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An Update on New HIV Antiretroviral Agents Faculty: Edwin DeJesus, M.D., F.A.C.P. Medical Director of the Orlando Immunology Center in Orlando, Fla. Edwin DeJesus, M.D., F.A.C.P. This activity is supported by an educational grant from Copyright © 2008 Body Health Resources Corporation. All rights reserved. 1 Faculty For This Activity The Body PRO Edwin DeJesus, M.D., F.A.C.P. Dr. DeJesus is Medical Director of the Orlando Immunology Center in downtown Orlando, Fla., and the medical director of the HUG-Me Program's adult clinic at Orlando Regional Medical Center. Since 1993, Dr. DeJesus has devoted most of his time to caring for HIV- and hepatitis-infected patients. He is also deeply involved in HIV-related research: He is the principal investigator for the Orlando Immunology Center Research Facility, where he oversees several phase 1-4 clinical trials. In this capacity, he has presented study results at major international conferences, including the International AIDS Conference, International AIDS Society Conference, Interscience Conference on Antimicrobial Agents and Chemotherapy, Conference on Retroviruses and Opportunistic Infections and European AIDS Conference. Disclosures Dr. DeJesus has received grants and research support from Abbott Laboratories, Boehringer Ingelheim, Bristol-Myers Squibb Company, Gilead Sciences, GlaxoSmithKline, HoffmanLaRoche Inc., Merck & Co., Inc., Pfizer, Inc., Schering-Plough Corporation and Tibotec Therapeutics. He has been a consultant to Boehringer Ingelheim, Bristol-Myers Squibb, Gilead Sciences, GlaxoSmithKline, Merck, Tibotec and Vertex Pharmaceuticals, Inc., and he serves on speakers bureaus for Gilead, GlaxoSmithKline, Merck and Tibotec. An Update on New HIV Antiretroviral Agents 2 What Drives the Search for New Antiretroviral Agents? The Body PRO HIV Drug Resistance Safety and Tolerability Cost and Convenience • Five to 15% of newly diagnosed patients have drug resistance1-4 • Metabolic side effects: lipoatrophy, dyslipidemia, insulin resistance5 • A proportion of treatment-experienced patients have multiclass resistance4 • Other side effects: bone, hematologic, central nervous system, renal, reproductive and gastrointestinal • Treatment-experienced patients may need mega-HAART with as much as seven agents or more6 • Patients must take lifelong therapy7 1. Sabine Yerly et al. Lancet. August 28, 1999;354(9180):729. 2. Bluma Brenner et al, and the Quebec Primary Infection Study Team. Int J Antimicrob Agents. December 2000;16(4):429-434. 3. Daniel Boden et al. JAMA. September 22, 1999;282(12):1135-1141. 4. William Wheeler et al. CROI 2007; abstract 648. 5. Katherine Samaras. Diabetes Care. January 2007;30(1):113-119. 6. Julio Montaner et al. AIDS. January 5, 2001;15(1):61-69. 7. Strategies for Management of Antiretroviral Therapy (SMART) Study Group et al. N Engl J Med. November 30, 2006;355(22):2283-2296. An Update on New HIV Antiretroviral Agents 3 Goals of Therapy for TreatmentExperienced Patients The Body PRO IAS-USA Guidelines, August 20061: US DHHS Guidelines, January 29, 20082: “Trials with newer antiretroviral agents have shown that it is possible to achieve plasma HIV-1 RNA levels below 50 copies/mL even in highly treatment-experienced patients.” “The goal of treatment for patients with prior drug exposure and drug resistance is to reestablish maximal virologic suppression, HIV-1 RNA < 50 copies/mL.” 1. Scott M. Hammer et al. JAMA. 2006;296:827-843. 2. DHHS Guidelines for the Use of Antiretroviral Agents in HIV-1Infected Adults and Adolescents. January 29, 2008. Available at: http://www.aidsinfo.nih.gov/guidelines. Accessed June 11, 2008. An Update on New HIV Antiretroviral Agents 4 Timeline of Antiretroviral Development The Body PRO 1987 zidovudine 1999 amprenavir 1991 didanosine 2000 lopinavir/ritonavir 1992 zalcitabine 2001 tenofovir 1994 stavudine 2003 emtricitabine, atazanavir, enfuvirtide, fosamprenavir 1995 lamivudine, saquinavir 1996 2005 tipranavir nevirapine, ritonavir, indinavir 2006 darunavir 1997 delavirdine, nelfinavir 2007 raltegravir, maraviroc 1998 efavirenz, abacavir 2008 etravirine An Update on New HIV Antiretroviral Agents Key NRTI NNRTI PI Entry Inhibitor Integrase Inhibitor 5 The Body PRO Etravirine (TMC125): Next-Generation NNRTI An Update on New HIV Antiretroviral Agents 6 Need for Next-Generation NNRTIs The Body PRO Tolerability and toxicity CNS adverse effects, rash Hypersensitivity reactions (HSRs) Limits on prescribing to the target population Women of childbearing potential (i.e., efavirenz) Individuals with higher CD4+ cell counts (i.e., nevirapine) HIV drug Resistance Broad cross-resistance among first-generation NNRTIs Transmitted NNRTI resistance in up to 10% of treatmentnaive individuals* * Potential importance of minority variants that cannot be detected currently in clinical practice An Update on New HIV Antiretroviral Agents 7 Etravirine The Body PRO In vitro characteristics EC50 WT HIV-1: 1.4 nmol/L < 5-fold reduction in susceptibility against N N K103N, Y181C, Y188L, and L100I Phase I pharmacokinetics H3C Elimination half-life: 30-40 hours Steady state attained within 5 days Metabolized by cytochrome P450 CYP3A O N Br NH2 Phase IIa CH3 N NH 2.0 log10 decline in plasma HIV-1 RNA over 7 days Adapted from Marie-Pierre de Bethune et al. ICAAC 2000; abstract 1841. Adapted from Stephen Piscitelli et al. Pharmacology Workshop 2002; abstract 5.3. Adapted from Boris Gruzdev et al. AIDS. 2003;17:2487-2494. An Update on New HIV Antiretroviral Agents 8 Etravirine: Proof-of-Principle Trial in Treatment-Experienced Patients The Body PRO HIV-1 RNA (Log10 Copies/mL) Failing NNRTI therapy Etravirine* New Tx 4.5 N = 16 Patients 4.0 0.86 log10 3.5 3.0 -10 -8 -6 -4 -2 0 2 Time (Days) 4 6 8 *Etravirine 900 mg BID + continued NRTIs for seven days Adapted from Brian Gazzard et al. AIDS. 2003;17:F49-F54. An Update on New HIV Antiretroviral Agents 9 The Body PRO DUET: Study Design and Major Inclusion Criteria Screening 6 weeks 48-week treatment period with optional 48-week extension Follow up 4 weeks 24-week primary analysis† Etravirine (TMC125) (200 mg BID) + BR* 600 patients target per trial Placebo + BR* BR* = darunavir/ritonavir (600/100 mg/mL) with optimised NRTIs and optional enfuvirtide • DUET-1 and -2 differed only in geographical location; pooled analysis was pre-specified • Plasma viral load > 5,000 HIV-1 RNA copies/mL and stable therapy for ≥ 8 weeks • ≥ 1 NNRTI RAM*, at screening or in documented historical genotype • ≥ 3 primary PI mutations at screening • Patients recruited from Thailand, Australia, Europe and the Americas * BR = background regimen; RAM = resistance-associated mutation † Primary endpoint HIV-1 RNA < 50 copies/mL (TLOVR) Adapted from Pedro Cahn et al. ICAAC 2007; abstract H-717. An Update on New HIV Antiretroviral Agents 10 DUET: Patients with Viral Load < 50 Copies/mL at Week 48 (ITT-TLOVR) The Body PRO * Pooled DUET data included for comparison; ‡ Logistic regression model; TLOVR = time to loss of virologic response imputation algorithm. CI = confidence interval Richard Haubrich et al. CROI 2008; abstract 790. Reprinted with permission. An Update on New HIV Antiretroviral Agents 11 DUET: Response (<50 Copies/mL) by PSS (DRV FC < 10 and < 40)* at Week 48 The Body PRO <10 FC < 40 FC *PSS = phenotypic sensitivity score; DRV = darunavir; FC = fold change; ETR = etravirine; BR = background regimen; ARVs = antiretrovirals; VL = viral load ‡Analysis excludes pts who DC except for virologic failure; ENF counted as sensitive if used de novo Richard Haubrich et al. CROI 2008; abstract 790. Reprinted with permission. An Update on New HIV Antiretroviral Agents 12 The Body PRO DUET: Overview of Adverse Events (Regardless of Causality) at Week 48 • No consistent or clinically relevant trends in lab, vital signs or ECGs observed • Lab abnormalities, including hepatic and lipid parameters similar between arms ‡ All deaths in the ETR group were considered not or doubtfully related to trial medication. One death in the pooled placebo group was considered possibly related to the background regimen (BR); AE = adverse event; ETR = etravirine Richard Haubrich et al. CROI 2008; abstract 790. Reprinted with permission. An Update on New HIV Antiretroviral Agents 13 DUET: Response (< 50 Copies/mL) According to Number of TMC125 RAMS The Body PRO Number of TMC125 RAMs Present at Baseline TMC125 + BR (n=406) 0 121/161 64/147 1 73/121 59/157 2 37/64 17/68 3 13/32 6/24 7/28 3/18 ≥4 0 Placebo + BR (n=414) 75% 44% 60% 38% 58% 25% 41% 25% 25% 17% 20 40 60 Patients with Viral Load < 50 Copies/mL at Week 24 (%) 80 • The greatest added benefit in the TMC125 versus placebo group was seen in patients with <3 TMC125 RAMs • 86% of patients had <3 TMC125 RAMs Analysis excludes patients who used de-novo enfuvirtide or discontinued except for virological failure BR = background regimen; RAM = resistance-associated mutation Pedro Cahn et al. ICAAC 2007; abstract H-717. Reprinted with permission. An Update on New HIV Antiretroviral Agents 14 Etravirine The Body PRO Recommended dose of etravirine is 200mg BID with a meal It can be dispersed in a glass of water Substrate CYP3A4, CYP2C9, CYP2C19 Rash: main AE in clinical studies Grade 2 - 4 (9%), discontinuation from study (2%), Stevens-Johnson Syndrome (<.1%) Mutations V179F/I and Y181C/I most commonly selected on virologic failure Fold change (FC) susceptibility: < 3 FC (Monogram); < 1.6 to > 27.6 (Virco) Populations: Pregnancy Category B No renal dose adjustment needed OK for mild to moderate liver disease An Update on New HIV Antiretroviral Agents 15 ARV Drug-Drug Interactions: Etravirine The Body PRO No dose adjustment required Didanosine Tenofovir Saquinavir/r Lopinavir + Saquinavir2 Darunavir/r Raltegravir Elvitegravir/r3 a AUC Co-administer with caution1 Lopinavir/ra Dose modification1 Maraviroc4 (modify dose) Co-administered contraindicated with1 of ETR after co-administration with LPV/r is anticipated to be ~85% higher than AUC of ETR observed in DUET trials.1 b AUC of ETR after co-administration with ATV/r is anticipated to be ~100% higher than AUC of etravirine observed in DUET trials.1 c Due to a significant increase in AUC of APV, the appropriate doses of the combination of ETR and FPV/r have not been established.1 1 Intelence Tipranavir/r Atazanavir/rb Fosamprenavir/rc Full dose ritonavir Unboosted PIs Atazanavir Fosamprenavir Indinavir Nelfinavir Delavirdine Nevirapine Efavirenz [package insert]. Raritan, NJ: Tibotec, Inc.; January 2008. 2 Marianne Harris et al. CROI 2006; abstract 575b. 3Srinivasan Ramanathan et al. ICAAC 2007; abstract H-1049. 4 J. Davis et al. EACS 2007. Abstract P4.3/02. An Update on New HIV Antiretroviral Agents 16 The Body PRO Protease Inhibitors An Update on New HIV Antiretroviral Agents 17 Similar Efficacy of Protease Inhibitors in Treatment-Naïve Patients at 48 Weeks The Body PRO Percent With HIV-1 RNA < 50 Copies/mL ARTEMIS (ITT: TLOVR)1 Intent to Treat: Time to Loss of Virologic Response Darunavir/ritonavir (800/100) mg QD (N = 343) 84 Lopinavir/ritonavir (400/100) mg BID or (800/200) mg QD + tenofovir/emtricitabine* (N = 346) 78 CASTLE (ITT-CVR: NC = F)2 78 Lopinavir/ritonavir soft-gel capsule (400/100 mg) BID + tenofovir/emtricitabine (N = 443) 76 1.7 (95% CI:-3.8, 7.1) Intent to Treat Lopinavir/ritonavir soft-gel capsule (400/100 mg) BID + tenofovir/emtricitabine (N = 170) 65 Saquinavir/ritonavir (1000/100 mg) BID + tenofovir/emtricitabine (N = 167) 64 KLEAN (ITT-E: TLOVR)4 5.5 (95% CI:-0.3, 11.2) Intent to Treat-Confirmed Virologic Response: Non-completer = Failure Atazanavir/ritonavir (300/100 mg) QD + tenofovir/emtricitabine (N = 440) GEMINI (ITT)3 Approximated Difference, % 1.14 (96% CI:-9.6, 11.9) Intent to Treat-Exposed: Time to Loss of Virologic Response Fosamprenavir/ritonavir (700/100 mg) BID + abacavir/lamivudine (N = 434) 66 Lopinavir/ritonavir soft-gel capsule (400/100 mg) BID + abacavir/lamivudine (N = 444) 65 n/a *77% of patients received BID dosing throughout study, 83% of patients switched from soft-gel capsule to tablet formulation. 1Adapted 3Adapted from Nathan Clumeck et al. CROI 2008; abstract 37. 2Adapted from Jean-Michel Molina et al. CROI 2008; abstract 37. from Sharon Walmsley et al. EACS 2007; abstract PS1/4. 4Adapted from Joseph Eron Jr et al. Lancet. 2006;368:476-482. An Update on New HIV Antiretroviral Agents 18 The Evolution of Darunavir/r in the Treatment of HIV Infection The Body PRO Patients With Heavy ARV Experience POWER 1 and POWER 2 POWER 3 DUET 1 and DUET 2 Patients With Limited ARV Experience TITAN Patients Naïve to Therapy ARTEMIS An Update on New HIV Antiretroviral Agents 19 TITAN (TMC114-C214): Study Design The Body PRO Jose Valdez Madruga et al. IAS 2007; abstract TUAB101. Reprinted with permission. An Update on New HIV Antiretroviral Agents 20 TITAN: Baseline Characteristics The Body PRO Jose Valdez Madruga et al. IAS 2007; abstract TUAB101. Reprinted with permission. An Update on New HIV Antiretroviral Agents 21 TITAN: Viral Load < 50 Copies/mL to Week 48 (TLOVR) — All Patients The Body PRO Jose Valdez Madruga et al. IAS 2007; abstract TUAB101. Reprinted with permission. An Update on New HIV Antiretroviral Agents 22 TITAN: Viral Load < 50 Copies/mL at Week 48 by Baseline LPV FC (TLOVR) The Body PRO * DRV/r 600/100mg bid † Estimated from a logistic regression model including treatment and stratification factors: baseline log 10 HIV-RNA and use of NNRTIs in the optimised background regimen Jose Valdez Madruga et al. IAS 2007; abstract TUAB101. Reprinted with permission. An Update on New HIV Antiretroviral Agents 23 TITAN: Most Common Adverse Events The Body PRO Jose Valdez Madruga et al. IAS 2007; abstract TUAB101. Reprinted with permission. An Update on New HIV Antiretroviral Agents 24 ARTEMIS: Phase III Study Design The Body PRO 689 ARV-naïve patients VL > 5,000; no CD4 entry DRV/r 800/100mg QD + TDF 300mg and FTC 200mg (N=343) LPV/r 400/100mg bid or 800/200mg QD + TDF 300mg and FTC 200mg (N=346) LPV dosing LPV formulation QD = 15% Capsule only = BID = 77% Tablet only = BID/QD = 7% 15% 2% Capsule/tablet switch = 83% Dosing was based on regulatory approval; switch was made according to local regulatory approval and drug availability Edwin DeJesus et al. ICAAC 2007; abstract H-718b. Reprinted with permission. An Update on New HIV Antiretroviral Agents 25 ARTEMIS: Viral Load < 50 Copies/mL to Week 48 (ITT-TLOVR) Patients with VL < 50 Copies/mL (% [±SE]) The Body PRO 100 DRV/r QD (N=343) 90 LPV/r QD or BID (N=346) 80 84% 78% 70 60 50 40 Estimated difference in response vs LPV/r for non-inferiority: PP = 5.6% (95% CI –0.1;11.3) p<0.001 Estimated difference in response vs LPV/r for superiority: ITT = 5.5% (95% CI –0.3;11.2) p=0.062 30 20 10 0 2 4 8 12 16 24 Time (weeks) 36 Edwin DeJesus et al. ICAAC 2007; abstract H-718b. Reprinted with permission. An Update on New HIV Antiretroviral Agents 48 26 ARTEMIS: Week 48 Response by QD and BID Dosing (ITT-TLOVR) The Body PRO Difference 3% (95% CI -3; 9) Difference 13% (95% CI 1; 24; p<0.05) Patients with VL < 50 Copies/mL (%) 100 Difference 9%* (95% CI -3; 21) 80 84 81 78 71 60 *Difference rounded †27 patients receiving LPV/r BID and QD during the study were excluded from this analysis. 40 20 0 N= LPV/r overall LPV/r BID† LPV/r QD† DRV/r QD 346 267 52 343 Adapted from Edwin DeJesus et al. ICAAC 2007; abstract H-718b. An Update on New HIV Antiretroviral Agents 27 ARTEMIS: Grade 2–4 Adverse Events The Body PRO DRV/r QD LPV/r QD or BID (N=343) (N=346) GI (all AEs) 23 (7) 47 (14) p < 0.01 Diarrhea 14 (4) 34 (10) p < 0.05 Nausea 6 (2) 10 (3) 9 (3) 4 (1) Gr 2–4 AEs† ≥ 2% Incidence, n (%) Rash (all types) †At least possibly related to study drug, excluding laboratory-related events • No renal SAEs and no treatment discontinuations due to renal AEs Edwin DeJesus et al. ICAAC 2007; abstract H-718b. Reprinted with permission. An Update on New HIV Antiretroviral Agents 28 ARTEMIS: Mean Fasting Lipid Levels Over Time The Body PRO mM ng/mL 250 3.5 Mean Triglycerides DRV/r QD (n=343) LPV/r QD or BID (n=346) 2.9 2.3 200 NCEP cut-off 1.7 150 1.1 100 2 4 8 12 16 24 36 Time (weeks) DRV/r n=343 LPV/r n= 346 320 313 Total Cholesterol/HDL Ratio Mean Total Cholesterol/HDL Ratio (± SE) Mean Triglyceride Concentration ( ± SE) 300 5.5 DRV/r QD (n=343) LPV/r QD or bid (n=346) 5.0 4.5 4.0 3.5 3.0 2 4 8 12 16 48 306 301 343 346 Edwin DeJesus et al. ICAAC 2007; abstract H-718b. Reprinted with permission. An Update on New HIV Antiretroviral Agents 24 320 313 36 48 305 301 29 The Body PRO Raltegravir: Integrase Inhibitor An Update on New HIV Antiretroviral Agents 30 BENCHMRK-1 & -2: Study Design The Body PRO • Randomized, double-blind, placebo-controlled with Data and Safety Monitoring Board • Primary analysis at Week 16; secondary analysis at Week 48 Primary endpoints Week 16 HIV-1-infected Triple-class resistant HIV-1 RNA > 1,000 copies/mL No CD4 cell cut-off Protocol 018* (N=352) Europe, Asia/Pacific and Peru Protocol 019* (N=351) North and South America Planned duration Week 156 Raltegravir 400 mg BID + OBT P018* (n=232) P019* (n=230) 2:1 Placebo + OBT P018* (n=118) P019* (n=119) • OBT was selected by investigator based on baseline resistance testing and prior treatment history. Selected investigational ARTs, darunavir and tipranavir, were permitted. *Protocol 018 (P018) is BENCHMRK-1; Protocol 019 (P019) is BENCHMRK-2 David Cooper et al. CROI 2008; abstract 788. Reprinted with permission. Copyright © 2008 Merck & Co., Inc., Whitehouse Stations, New Jersey, USA, All Rights Reserved An Update on New HIV Antiretroviral Agents 31 BENCHMRK-1 & -2: Patients With HIV-1 RNA < 50 Copies/mL at Week 48 The Body PRO BENCHMRK-1[1] BENCHMRK-2[2] *+OBR; P < .001 for RAL vs placebo, derived from a logistic regression model adjusted for baseline HIV-1 RNA level (log10), first ENF use in OBR, first DRV use in OBR, active PI in OBR. 1David Cooper et al. CROI 2008; abstract 788. Reprinted with permission. Steigbigel et al. CROI 2008; abstract 789. Reprinted with permission. Copyright © 2008 Merck & Co., Inc., Whitehouse Stations, New Jersey, USA, All Rights Reserved 2Roy An Update on New HIV Antiretroviral Agents The Body PRO BENCHMRK-1 & -2 Combined Efficacy: Percent of Patients With HIV RNA <50 Copies/mL at Week 48 by Selected ARTs in OBT David Cooper et al. CROI 2008; abstract 788. Reprinted with permission. Copyright © 2008 Merck & Co., Inc., Whitehouse Stations, New Jersey, USA, All Rights Reserved An Update on New HIV Antiretroviral Agents 32 33 BENCHMRK-1 and -2: Drug-Related Adverse Events at Week 48 The Body PRO BENCHMRK-11 BENCHMRK-22 Placebo + OBT (N = 118) RAL + OBT (N = 232) Placebo + OBT (N = 119) RAL + OBT (N = 230) Diarrhea 14.4% 6.9% 10.1% 13.9% Fatigue 0% 2.2% 2.5% 5.2% Headache 6.8% 3.0% 5.0% 8.7% Nausea 6.8% 3.9% 9.2% 9.6% Rates of all-cause, serious and drug-related AEs, death and laboratory abnormalities did not differ significantly between treatment arms. Malignancy rate: RAL 3.5/100 person-years vs. placebo 2.3/100 person-years RR: 1.5 (95% CI: 0.5-6.3) 1Adapted from David Cooper et al. CROI 2008; abstract 788. from Roy Steigbigel et al. CROI 2008; abstract 789. Copyright © 2008 Merck & Co., Inc., Whitehouse Stations, New Jersey, USA, All Rights Reserved 2Adapted An Update on New HIV Antiretroviral Agents 34 Study Design: MK-0518 Protocol 004 The Body PRO 48 Week Phase II Multicenter Double-Blind, Randomized Study 198 patients treated Mean age 36, 80% male, 69% non-white, 34% AIDS, Mean HIV RNA at baseline 4.6-4.8 log10 MK-518 2 weeks monotherapy EFV (TDF + 3TC) MK-518 (100, 200, 300, 400 BID) (TDF + 3TC) *Virologic failure defined as early (rebound or lack of suppression by 1 log10) or late (failure to suppress to <200 c/mL or rebound) Adapted from Martin Markowitz et al. IAC 2006; abstract THLB0214. An Update on New HIV Antiretroviral Agents 35 Protocol 004: Percent (95% CI) of Patients with HIV RNA < 50 Copies/mL (NC=F) Percent of Patients with HIV RNA < 50 Copies/mL The Body PRO 100 80 60 * 40 * 20 0 0 MK-0518 100mg MK-0518 200mg MK-0518 400mg MK-0518 600mg Efavirenz 2 4 8 12 Week 16 24 39 40 41 40 38 39 40 41 40 38 39 40 41 40 38 39 40 41 40 38 39 40 41 40 38 39 40 41 40 37 * P < 0.001 for MK-0518 at each dose vs. EFV Martin Markowitz et al. IAC 2006; abstract THLB0214. Reprinted with permission. An Update on New HIV Antiretroviral Agents 36 MK-0518 vs. EFV: Adverse Events The Body PRO MK-0518 (all doses) N=160 (%) Efavirenz* N=38 (%) Nausea 11 13 Headache 9 24 Dizziness 8 26 Diarrhea 7 11 Insomnia 7 11 Abnormal dreams 6 18 Flatulence 6 - Additional adverse events seen at ≥ 5% in efavirenz group: Nightmare (11%) Vomiting (8%) Malaise (8%) Fatigue (5%) Disturbance in attention (5%) Lethargy (5%) Anxiety (5%) Adapted from Martin Markowitz et al. IAC 2006; abstract THLB0214. An Update on New HIV Antiretroviral Agents * With TFV/3TC 37 Raltegravir vs. EFV: Serum Lipids The Body PRO N = number of patients with data * p-value < 0.05 for comparison to efavirenz ** MK-0518 and EFV were given in combination with TFV/3TC Hedy Teppler et al. ICAAC 2006; abstract H-0256a. Reprinted with permission. An Update on New HIV Antiretroviral Agents 38 The Body PRO Maraviroc: CCR5 Entry Inhibitor An Update on New HIV Antiretroviral Agents 39 CCR5 Inhibitors: The Good, The Bad, The Unknown The Body PRO Dual tropic X4 (SI) CD4 CCR5 CXCR4 T-cell lines R5 (NSI) Primary lymphocytes CD4 Naïve Monocyte/macrophages CD4 memory Dan Kuritzkes. Infectious Disease Grand Rounds Feb. 2008, University of Colorado. Reprinted with permission. An Update on New HIV Antiretroviral Agents 40 Tropism Testing The Body PRO Panel on Antiretroviral Guidelines for Adults and Adolescents. Washington, DC: US Dept of Health and Human Services; December 1, 2007. An Update on New HIV Antiretroviral Agents 41 Tropism Testing The Body PRO Standard Trofile Assay Enhanced Trofile Assay The Trofile test, which was used to establish eligibility for clinical trials of maraviroc, has been proven an effective test for identifying individuals with X4-tropic virus.1 It identified D/M tropism in more patients in ACTG 5211 than the standard assay:2 However, the test sometimes fails to identify X-4 tropic minority subpopulations. 25 of the 116 patients who were believed to have changed from CCR5-only to D/M tropism while taking vicriviroc, were found to have D/M virus at study entry when the enhanced Trofile assay was used. 1. Jeannette M. Whitcomb et al. Antimicrob Agents Chemother. February 2007;51(2):566-475. 2. Jacqueline Reeves et al. CROI 2008; abstract 869. An Update on New HIV Antiretroviral Agents 42 MOTIVATE-1 & -2: Study Design The Body PRO OBT* + Placebo Randomization 1:2:2 MOTIVATE 1 N=601 MOTIVATE 2 N=474 OBT* + Maraviroc (150 mg† QD) OBT* + Maraviroc (150 mg† BID) Screening (6 weeks) 0 Patient eligibility criteria: • R5 HIV-1 infection • HIV-1 RNA ≥ 5,000 copies/mL • Stable pre-study ARV regimen, or no ARVs for ≥ 4 weeks • Resistance to and/or ≥ 6 months’ experience with ≥ one ARV from three classes (≥ two for PIs) Patients stratified by: • Enfuvirtide use in OBT • HIV-1 RNA < and ≥ 100,000 copies/mL at screening 24w 48w Planned interim analysis * OBT = optimized background therapy of 3–6 ARVs (PK boosting doses of RTV not counted as an ARV) † Patients receiving a PI (except TPV) and/or delavirdine in their OBT received 150 mg dose of MVC, all other patients received 300 mg dose of MVC Elna van der Ryst et al. ICAAC 2007; abstract H-715. Reprinted with permission. An Update on New HIV Antiretroviral Agents 43 MOTIVATE 1 & 2: Combined Virologic Efficacy at Week 48 The Body PRO Percentage of Patients with HIV-1 RNA Suppression (solid lines, HIV-1 RNA <400 copies/mL; dashed lines, HIV-1 RNA <50 copies/mL) David Hardy et al. CROI 2008; abstract 792. Reprinted with permission. An Update on New HIV Antiretroviral Agents 44 80 58 60 Patients (% ) The Body PRO MOTIVATE-1 & -2: HIV-1 RNA < 50 Copies/mL at Week 24 by Number of Active Drugs in OBT MVC BID + OBT MVC QD + OBT Placebo + OBT 61 55 53 52 43 43 40 29 19 18 20 9 3 0 3 or More N= 121 132 64 2 1 0 104 88 59 134 130 44 56 51 35 Number of Active Drugs in OBT Adapted from Mark Nelson et al. CROI 2007; abstract 104aLB. Adapted from Jacob Lalezari et al. CROI 2007; abstract 104bLB. An Update on New HIV Antiretroviral Agents 45 MOTIVATE 1 & 2: Virologic Outcomes Based on Tropism The Body PRO HIV-1 RNA <50 c/mL OBT alone MVC BID + OBT MVC QD + OBT 100 90 80 Patients (%) 70 Tropism result at baseline: D/M R5 60 50 50 50 40 27 30 20 18 26 18 10 0 N= 17 33 33 187 362 377 Elna van der Ryst et al. ICAAC 2007; abstract H-715. Reprinted with permission. An Update on New HIV Antiretroviral Agents 46 MOTIVATE 1 & 2: 48-Week Safety Unadjusted for Duration of Exposure The Body PRO All casualties and severities, n (%) Placebo + OBT N=209 Maraviroc QD + OBT N=414 Maraviroc BID + OBT N=426 Total exposure to study treatment, patient-years 111 300 309 Treatment-emergent adverse events 177 (84.7) 375 (90.6) 393 (92.3) Discontinuation due to adverse events 11 (5.3) 24 (5.8) 21 (4.9) Serious adverse events 35 (16.7) 62 (14.9) 72 (16.9) Grade 3 adverse events 46 (22.0) 84 (20.3) 104 (24.4) Grade 4 adverse events 16 (7.7) 37 (8.9) 45 (10.6) Category C events 16 (7.7) 29 (7.0) 23 (5.4) Category C malignancies 5 (2.4) 3 (0.7) 4 (0.9) Non-HIV malignancies 11 (5.3) 12 (2.9) 19 (4.5) Deaths* 2† (1.0) 6 (1.4) 9 (2.1) Similar frequency of serious, all-grade adverse events, toxicity-driven discontinuations, laboratory abnormalities, AIDS-defining events among MVC and placebo arms at Week 48. *Includes all patients who received at least one dose of study medication. †Includes deaths reported up to 28 days after stopping study drug. No deaths were related to study drug according to the investigator. David Hardy et al. CROI 2008; abstract 792. Reprinted with permission. An Update on New HIV Antiretroviral Agents 47 MERIT: Comparison of Efavirenz and Maraviroc in ARV-Naïve Patients The Body PRO Efavirenz (EFV 600 mg QD) + Combivir (ZDV+3TC)* Randomization 1:1 Maraviroc (MVC 300 mg BID) + Combivir (ZDV+3TC)* Screening (6 weeks) 0 48 wk First patient visit Nov, 2004 Primary analysis Patient eligibility criteria: • ≥ 16 years of age • Treatment naive • R5 HIV-1 infection • HIV-1 RNA ≥ 2,000 copies/mL • No evidence of resistance to EFV, ZDV, or 3TC 96 wk MVC QD arm discontinued at end of Phase 2b (week 16) for failure to meet protocol-defined criteria to continue (205 pts completed 16 weeks) *Patients experiencing toxicity to ZDV or 3TC were Patients stratified by: permitted to substitute an alternative NRTI • HIV-1 RNA < and ≥ 100,000 copies/mL at screening • Geographic location: Northern Hemisphere and Southern Hemisphere Michael Saag et al. IAS 2007; abstract WESS104. Reprinted with permission. An Update on New HIV Antiretroviral Agents 48 MERIT: Summary of Discontinuations Through 48 Weeks The Body PRO EFV + CBV N=361 MVC + CBV N=360 91 (25.2) 97 (26.9) Adverse event, N (%) 49 (13.6) 15 (4.2) Lack of efficacy, N (%) 15 (4.2) 43 (11.9) Other reason, N (%) 9 (2.5) 14 (3.9) Withdrew consent or lost to follow-up, N (%) 18 (5.0) 25 (6.9) Reason for Discontinuation All, N (%) Michael Saag et al. IAS 2007; abstract WESS104. Reprinted with permission. An Update on New HIV Antiretroviral Agents 49 MERIT: Percentage of Patients with Undetectable HIV-1 RNA at Week 48 (Primary Endpoint) The Body PRO 100 90 80 < 400 Copies/mL < 50 Copies/mL –3.0* (–9.5†) –4.2* (–10.9†) 73.1 Patients (%) 70 70.6 69.3 EFV + CBV MVC + CBV 65.3 Mean ∆ CD4+ from baseline: EFV +144 vs. MVC +170 cells/mm3 Difference: +26 (95% CI: +7, +46) 60 50 40 *Difference (adjusted for randomization strata) 30 20 Intent-to-treat (ITT) analysis 10 0 N= 361 360 361 360 †Lower bound of 1-sided 97.5% confidence interval; noninferiority margin = –10% Per-protocol analysis: <400 copies/mL difference = -4.1 (-10.5†), <50 copies/mL difference = -4.4 (-11.2†) Michael Saag et al. IAS 2007; abstract WESS104. Reprinted with permission. An Update on New HIV Antiretroviral Agents 50 MERIT: Percentage of Patients with HIV-1 RNA < 50 Copies/mL by HIV-1 RNA at Screening The Body PRO 100 < 100,000 copies/mL 90 80 71.6 Patients (%) 70 ≥ 100,000 copies/mL EFV + CBV 69.6 66.6 60 MVC + CBV 59.6 50 40 30 20 10 0 N= 211 204 150 156 Difference in < 50 noted in Southern Hemisphere (71% vs. 62%); No difference in Northern Hemisphere (67% vs. 68%) Missing values classified as failures/non-responders Michael Saag et al. IAS 2007; abstract WESS104. Reprinted with permission. An Update on New HIV Antiretroviral Agents 51 Summary of Dose Modifications with Maraviroc The Body PRO Concomitant Treatment A.M. Dose P.M. Dose 150 mg 150 mg Includes a Potent CYP3A4 Inhibitor PIs ± ritonavir (except tipranavir), clarithromycin, delavirdine, elvitegravir, itraconazole, ketoconazole, nefazadone, telithromycin YES NO Includes a CYP3A4 Inducer efavirenz, etravirine, rifampicin YES 300 mg 300 mg 300 mg 300 mg 300 mg 300 mg NO No CYP3A4 Inhibitors or Inducers NRTIs, nevirapine, tipranavir/r Adapted from Maraviroc [package insert]. New York, NY: Pfizer Labs; 2007. An Update on New HIV Antiretroviral Agents 52 Take Home Message The Body PRO ARV development has been very successful in the past decade. The availability of new agents and new classes have increased treatment options for our treatment experienced patients. The potential use of these agents earlier in therapy have opened the door for new treatment strategies. There are several other agents in development that can further complement the enhanced activity of these new agents. An Update on New HIV Antiretroviral Agents
