By Liz Highleyman

As previously reported, VICTOR-E1 was a double-blind Phase 2b trial that included more than 100 highly treatment-experienced participants in 12 countries with exclusively CCR5-tropic HIV who had viral load > 1000 copies/mL despite stable antiretroviral therapy (ART).

Participants were randomly assigned to receive 20 mg or 30 mg once-daily vicriviroc or placebo, in combination with optimized background therapy (OBT) containing a ritonavir-boosted protease inhibitor (PI).

After 48 weeks, in an intent-to-treat analysis, 56% of patients in the 30 mg vicriviroc arm and 53% in the 20 mg arm achieved HIV RNA < 50 copies/mL, compared with 14% in the placebo arm. Patients with more active drugs in their OBT regimen were more likely to achieve undetectable HIV RNA. Rates of virological failure were 13% in the 30 mg vicriviroc arm, 8% in the 20 mg arm, and 38% in the placebo arm. Mean CD4 cell gains were 102, 134, and 65 cells/mm3, respectively. Rates of serious adverse events were 12%, 14%, and 22%, respectively, and treatment-related side effects occurred with similar frequency across arms.

Participants who completed the 48-week double-blind study were given the option to join an open-label extension phase in which everyone used 30 mg vicriviroc as part of an ART regimen including a boosted PI. OBT could also be re-optimized at this point. A total of 85 people -- all but 1 -- continued the study (32 from the original vicriviroc 30 mg arm, 35 from the 20 mg arm, and 18 from the placebo arm).

Among continuing patients, the mean age was about 45 years, about three-quarters were men, about 70% were Caucasian, and about 15% were black. About 70% were from study sites in Latin America or South Africa, with the rest from North America or Europe. The mean baseline viral load was about 2.5 log10 copies/mL (56% < 50 copies/mL) and the mean CD4 count was 366 cells/mm3 (81% > 200 cells/mm3). The mean duration on open-label vicriviroc therapy was 13 months.

Results

	The mean HIV RNA level fell by an additional 0.32 log10 copies/mL between week 48 and week 96, to 2.07 log10 copies/mL.
	The mean CD4 count increased by an additional 50 cells/mm3, to 422 cells/mm3.
	68% of patients reported at least 1 adverse event, mostly (93%) mild or moderate in severity.
	13% experienced treatment failure (the most common reason for discontinuation during the extension phase).
	2 patients with virological failure had vicriviroc-resistant virus during the double-blind phase, and 2 more developed resistance mutations during the extension phase.
	The only adverse events observed in at least 5% of participants were sinusitis (6%), cough (5%), and insomnia (5%).
	13% of adverse events were judged to be treatment-related.
	4 patients reported serious adverse events, and 2 discontinued therapy for this reason: 1 man discontinued after being simultaneously diagnosed with Hodgkin lymphoma and Kaposi's sarcoma, which the researchers judged were not treatment-related. 1 woman discontinued due to pregnancy, which ended 1 week later with a spontaneous abortion (miscarriage).
	There were no treatment-emergent deaths, seizures, or liver toxicity events.
	There were 2 cases of new-onset diabetes considered possibly related to the study drug.
	Only 1 patient with documented CCR5-tropic HIV at the start of the extension phase subsequently exhibited CXCR4-tropic or dual/mixed-tropic virus (discontinued due to treatment failure).

Schering-Plough Res. Inst., Kenilworth, NJ; Brazilmed Assistencia Medica e Pesquisa, Sao Paulo, Brazil; Federal Univ., Sao Paulo, Brazil; Centro de Referencia e Treinamento em DST/AIDS, Sao Paulo, Brazil; Orlando Immunology Ctr., Orlando, FL; Montefiore Med. Ctr., Bronx, NY; Einstein-Montefiore Ctr. for AIDS Res., Bronx, NY; St. Michael's Med. Ctr., Newark, NJ.

9/15/09

Reference

MC McCarthy, J Suleiman, R Diaz, and others.Vicriviroc Long-Term Safety and Efficacy: 96-Week Results from the VICTOR-E1 Study. 49th Interscience Conference on Antimicrobial Agents and Chemotherapy (ICAAC 2009). San Francisco. September 12-15, 2009. Abstract H-923.