By Liz Highleyman

STARTMRK Trial

Raltegravir (Isentress)

Efavirenz (Sustiva)

The first integrase inhibitor, raltegravir (Isentress), was approved in October 2007 for use by treatment-experience patients with drug-resistant HIV.

In a late-breaker session at the 48th International Conference on Antimicrobial Agents and Chemotherapy (ICAAC 2008), taking place this week in Washington, DC, researchers presented data from a study of raltegravir in people starting therapy for the first time.

The STARTMRK trial included 563 treatment-naive patients randomly assigned (1:1) to start therapy with either 400 mg twice-daily raltegravir or 600 mg once-daily efavirenz (Sustiva), both in combination with tenofovir (Viread) plus emtricitabine (Emtriva), the 2 drugs in the fixed-dose Truvada pill.

Participants entered the study with a viral load of at least 5000 copies/mL and no documented resistance to efavirenz, tenofovir, or emtricitabine. About 80% were men, the mean age was about 38 years, about 40% were white, the mean baseline CD4 count was just under 220 cells/mm3, and mean viral loads were approximately 103,000 copies/mL in the raltegravir arm and 106,000 copies/mL in the efavirenz arm. About half had HIV RNA > 105 copies/mL (53%) and a CD4 count < 200 cells/mm3 (47%).

Results

• At week 48, raltegravir was found to be non-inferior to efavirenz.

• In a non-completer = failure analysis, 86% of patients taking raltegravir achieved HIV RNA < 50 copies/mL, compared with 82% of those taking efavirenz (P < 0.001).

• Time to virological response was significantly shorter in the raltegravir arm compared with the efavirenz arm (P < 0.001).

• 10% of raltegravir recipients and 14% of efavirenz recipients experienced virological failure.

• The mean CD4 cell increase from baseline was 189 cells/mm3 in the raltegravir arm versus 163 cells/mm3 in the efavirenz group (not a significant difference).

• 9% of raltegravir recipients and 12% of efavirenz recipients discontinued therapy before week 48.

• 44% of raltegravir recipients and 77% of efavirenz recipients experienced drug-related clinical adverse events (P < 0.001).

• Moderate-to-severe drug-related adverse events occurred half as often in the raltegravir group (16% vs 32%; P < 0.001).

• About 10% of patients in both groups experienced serious clinical adverse events:

• Malignancies (mostly Kaposi's sarcoma): 1 raltegravir recipient (0.4) and 9 efavirenz recipients (3.2%); 2 cases in the efavirenz group were considered drug-related.

• Deaths: 2 raltegravir recipients (0.4%) and 0 efavirenz recipients (0.0%).

• Patients in the raltegravir group were significantly less likely to report central nervous system (CNS) symptoms such as depression and abnormal dreams during the first 8 weeks of treatment (10% vs 18%; P < 0.001).

• At week 48, raltegravir recipients experienced significantly smaller increases from baseline in total cholesterol, low-density lipoprotein (LDL or "bad") cholesterol, and triglycerides (all P < 0.001).

• Modest increases in high-density lipoprotein (HDL or "good") cholesterol were observed in both groups, but were significantly larger in the efavirenz arm.

• Of the 12 patients who experienced virological failure while on raltegravir, 4 had integrase resistance mutations (2 with G120S + Q148H/R; 1 with Y143R; 1 with Y143H + L47M + E92Q + T97A), 5 had no detectable resistance mutations, and 3 could not be tested.

Based on these findings, the researchers concluded that in treatment-naive patients given 48 weeks of therapy, raltegravir/tenofovir/emtricitabine "had non-inferior antiretroviral activity" compared with efavirenz/tenofovir/emtricitabine and "was associated with greater increases in CD4 counts and fewer CNS symptoms."

Emory Univ., Atlanta, GA; Orlando Immunology Ctr., Orlando, FL; Univ. Vita-Salute San Raffaele, Milan, Italy; Univ. of California Davis, Sacramento, CA; Centro de Referencia d Treinamento DST/AIDS, Sao Paulo, Brazil; Merck Research Labs, North Wales, PA.

10/28/08

Reference
J Lennox, E Dejesus, A Lazzarin, and others. STARTMRK, A Phase III study of the safety & efficacy of raltegravir (RAL)-based vs efavirenz (EFV)-based combination therapy in treatment-naive HIV-infected patients. 48th International Conference on Antimicrobial Agents and Chemotherapy (ICAAC 2008). Washington, DC. October 25-28, 2008. Abstract H-896a.