions: Brecanavir/ritonavir was well tolerated and showed potent antiviralactivity in HIV-1-infected patients harbouring both PI-sensitiveand PI-resistant virus, following 24 weeks of dosing.

Keywords: antiretroviral therapy , acquired immune deficiency syndrome , AIDS , HIV-1 infection

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