Merck’s ISENTRESS® (raltegravir) Demonstrated Durable Reductions in HIV-1 Viral Load and Sustained Tolerability At Three Years of Treatment in Previously Untreated Adult Patients Infected with HIV-1

BOSTON--()--Merck (NYSE: MRK), known as MSD outside the United States and Canada, announced today that new Phase III data showed that adult patients with HIV-1 infection maintained undetectable viral loads and increases in CD4 cell counts at three years of treatment with ISENTRESS® (raltegravir) tablets in combination therapy, comparable to treatment with efavirenz in combination therapy. The new data demonstrated that the antiviral efficacy and safety profile of ISENTRESS seen at weeks 48 and 96 of treatment in this study were sustained through week 156. Data also showed that patients in both treatment arms of this study experienced similar changes in body fat composition. Additionally, ISENTRESS in combination therapy demonstrated less impact on lipids [total, low-density lipoprotein (LDL), high-density lipoprotein (HDL) cholesterol] and triglycerides at week 144. These findings from the ongoing STARTMRK clinical trial in previously untreated adult patients infected with HIV-1 (Poster Board 542) were presented at the Conference on Retroviruses and Opportunistic Infections (CROI) in Boston.

"These three-year results for ISENTRESS reinforce what we saw previously at week 96 with sustained decreases in HIV-1 viral loads and increases in CD4 cell counts," said Dr. Jürgen Rockstroh, University of Bonn, Bonn-Venusberg, Germany, who presented the data. "Also of note are the data on lipids, which were consistent with what we saw previously with the week 96 results."

ISENTRESS is indicated in combination with other antiretroviral (ARV) agents for the treatment of HIV-1 infection in treatment-naïve and treatment-experienced adults. The label for ISENTRESS is based on analyses of plasma HIV-1 RNA levels through 96 weeks in three double-blind controlled clinical studies of ISENTRESS. Two of these studies were conducted in clinically advanced, three-class antiretroviral (ARV) [non-nucleoside reverse transcriptase inhibitor (NNRTI), nucleoside reverse transcriptase inhibitor (NRTI), protease inhibitor (PI)] treatment-experienced adults and one was conducted in treatment-naïve adults. The safety and efficacy of ISENTRESS have not been established in pediatric patients. The use of other active agents with ISENTRESS is associated with a greater likelihood of treatment response.

STARTMRK study design

In this ongoing multicenter, double-blind, randomized, active-controlled Phase III study, 563 previously untreated HIV-1 infected adult patients received either 400 mg ISENTRESS orally twice daily (n=281) or 600 mg efavirenz orally once daily (n=282), each in combination with tenofovir/emtricitabine. The primary endpoints of the study were reductions in HIV-1 viral load to less than 50 copies/mL and an evaluation of safety and tolerability at week 48. Secondary endpoints included ARV activity as measured by the proportion of patients achieving HIV-1 viral load to less than 50 copies/mL, less than 400 copies/mL, and change from baseline in CD4 cell count at week 96, as well as tolerability and safety at week 96. The 156 week data reported at CROI represent three-year results from a planned five-year monitoring of outcomes.

Patients who entered the study were required to have HIV-1 viral loads greater than 5,000 copies/mL. At baseline, the geometric mean HIV-1 viral load level for patients on the regimen including ISENTRESS was 103,205 copies/mL (n=281) and for the efavirenz regimen was 106,215 copies/mL (n=282). Mean baseline CD4 cell counts were 218.9 cells/mm3 and 217.4 cells/mm3 for the groups receiving ISENTRESS and efavirenz, respectively.

STARTMRK study showed sustained suppression of HIV-1 viral load and increases in CD4 cell counts maintained at 156 weeks

At week 156 of treatment, the regimen containing ISENTRESS suppressed HIV-1 viral load levels to below 50 copies/mL at a greater rate; 75.4 percent of patients (n=212/281) on the regimen containing ISENTRESS and 68.1 percent of patients (n=192/282) on the regimen containing efavirenz maintained HIV-1 viral load suppression below 50 copies/mL [treatment difference of 7.3 percent of patients with 95 percent confidence interval (CI): -0.2, 14.7].

Additionally, 79.7 percent of patients (n=224/281) on the regimen containing ISENTRESS and 72 percent of patients (n=203/282) on the regimen containing efavirenz maintained HIV-1 viral load suppression below 400 copies/mL [treatment difference of 7.6 percent of patients with 95 percent CI: 0.5, 14.6].

Results also showed that patients on the regimen containing ISENTRESS in combination therapy experienced an increase from baseline in mean CD4 cell count of 332 cells/mm3 and those on the regimen containing efavirenz of 295 cells/mm3 [treatment difference of 37 with 95 percent CI: 4, 69].

Metabolic profiles and body composition changes studied in STARTMRK

Metabolic parameters, including fasting lipids and glucose abnormalities, were evaluated according to the National Institutes of Health’s Division of Acquired Immunodeficiency Syndrome (NIH-DAIDS) criteria and compared against the National Cholesterol Education Program (NCEP) goals.

A fasting lipid visit was conducted at week 144, and ISENTRESS in combination therapy had less impact on total, LDL and HDL cholesterol levels, and triglycerides levels. Total cholesterol/HDL-C ratio and fasting glucose levels did not differ between the two treatment groups.

Mean changes from baseline in lipid levels and fasting glucose at week 144

                               
     

Baseline for
ISENTRESS
combination
therapy

    ISENTRESS    

Baseline for
Efavirenz
combination
therapy

    Efavirenz     P Value
Total Cholesterol     159.5 mg/dL     12.60 mg/dL     155.5 mg/dL     39.77 mg/dL     ≤0.001
HDL Cholesterol     38.37 mg/dL     4.48 mg/dL     37.94 mg/dL     10.54 mg/dL     ≤0.001
LDL Cholesterol     96.87 mg/dL     7.16 mg/dL     91.61 mg/dL     22.52 mg/dL     ≤0.001
Triglycerides     125.9 mg/dL     1.03 mg/dL     138.8 mg/dL     45.24 mg/dL     0.004
Total Cholesterol/

HDL-C Ratio

    4.41     -0.20     4.38     0.04     0.061
Glucose     91.47 mg/dL     3.16 mg/dL     90.21 mg/dL     6.04 mg/dL     0.137

To assess the metabolic changes related to body fat distribution, dual energy X-ray absorptiometry (DEXA) scans were evaluated in a subset of patients. The scans measured body fat redistribution, known as lipodystrophy. Body fat composition changes as measured by DEXA scan were experienced in both treatment groups, with a majority of patients experiencing modest fat gain overall and modest increases in trunk and appendicular (limb) fat at week 156. One in 25 patients on the regimen containing ISENTRESS and two in 32 patients on the regimen containing efavirenz experienced at least a 20 percent loss of body fat, or lipoatrophy.

Mean percent (95% CI) body composition change from baseline at 156 weeks*

             
Region     ISENTRESS (n=25)     Efavirenz (n=32)
Arms     19.07     34.91
Legs     16.55     22.74
Appendicular     16.92     24.90
Trunk     21.31     37.85
Total     18.94     31.07

*Subset includes patients who had scans at baseline, week 48 and/or week 96; and week 156

Tolerability profile of ISENTRESS in treatment-naïve patients at 156 weeks

At week 156, the overall incidence of drug-related clinical adverse events (AEs) in this study was lower for patients on the regimen containing ISENTRESS compared to the regimen containing efavirenz (49.5 percent vs. 79.8 percent, respectively). There were few treatment discontinuations due to clinical AEs for either regimen, 4.6 percent for patients on the regimen containing ISENTRESS vs. 7.4 percent for patients on the regimen containing efavirenz. The rate of serious clinical AEs seen in this study was similar (16.4 percent vs. 16.3 percent, respectively). Between week 96 and week 156, there were 32 new serious clinical AEs (n=15 and n=17, respectively). Although not considered drug-related, there were four deaths in the treatment group containing ISENTRESS and zero in the treatment group containing efavirenz.

At week 96, the most commonly reported drug-related adverse event of moderate to severe intensity that occurred in greater than or equal to two percent of patients and at a higher incidence than efavirenz in treatment-naïve patients receiving ISENTRESS was insomnia (4 percent vs. 3 percent, respectively).

Additional ISENTRESS data presentations at CROI 2011

Oral presentation

  • QDMRK, A Phase III Study of the Safety & Efficacy of Once Daily Versus Twice Daily Raltegravir (RAL) in Combination Therapy for Treatment-Naïve HIV-Infected Patients (Paper 150LB)

Poster presentation

  • Interim Results from IMPAACT P1066: Raltegravir (RAL) Oral Chewable Tablet Formulation for 2-5 Year Olds (Poster Board 715)

In addition, a total of 19 data presentations evaluating ISENTRESS from the Merck Investigator Studies Program (MISP) were presented at the conference.

About ISENTRESS

ISENTRESS is Merck's integrase inhibitor for the treatment of HIV-1 infection in treatment-naïve and treatment-experienced adult patients. ISENTRESS currently is the only approved integrase inhibitor for the treatment of HIV-1. ISENTRESS works by inhibiting the insertion of HIV-1 DNA into human DNA by the integrase enzyme and has demonstrated rapid antiviral activity. Inhibiting integrase from performing this essential function limits the ability of the virus to replicate and infect new cells. Other HIV-1 drugs in use inhibit two other enzymes critical to the HIV-1 replication process – protease and reverse transcriptase – but ISENTRESS is the only approved drug that inhibits the integrase enzyme. ISENTRESS is now approved in more than 90 countries worldwide. Merck is continuing to move forward with filings in additional countries around the world for use of ISENTRESS in both treatment-experienced and treatment-naïve HIV-infected patients.

Important safety information about ISENTRESS

ISENTRESS does not cure HIV or AIDS and does not prevent passing HIV to others. Healthcare providers should know that immune reconstitution syndrome has been reported in patients treated with ARV therapy, which may necessitate further evaluation and treatment.

Creatine kinase elevations were observed in subjects who received ISENTRESS. Myopathy and rhabdomyolysis have been reported. ISENTRESS should be used with caution in patients at increased risk of myopathy or rhabdomyolysis, such as patients receiving concomitant medication known to cause these conditions.

The most commonly reported drug-related adverse event (AE) of moderate to severe intensity that occurred in greater than or equal to two percent of patients and at a higher incidence than efavirenz in treatment-naïve patients receiving ISENTRESS was insomnia (four percent versus three percent, respectively).

The most commonly reported (greater than or equal to two percent in either treatment group) drug-related clinical AE of moderate or severe intensity in treatment-experienced patients receiving ISENTRESS and at a higher rate compared to placebo was headache (two percent vs. less than two percent) for ISENTRESS plus optimized background therapy (OBT) and placebo plus OBT, respectively.

In treatment-experienced patients, rash occurred more often in patients taking ISENTRESS and darunavir together than with either drug separately. Rashes were mild to moderate in severity and did not limit therapy. There were no discontinuations due to rash.

Dosing and administration

ISENTRESS is a single 400 mg tablet taken twice daily without regard to food. The dose of ISENTRESS should be increased during coadmistration with rifampin to 800 mg twice daily.

Drug interactions

Co administration with strong inducers of uridine diphosphate glucuronosyltransferase (UGT) 1A1 may reduce plasma concentrations of ISENTRESS. Rifampin, a strong inducer of (UGT) 1A1 reduces plasma concentrations of ISENTRESS. Based on the results of drug interaction studies and the clinical trials data, no dose adjustment of ISENTRESS is required when co administered with other ARV agents. Also, preclinical studies show that ISENTRESS is not metabolized by cytochrome P450 enzymes.

About Merck

Today's Merck is a global healthcare leader working to help the world be well. Merck is known as MSD outside the United States and Canada. Through our prescription medicines, vaccines, biologic therapies, and consumer care and animal health products, we work with customers and operate in more than 140 countries to deliver innovative health solutions. We also demonstrate our commitment to increasing access to healthcare through far-reaching policies, programs and partnerships. For more information, visit www.merck.com.

Forward-Looking Statement

This news release includes “forward-looking statements” within the meaning of the safe harbor provisions of the United States Private Securities Litigation Reform Act of 1995. Such statements may include, but are not limited to, statements about the benefits of the merger between Merck and Schering-Plough, including future financial and operating results, the combined company’s plans, objectives, expectations and intentions and other statements that are not historical facts. Such statements are based upon the current beliefs and expectations of Merck’s management and are subject to significant risks and uncertainties. Actual results may differ from those set forth in the forward-looking statements.

The following factors, among others, could cause actual results to differ from those set forth in the forward-looking statements: the possibility that the expected synergies from the merger of Merck and Schering-Plough will not be realized, or will not be realized within the expected time period; the impact of pharmaceutical industry regulation and health care legislation; the risk that the businesses will not be integrated successfully; disruption from the merger making it more difficult to maintain business and operational relationships; Merck’s ability to accurately predict future market conditions; dependence on the effectiveness of Merck’s patents and other protections for innovative products; the risk of new and changing regulation and health policies in the United States and internationally and the exposure to litigation and/or regulatory actions.

Merck undertakes no obligation to publicly update any forward-looking statement, whether as a result of new information, future events or otherwise. Additional factors that could cause results to differ materially from those described in the forward-looking statements can be found in Merck’s 2010 Annual Report on Form 10-K and the company’s other filings with the Securities and Exchange Commission (SEC) available at the SEC’s Internet site (www.sec.gov).

Before prescribing ISENTRESS® (raltegravir) Tablets, please read the attached prescribing information, which also is available at http://www.merck.com/product/usa/pi_circulars/i/isentress/isentress_pi.pdf, and the attached patient information, which also is available at http://www.merck.com/product/usa/pi_circulars/i/isentress/isentress_ppi.pdf.

ISENTRESS® is a registered trademark of Merck & Co., Inc., Whitehouse Station, N.J., USA

HIGHLIGHTS OF PRESCRIBING INFORMATION

These highlights do not include all the information needed to use ISENTRESS safely and effectively. See full prescribing information for ISENTRESS.

ISENTRESS (raltegravir) Tablets
Initial U.S. Approval: 2007

RECENT MAJOR CHANGES

Indications And Usage (1) 06/2010

INDICATIONS AND USAGE

ISENTRESS® is a human immunodeficiency virus integrase strand transfer inhibitor (HIV-1 INSTI) indicated:

  • In combination with other antiretroviral agents for the treatment of HIV-1 infection in adult patients (1).

The safety and efficacy of ISENTRESS have not been established in pediatric patients (1).

DOSAGE AND ADMINISTRATION

  • 400 mg administered orally, twice daily with or without food (2).
  • During coadministration with rifampin, 800 mg twice daily (2).

DOSAGE FORMS AND STRENGTHS

Tablets: 400 mg (3).

CONTRAINDICATIONS

None (4).

WARNINGS AND PRECAUTIONS

Monitor for Immune Reconstitution Syndrome (5.1).

ADVERSE REACTIONS

  • The most common adverse reactions of moderate to severe intensity (≥2%) which occurred at a higher rate than the comparator are insomnia and headache (6.1).
  • Creatine kinase elevations were observed in subjects who received ISENTRESS. Myopathy and rhabdomyolysis have been reported. Use with caution in patients at increased risk of myopathy or rhabdomyolysis, such as patients receiving concomitant medications known to cause these conditions (6.1).

To report SUSPECTED ADVERSE REACTIONS, contact Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc., at 1-877-888-4231 or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch.

DRUG INTERACTIONS

  • Coadministration of ISENTRESS with drugs that are strong inducers of UGT1A1 may result in reduced plasma concentrations of raltegravir (7.2).

USE IN SPECIFIC POPULATIONS

Pregnancy:

  • ISENTRESS should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus. Physicians are encouraged to register pregnant women exposed to ISENTRESS by calling 1-800-258-4263 so that Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc., can monitor maternal and fetal outcomes (8.1).

Nursing Mothers:

  • Breast-feeding is not recommended while taking ISENTRESS (8.3).

See 17 for PATIENT COUNSELING INFORMATION and FDA-approved patient labeling.

Revised: 02/2011

FULL PRESCRIBING INFORMATION: CONTENTS*

1

 

INDICATIONS AND USAGE

2

DOSAGE AND ADMINISTRATION

3

DOSAGE FORMS AND STRENGTHS

4

CONTRAINDICATIONS

5

WARNINGS AND PRECAUTIONS

5.1   Immune Reconstitution Syndrome

6

ADVERSE REACTIONS

6.1 Clinical Trials Experience
6.2 Postmarketing Experience

7

DRUG INTERACTIONS

7.1 Effect of Raltegravir on the Pharmacokinetics of Other Agents
7.2 Effect of Other Agents on the Pharmacokinetics of Raltegravir

8

USE IN SPECIFIC POPULATIONS

8.1 Pregnancy
8.3 Nursing Mothers
8.4 Pediatric Use
8.5 Geriatric Use
8.6 Use in Patients with Hepatic Impairment
8.7 Use in Patients with Renal Impairment

10

OVERDOSAGE

11

DESCRIPTION

12

CLINICAL PHARMACOLOGY

12.1 Mechanism of Action
12.2 Pharmacodynamics
12.3 Pharmacokinetics
12.4 Microbiology

13

NONCLINICAL TOXICOLOGY

13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

14

CLINICAL STUDIES

16

HOW SUPPLIED/STORAGE AND HANDLING

17

PATIENT COUNSELING INFORMATION

*Sections or subsections omitted from the Full Prescribing Information are not listed.

FULL PRESCRIBING INFORMATION

1 INDICATIONS AND USAGE

ISENTRESS1 is indicated in combination with other antiretroviral agents for the treatment of human immunodeficiency virus (HIV-1) infection in adult patients.

This indication is based on analyses of plasma HIV-1 RNA levels through 96 weeks in three double-blind controlled studies of ISENTRESS. Two of these studies were conducted in clinically advanced, 3-class antiretroviral (NNRTI, NRTI, PI) treatment-experienced adults and one was conducted in treatment-naïve adults.

The use of other active agents with ISENTRESS is associated with a greater likelihood of treatment response [see Clinical Studies (14)].

The safety and efficacy of ISENTRESS have not been established in pediatric patients.

2 DOSAGE AND ADMINISTRATION

For the treatment of patients with HIV-1 infection, the dosage of ISENTRESS is 400 mg administered orally, twice daily with or without food. During coadministration with rifampin, the recommended dosage of ISENTRESS is 800 mg twice daily with or without food.

3 DOSAGE FORMS AND STRENGTHS

400 mg pink, oval-shaped, film-coated tablets with "227" on one side.

4 CONTRAINDICATIONS

None

5 WARNINGS AND PRECAUTIONS

5.1 Immune Reconstitution Syndrome

During the initial phase of treatment, patients responding to antiretroviral therapy may develop an inflammatory response to indolent or residual opportunistic infections (such as Mycobacterium avium complex, cytomegalovirus, Pneumocystis jiroveci pneumonia, Mycobacterium tuberculosis, or reactivation of varicella zoster virus), which may necessitate further evaluation and treatment.

6 ADVERSE REACTIONS

6.1 Clinical Trials Experience

Because clinical trials are conducted under widely varying conditions, adverse reaction rates observed in the clinical trials of a drug cannot be directly compared to rates in the clinical trials of another drug and may not reflect the rates observed in practice.

Treatment-Naïve Studies

The following safety assessment of ISENTRESS in treatment-naïve subjects is based on the randomized double-blind active controlled study of treatment-naïve subjects, STARTMRK (Protocol 021) with ISENTRESS 400 mg twice daily in combination with a fixed dose of emtricitabine 200 mg (+) tenofovir 300 mg, (N=281) versus efavirenz (EFV) 600 mg at bedtime in combination with emtricitabine (+) tenofovir, (N=282). During double-blind treatment, the total follow-up for subjects receiving ISENTRESS 400 mg twice daily + emtricitabine (+) tenofovir was 480 patient-years and 463 patient-years for subjects receiving efavirenz 600 mg at bedtime + emtricitabine (+) tenofovir.

In Protocol 021, the rate of discontinuation of therapy due to adverse reactions was 4% in subjects receiving ISENTRESS + emtricitabine (+) tenofovir and 7% in subjects receiving efavirenz + emtricitabine (+) tenofovir.

The clinical adverse drug reactions (ADRs) listed below were considered by investigators to be causally related to ISENTRESS + emtricitabine (+) tenofovir or efavirenz + emtricitabine (+) tenofovir. Clinical ADRs of moderate to severe intensity occurring in ≥2% of treatment-naïve subjects treated with ISENTRESS and occurring at a higher rate than efavirenz are presented in Table 1.

   

Table 1: Adverse Reactions* of Moderate to Severe Intensity(†) Occurring in ≥2% of

Treatment-Naïve Adult Subjects Receiving ISENTRESS
and at a Higher Rate Compared to Efavirenz
(96 Week Analysis)
 

System Organ Class,
Preferred Term

Randomized Study Protocol 021
   

ISENTRESS 400 mg
Twice Daily +
Emtricitabine (+) Tenofovir
(n = 281)
%

 

   

Efavirenz 600 mg
At Bedtime +
Emtricitabine (+) Tenofovir
(n = 282)
%

 

Psychiatric Disorders
Insomnia     4     3
*Includes adverse experiences considered by investigators to be at least possibly, probably, or definitely related to the drug.
(†)Intensities are defined as follows: Moderate (discomfort enough to cause interference with usual activity); Severe (incapacitating with inability to work or do usual activity).
(‡)n = total number of subjects per treatment group
 

Laboratory Abnormalities

The percentages of adult subjects treated with ISENTRESS 400 mg twice daily or efavirenz in Protocol 021 with selected Grades 2 to 4 laboratory abnormalities that represent a worsening Grade from baseline are presented in Table 2.

 
Table 2: Selected Grade 2 to 4 Laboratory Abnormalities
Reported in Treatment-Naïve Subjects
(96 Week Analysis)
   
Randomized Study Protocol 021
Laboratory Limit ISENTRESS   Efavirenz
Parameter 400 mg 600 mg
Preferred Term Twice Daily + At Bedtime +
(Unit) Emtricitabine Emtricitabine
(+) Tenofovir (+) Tenofovir
        (N = 281)   (N = 282)
Hematology  

Absolute neutrophil count (103/μL)

Grade 2 0.75 - 0.999 3% 4%
Grade 3 0.50 - 0.749 2% 1%
Grade 4   <0.50   <1%   <1%
Hemoglobin (gm/dL)
Grade 2 7.5 - 8.4 1% 1%
Grade 3 6.5 - 7.4 <1% 1%
Grade 4   <6.5   <1%   0%
Platelet count (103/μL)
Grade 2 50 - 99.999 2% 0%
Grade 3 25 - 49.999 <1% <1%
Grade 4   <25   0%   0%
Blood chemistry  
Fasting (non-random) serum glucose test (mg/dL)
Grade 2 126 - 250 3% 4%
Grade 3 251 - 500 1% 0%
Grade 4   >500   0%   0%
Total serum bilirubin
Grade 2 1.6 - 2.5 x ULN 4% 0%
Grade 3 2.6 - 5.0 x ULN 1% 0%
Grade 4   >5.0 x ULN   0%   0%
Serum aspartate aminotransferase
Grade 2 2.6 - 5.0 x ULN 4% 5%
Grade 3 5.1 - 10.0 x ULN 2% 2%
Grade 4   >10.0 x ULN   1%   <1%
Serum alanine aminotransferase
Grade 2 2.6 - 5.0 x ULN 6% 9%
Grade 3 5.1 - 10.0 x ULN 1% 2%
Grade 4   >10.0 x ULN   1%   1%
Serum alkaline phosphatase
Grade 2 2.6 - 5.0 x ULN 1% 3%
Grade 3 5.1 - 10.0 x ULN 0% <1%
Grade 4   >10.0 x ULN   0%   <1%
ULN = Upper limit of normal range
 

Lipids, Change from Baseline

Changes from baseline in fasting lipids are shown in Table 3.

   

Table 3: Lipid Values, Mean Change from Baseline, Protocol 021

 
Laboratory Parameter ISENTRESS 400 mg Efavirenz 600 mg
Preferred Term Twice Daily + Emtricitabine (+) Tenofovir At Bedtime + Emtricitabine (+) Tenofovir
    N = 281   N = 282
  Change from   Change from
Baseline at Baseline at
    Week 96       Week 96
Baseline   Week 96 Mean Change Baseline   Week 96 Mean Change
Mean Mean Mean Mean
    (mg/dL)   (mg/dL)   (mg/dL)   (mg/dL)   (mg/dL)   (mg/dL)
LDL-Cholesterol* 96 103 7 93 115 21
HDL-Cholesterol* 39 42 3 38 48 10
Total Cholesterol* 159 169 10 156 194 38
Triglyceride*   125   121   -4   137   177   40
*Fasting (non-random) laboratory tests.
Notes:
N = Number of subjects in the treatment group. The analysis is based on all available data.
If subjects initiated or increased serum lipid-reducing agents, the last available lipid values prior to the change in therapy were used in the analysis. If the missing data was due to other reasons, subjects were censored thereafter for the analysis.
At baseline, serum lipid-reducing agents were used in 5% of subjects in the group receiving ISENTRESS and 3% in the efavirenz group. Through Week 96, serum lipid-reducing agents were used in 7% of subjects in the group receiving ISENTRESS and 9% in the efavirenz group.
 

Treatment-Experienced Studies

The safety assessment of ISENTRESS in treatment-experienced subjects is based on the pooled safety data from the randomized, double-blind, placebo-controlled trials, BENCHMRK 1 and BENCHMRK 2 (Protocols 018 and 019) in antiretroviral treatment-experienced HIV-1 infected adult subjects. A total of 462 subjects received the recommended dose of ISENTRESS 400 mg twice daily in combination with optimized background therapy (OBT) compared to 237 subjects taking placebo in combination with OBT. The median duration of therapy in these trials was 96 weeks for subjects receiving ISENTRESS and 38 weeks for subjects receiving placebo. The total exposure to ISENTRESS was 708 patient-years versus 244 patient-years on placebo. The rates of discontinuation due to adverse events were 4% in subjects receiving ISENTRESS and 5% in subjects receiving placebo.

Clinical ADRs were considered by investigators to be causally related to ISENTRESS + OBT or placebo + OBT. Clinical ADRs of moderate to severe intensity occurring in ≥2% of subjects treated with ISENTRESS and occurring at a higher rate compared to placebo are presented in Table 4.

 
Table 4: Adverse Drug Reactions* of Moderate to Severe Intensity(†) Occurring in ≥2%
of Treatment-Experienced Adult Subjects Receiving ISENTRESS
and at a Higher Rate Compared to Placebo
(96 Week Analysis)
 

System Organ Class,
Adverse Reactions

Randomized Studies Protocol 018 and 019
 

ISENTRESS 400 mg Twice Daily
+ OBT
(n = 462)

 

 

Placebo + OBT
(n = 237)

 

Nervous System Disorders
Headache   2   <1
*Includes adverse reactions at least possibly, probably, or definitely related to the drug.
(†)Intensities are defined as follows: Moderate (discomfort enough to cause interference with usual activity); Severe (incapacitating with inability to work or do usual activity).
(‡)n=total number of subjects per treatment group.
 

Laboratory Abnormalities

The percentages of adult subjects treated with ISENTRESS 400 mg twice daily or placebo in Protocols 018 and 019 with selected Grade 2 to 4 laboratory abnormalities representing a worsening Grade from baseline are presented in Table 5.

   
Table 5: Selected Grade 2 to 4 Laboratory Abnormalities Reported in
Treatment-Experienced Subjects (96 Week Analysis)
 
Randomized Studies Protocol 018 and 019
Laboratory Limit ISENTRESS   Placebo
Parameter 400 mg +
Preferred Term Twice Daily OBT
(Unit)

+ OBT

(N = 237)
        (N = 462)    
Hematology  

Absolute neutrophil count (103/μL)

Grade 2 0.75 - 0.999 4% 5%
Grade 3 0.50 - 0.749 3% 3%
Grade 4   <0.50   1%   <1%
Hemoglobin (gm/dL)
Grade 2 7.5 - 8.4 1% 3%
Grade 3 6.5 - 7.4 1% 1%
Grade 4   <6.5   <1%   0%
Platelet count (103/μL)
Grade 2 50 - 99.999 3% 5%
Grade 3 25 - 49.999 1% <1%
Grade 4   <25   1%   <1%
Blood chemistry  

Fasting (non-random) serum glucose test (mg/dL)

Grade 2 126 - 250 10% 7%
Grade 3 251 - 500 3% 1%
Grade 4   >500   0%   0%
Total serum bilirubin
Grade 2 1.6 - 2.5 x ULN 6% 3%
Grade 3 2.6 - 5.0 x ULN 3% 3%
Grade 4   >5.0 x ULN   1%   0%
Serum aspartate aminotransferase
Grade 2 2.6 - 5.0 x ULN 9% 7%
Grade 3 5.1 - 10.0 x ULN 4% 3%
Grade 4   >10.0 x ULN   1%   1%
Serum alanine aminotransferase
Grade 2 2.6 - 5.0 x ULN 9% 9%
Grade 3 5.1 - 10.0 x ULN 4% 2%
Grade 4   >10.0 x ULN   1%   2%
Serum alkaline phosphatase
Grade 2 2.6 - 5.0 x ULN 2% <1%
Grade 3 5.1 - 10.0 x ULN <1% 1%
Grade 4   >10.0 x ULN   1%   <1%
Serum pancreatic amylase test
Grade 2 1.6 - 2.0 x ULN 2% 1%
Grade 3 2.1 - 5.0 x ULN 4% 3%
Grade 4   >5.0 x ULN   <1%   <1%
Serum lipase test
Grade 2 1.6 - 3.0 x ULN 5% 4%
Grade 3 3.1 - 5.0 x ULN 2% 1%
Grade 4   >5.0 x ULN   0%   0%
Serum creatine kinase
Grade 2 6.0 - 9.9 x ULN 2% 2%
Grade 3 10.0 - 19.9 x ULN 4% 3%
Grade 4   ≥20.0 x ULN   3%   1%
ULN = Upper limit of normal range
 

Less Common Adverse Reactions Observed in Treatment-Naïve and Treatment-Experienced Studies

The following ADRs occurred in <2% of treatment-naïve or treatment-experienced subjects receiving ISENTRESS in a combination regimen. These events have been included because of their seriousness, increased frequency on ISENTRESS compared with efavirenz or placebo, or investigator's assessment of potential causal relationship.

Gastrointestinal Disorders: abdominal pain, gastritis, dyspepsia, vomiting, nausea

General Disorders and Administration Site Conditions: fatigue, asthenia

Hepatobiliary Disorders: hepatitis

Immune System Disorders: hypersensitivity

Infections and Infestations: genital herpes, herpes zoster

Nervous System Disorders: dizziness

Psychiatric Disorders: depression (particularly in subjects with a pre-existing history of psychiatric illness), including suicidal ideation and behaviors

Renal and Urinary Disorders: nephrolithiasis, renal failure

Selected Adverse Events

Cancers were reported in treatment-experienced subjects who initiated ISENTRESS or placebo, both with OBT, and in treatment-naïve subjects who initiated ISENTRESS or efavirenz, both with emtricitabine (+) tenofovir; several were recurrent. The types and rates of specific cancers were those expected in a highly immunodeficient population (many had CD4+ counts below 50 cells/mm3 and most had prior AIDS diagnoses). The risk of developing cancer in these studies was similar in the group receiving ISENTRESS and the group receiving the comparator.

Grade 2-4 creatine kinase laboratory abnormalities were observed in subjects treated with ISENTRESS (see Table 5). Myopathy and rhabdomyolysis have been reported. Use with caution in patients at increased risk of myopathy or rhabdomyolysis, such as patients receiving concomitant medications known to cause these conditions.

Rash occurred more commonly in treatment-experienced subjects receiving regimens containing ISENTRESS + darunavir/ritonavir compared to subjects receiving ISENTRESS without darunavir/ritonavir or darunavir/ritonavir without ISENTRESS. However, rash that was considered drug related occurred at similar rates for all three groups. These rashes were mild to moderate in severity and did not limit therapy; there were no discontinuations due to rash.

Patients with Co-existing Conditions

Patients Co-infected with Hepatitis B and/or Hepatitis C Virus

In the randomized, double-blind, placebo-controlled trials, treatment-experienced subjects (N = 114/699 or 16%) and treatment-naïve subjects (N = 34/563 or 6%) with chronic (but not acute) active hepatitis B and/or hepatitis C virus co-infection were permitted to enroll provided that baseline liver function tests did not exceed 5 times the upper limit of normal (ULN). In general the safety profile of ISENTRESS in subjects with hepatitis B and/or hepatitis C virus co-infection was similar to that in subjects without hepatitis B and/or hepatitis C virus co-infection, although the rates of AST and ALT abnormalities were higher in the subgroup with hepatitis B and/or hepatitis C virus co-infection for all treatment groups. In treatment-experienced subjects, Grade 2 or higher laboratory abnormalities that represent a worsening Grade from baseline of AST, ALT or total bilirubin occurred in 29%, 34% and 13%, respectively, of co-infected subjects treated with ISENTRESS as compared to 11%, 10% and 9% of all other subjects treated with ISENTRESS. In treatment-naïve subjects, Grade 2 or higher laboratory abnormalities that represent a worsening Grade from baseline of AST, ALT or total bilirubin occurred in 17%, 28% and 17%, respectively, of co-infected subjects treated with ISENTRESS as compared to 6%, 6% and 3% of all other subjects treated with ISENTRESS.

6.2 Postmarketing Experience

The following adverse reactions have been identified during postapproval use of ISENTRESS. Because these reactions are reported voluntarily from a population of uncertain size, it is not always possible to reliably estimate their frequency or establish a causal relationship to drug exposure.

Blood and Lymphatic System Disorders: thrombocytopenia

Gastrointestinal Disorders: diarrhea

Hepatobiliary Disorders: hepatic failure (with and without associated hypersensitivity) in patients with underlying liver disease and/or concomitant medications

Musculoskeletal and Connective Tissue Disorders: rhabdomyolysis

Psychiatric Disorders: anxiety, paranoia

Skin and Subcutaneous Tissue Disorders: rash, Stevens-Johnson syndrome

7 DRUG INTERACTIONS

7.1 Effect of Raltegravir on the Pharmacokinetics of Other Agents

Raltegravir does not inhibit (IC50>100 µM) CYP1A2, CYP2B6, CYP2C8, CYP2C9, CYP2C19, CYP2D6 or CYP3A in vitro. Moreover, in vitro, raltegravir did not induce CYP1A2, CYP2B6 or CYP3A4. A midazolam drug interaction study confirmed the low propensity of raltegravir to alter the pharmacokinetics of agents metabolized by CYP3A4 in vivo by demonstrating a lack of effect of raltegravir on the pharmacokinetics of midazolam, a sensitive CYP3A4 substrate. Similarly, raltegravir is not an inhibitor (IC50>50 µM) of the UDP-glucuronosyltransferases (UGT) tested (UGT1A1, UGT2B7), and raltegravir does not inhibit P-glycoprotein-mediated transport. Based on these data, ISENTRESS is not expected to affect the pharmacokinetics of drugs that are substrates of these enzymes or P-glycoprotein (e.g., protease inhibitors, NNRTIs, opioid analgesics, statins, azole antifungals, proton pump inhibitors and anti-erectile dysfunction agents).

In drug interaction studies, raltegravir did not have a clinically meaningful effect on the pharmacokinetics of the following: hormonal contraceptives, methadone, lamivudine, tenofovir, etravirine, darunavir/ritonavir.

7.2 Effect of Other Agents on the Pharmacokinetics of Raltegravir

Raltegravir is not a substrate of cytochrome P450 (CYP) enzymes. Based on in vivo and in vitro studies, raltegravir is eliminated mainly by metabolism via a UGT1A1-mediated glucuronidation pathway.

Rifampin, a strong inducer of UGT1A1, reduces plasma concentrations of ISENTRESS. Therefore, the dose of ISENTRESS should be increased during coadministration with rifampin [see Dosage and Administration (2)]. The impact of other inducers of drug metabolizing enzymes, such as phenytoin and phenobarbital, on UGT1A1 is unknown.

Coadministration of ISENTRESS with drugs that inhibit UGT1A1 may increase plasma levels of raltegravir.

Selected drug interactions are presented in Table 6 [see Clinical Pharmacology (12.3)].

 

Table 6: Selected Drug Interactions

   
Concomitant Drug Class: Effect on Clinical Comment
Drug Name Concentration
    of Raltegravir    
HIV-1-Antiviral Agents
atazanavir     Atazanavir, a strong inhibitor of UGT1A1, increases plasma concentrations of raltegravir. However, since concomitant use of ISENTRESS with atazanavir/ritonavir did not result in a unique safety signal in Phase 3 studies, no dose adjustment is recommended.
atazanavir/ritonavir     Atazanavir/ritonavir increases plasma concentrations of raltegravir. However, since concomitant use of ISENTRESS with atazanavir/ritonavir did not result in a unique safety signal in Phase 3 studies, no dose adjustment is recommended.
efavirenz     Efavirenz reduces plasma concentrations of raltegravir. The clinical significance of this interaction has not been directly assessed.
etravirine     Etravirine reduces plasma concentrations of raltegravir. The clinical significance of this interaction has not been directly assessed.
tipranavir/ritonavir     Tipranavir/ritonavir reduces plasma concentrations of raltegravir. However, since comparable efficacy was observed for this combination relative to other ISENTRESS-containing regimens in Phase 3 studies 018 and 019, no dose adjustment is recommended.
Other Agents
omeprazole     Coadministration of medicinal products that increase gastric pH (e.g., omeprazole) may increase raltegravir levels based on increased raltegravir solubility at higher pH. However, since concomitant use of ISENTRESS with proton pump inhibitors and H2 blockers did not result in a unique safety signal in Phase 3 studies, no dose adjustment is recommended.
rifampin     Rifampin, a strong inducer of UGT1A1, reduces plasma concentrations of raltegravir. The recommended dosage of ISENTRESS is 800 mg twice daily during coadministration with rifampin.
 

8 USE IN SPECIFIC POPULATIONS

8.1 Pregnancy

Pregnancy Category C

ISENTRESS should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus. There are no adequate and well-controlled studies in pregnant women. In addition, there have been no pharmacokinetic studies conducted in pregnant patients.

Developmental toxicity studies were performed in rabbits (at oral doses up to 1000 mg/kg/day) and rats (at oral doses up to 600 mg/kg/day). The reproductive toxicity study in rats was performed with pre-, peri-, and postnatal evaluation. The highest doses in these studies produced systemic exposures in these species approximately 3- to 4-fold the exposure at the recommended human dose. In both rabbits and rats, no treatment-related effects on embryonic/fetal survival or fetal weights were observed. In addition, no treatment-related external, visceral, or skeletal changes were observed in rabbits. However, treatment-related increases over controls in the incidence of supernumerary ribs were seen in rats at 600 mg/kg/day (exposures 3-fold the exposure at the recommended human dose).

Placenta transfer of drug was demonstrated in both rats and rabbits. At a maternal dose of 600 mg/kg/day in rats, mean drug concentrations in fetal plasma were approximately 1.5-to 2.5-fold greater than in maternal plasma at 1 hour and 24 hours postdose, respectively. Mean drug concentrations in fetal plasma were approximately 2% of the mean maternal concentration at both 1 and 24 hours postdose at a maternal dose of 1000 mg/kg/day in rabbits.

Antiretroviral Pregnancy Registry

To monitor maternal-fetal outcomes of pregnant patients exposed to ISENTRESS, an Antiretroviral Pregnancy Registry has been established. Physicians are encouraged to register patients by calling 1-800-258-4263.

8.3 Nursing Mothers

Breast-feeding is not recommended while taking ISENTRESS. In addition, it is recommended that HIV-1-infected mothers not breast-feed their infants to avoid risking postnatal transmission of HIV-1.

It is not known whether raltegravir is secreted in human milk. However, raltegravir is secreted in the milk of lactating rats. Mean drug concentrations in milk were approximately 3-fold greater than those in maternal plasma at a maternal dose of 600 mg/kg/day in rats. There were no effects in rat offspring attributable to exposure of ISENTRESS through the milk.

8.4 Pediatric Use

Safety and effectiveness of ISENTRESS in pediatric patients have not been established.

8.5 Geriatric Use

Clinical studies of ISENTRESS did not include sufficient numbers of subjects aged 65 and over to determine whether they respond differently from younger subjects. Other reported clinical experience has not identified differences in responses between the elderly and younger subjects. In general, dose selection for an elderly patient should be cautious, reflecting the greater frequency of decreased hepatic, renal, or cardiac function, and of concomitant disease or other drug therapy.

8.6 Use in Patients with Hepatic Impairment

No clinically important pharmacokinetic differences between subjects with moderate hepatic impairment and healthy subjects were observed. No dosage adjustment is necessary for patients with mild to moderate hepatic impairment. The effect of severe hepatic impairment on the pharmacokinetics of raltegravir has not been studied [see Clinical Pharmacology (12.3)].

8.7 Use in Patients with Renal Impairment

No clinically important pharmacokinetic differences between subjects with severe renal impairment and healthy subjects were observed. No dosage adjustment is necessary [see Clinical Pharmacology (12.3)].

10 OVERDOSAGE

No specific information is available on the treatment of overdosage with ISENTRESS. Doses as high as 1600-mg single dose and 800-mg twice-daily multiple doses were studied in healthy volunteers without evidence of toxicity. Occasional doses of up to 1800 mg per day were taken in the clinical studies of HIV-1 infected subjects without evidence of toxicity.

In the event of an overdose, it is reasonable to employ the standard supportive measures, e.g., remove unabsorbed material from the gastrointestinal tract, employ clinical monitoring (including obtaining an electrocardiogram), and institute supportive therapy if required. The extent to which ISENTRESS may be dialyzable is unknown.

11 DESCRIPTION

ISENTRESS contains raltegravir potassium, a human immunodeficiency virus integrase strand transfer inhibitor. The chemical name for raltegravir potassium is N-[(4-Fluorophenyl)methyl]-1,6-dihydro-5-hydroxy-1-methyl-2-[1-methyl-1-[[(5-methyl-1,3,4-oxadiazol-2-yl)carbonyl]amino]ethyl]-6-oxo-4-pyrimidinecarboxamide monopotassium salt.

The empirical formula is C20H20FKN6O5 and the molecular weight is 482.51. The structural formula is:

(Graphic Omitted)

Raltegravir potassium is a white to off-white powder. It is soluble in water, slightly soluble in methanol, very slightly soluble in ethanol and acetonitrile and insoluble in isopropanol.

Each film-coated tablet of ISENTRESS for oral administration contains 434.4 mg of raltegravir potassium (as salt), equivalent to 400 mg of raltegravir (free phenol) and the following inactive ingredients: microcrystalline cellulose, lactose monohydrate, calcium phosphate dibasic anhydrous, hypromellose 2208, poloxamer 407 (contains 0.01% butylated hydroxytoluene as antioxidant), sodium stearyl fumarate, magnesium stearate. In addition, the film coating contains the following inactive ingredients: polyvinyl alcohol, titanium dioxide, polyethylene glycol 3350, talc, red iron oxide and black iron oxide.

12 CLINICAL PHARMACOLOGY

12.1 Mechanism of Action

Raltegravir is an HIV-1 antiviral drug [see Clinical Pharmacology (12.4)].

12.2 Pharmacodynamics

In a monotherapy study raltegravir (400 mg twice daily) demonstrated rapid antiviral activity with mean viral load reduction of 1.66 log10 copies/mL by Day 10.

In the randomized, double-blind, placebo-controlled, dose-ranging trial, Protocol 005, and Protocols 018 and 019, antiviral responses were similar among subjects regardless of dose.

Effects on Electrocardiogram

In a randomized, placebo-controlled, crossover study, 31 healthy subjects were administered a single oral supratherapeutic dose of raltegravir 1600 mg and placebo. Peak raltegravir plasma concentrations were approximately 4-fold higher than the peak concentrations following a 400 mg dose. ISENTRESS did not appear to prolong the QTc interval for 12 hours postdose. After baseline and placebo adjustment, the maximum mean QTc change was -0.4 msec (1-sided 95% upper Cl: 3.1 msec).

12.3 Pharmacokinetics

Absorption

Raltegravir is absorbed with a Tmax of approximately 3 hours postdose in the fasted state. Raltegravir AUC and Cmax increase dose proportionally over the dose range 100 mg to 1600 mg. Raltegravir C12hr increases dose proportionally over the dose range of 100 to 800 mg and increases slightly less than dose proportionally over the dose range 100 mg to 1600 mg. With twice-daily dosing, pharmacokinetic steady state is achieved within approximately the first 2 days of dosing. There is little to no accumulation in AUC and Cmax. The average accumulation ratio for C12hr ranged from approximately 1.2 to 1.6.

The absolute bioavailability of raltegravir has not been established.

In subjects who received 400 mg twice daily alone, raltegravir drug exposures were characterized by a geometric mean AUC0-12hr of 14.3 μM●hr and C12hr of 142 nM.

Considerable variability was observed in the pharmacokinetics of raltegravir. For observed C12hr in Protocols 018 and 019, the coefficient of variation (CV) for inter-subject variability = 212% and the CV for intra-subject variability = 122%.

Effect of Food on Oral Absorption

ISENTRESS may be administered with or without food. Raltegravir was administered without regard to food in the pivotal safety and efficacy studies in HIV-1-infected patients. The effect of consumption of low-, moderate- and high-fat meals on steady-state raltegravir pharmacokinetics was assessed in healthy volunteers. Administration of multiple doses of raltegravir following a moderate-fat meal (600 Kcal, 21 g fat) did not affect raltegravir AUC to a clinically meaningful degree with an increase of 13% relative to fasting. Raltegravir C12hr was 66% higher and Cmax was 5% higher following a moderate-fat meal compared to fasting. Administration of raltegravir following a high-fat meal (825 Kcal, 52 g fat) increased AUC and Cmax by approximately 2-fold and increased C12hr by 4.1-fold. Administration of raltegravir following a low-fat meal (300 Kcal, 2.5 g fat) decreased AUC and Cmax by 46% and 52%, respectively; C12hr was essentially unchanged. Food appears to increase pharmacokinetic variability relative to fasting.

Distribution

Raltegravir is approximately 83% bound to human plasma protein over the concentration range of 2 to 10 µM.

Metabolism and Excretion

The apparent terminal half-life of raltegravir is approximately 9 hours, with a shorter α-phase half-life (~1 hour) accounting for much of the AUC. Following administration of an oral dose of radiolabeled raltegravir, approximately 51 and 32% of the dose was excreted in feces and urine, respectively. In feces, only raltegravir was present, most of which is likely derived from hydrolysis of raltegravir-glucuronide secreted in bile as observed in preclinical species. Two components, namely raltegravir and raltegravir-glucuronide, were detected in urine and accounted for approximately 9 and 23% of the dose, respectively. The major circulating entity was raltegravir and represented approximately 70% of the total radioactivity; the remaining radioactivity in plasma was accounted for by raltegravir-glucuronide. Studies using isoform-selective chemical inhibitors and cDNA-expressed UDP-glucuronosyltransferases (UGT) show that UGT1A1 is the main enzyme responsible for the formation of raltegravir-glucuronide. Thus, the data indicate that the major mechanism of clearance of raltegravir in humans is UGT1A1-mediated glucuronidation.

Special Populations

Pediatric

The pharmacokinetics of raltegravir in pediatric patients has not been established.

Age

The effect of age on the pharmacokinetics of raltegravir was evaluated in the composite analysis. No dosage adjustment is necessary.

Race

The effect of race on the pharmacokinetics of raltegravir was evaluated in the composite analysis. No dosage adjustment is necessary.

Gender

A study of the pharmacokinetics of raltegravir was performed in healthy adult males and females. Additionally, the effect of gender was evaluated in a composite analysis of pharmacokinetic data from 103 healthy subjects and 28 HIV-1 infected subjects receiving raltegravir monotherapy with fasted administration. No dosage adjustment is necessary.

Hepatic Impairment

Raltegravir is eliminated primarily by glucuronidation in the liver. A study of the pharmacokinetics of raltegravir was performed in subjects with moderate hepatic impairment. Additionally, hepatic impairment was evaluated in the composite pharmacokinetic analysis. There were no clinically important pharmacokinetic differences between subjects with moderate hepatic impairment and healthy subjects. No dosage adjustment is necessary for patients with mild to moderate hepatic impairment. The effect of severe hepatic impairment on the pharmacokinetics of raltegravir has not been studied.

Renal Impairment

Renal clearance of unchanged drug is a minor pathway of elimination. A study of the pharmacokinetics of raltegravir was performed in subjects with severe renal impairment. Additionally, renal impairment was evaluated in the composite pharmacokinetic analysis. There were no clinically important pharmacokinetic differences between subjects with severe renal impairment and healthy subjects. No dosage adjustment is necessary. Because the extent to which ISENTRESS may be dialyzable is unknown, dosing before a dialysis session should be avoided.

UGT1A1 Polymorphism

There is no evidence that common UGT1A1 polymorphisms alter raltegravir pharmacokinetics to a clinically meaningful extent. In a comparison of 30 subjects with *28/*28 genotype (associated with reduced activity of UGT1A1) to 27 subjects with wild-type genotype, the geometric mean ratio (90% CI) of AUC was 1.41 (0.96, 2.09).

Drug Interactions [see Drug Interactions (7)]

 

Table 7: Effect of Other Agents on the Pharmacokinetics of Raltegravir

     

Coadministered
Drug

Coadministered
Drug
Dose/Schedule

Raltegravir
Dose/Schedule

Ratio (90% Confidence Interval) of
Raltegravir Pharmacokinetic
Parameters with/without
Coadministered Drug;
No Effect = 1.00

      n   Cmax   AUC   Cmin
atazanavir 400 mg daily 100 mg single dose 10   1.53   1.72   1.95
(1.11, (1.47, (1.30,
                2.12)   2.02)   2.92)
atazanavir/ritonavir 300 mg/100 mg daily 400 mg twice daily 10 1.24 1.41 1.77
(0.87, (1.12, (1.39,
                1.77)   1.78)   2.25)
efavirenz 600 mg daily 400 mg single dose 9 0.64 0.64 0.79
(0.41, (0.52, (0.49,
                0.98)   0.80)   1.28)
etravirine 200 mg twice daily 400 mg twice daily 19 0.89 0.90 0.66
(0.68, (0.68, (0.34,
                1.15)   1.18)   1.26)
omeprazole 20 mg daily 400 mg single dose 14 4.15 3.12 1.46
(10 for (2.82, (2.13, (1.10,
            AUC)   6.10)   4.56)   1.93)
rifampin 600 mg daily 400 mg single dose 9 0.62 0.60 0.39
(0.37, (0.39, (0.30,
                1.04)   0.91)   0.51)
rifampin 600 mg daily 400 mg twice daily when 14
administered alone; 800 mg 1.62 1.27 0.47
twice daily when (1.12, (0.94, (0.36,
        administered with rifampin       2.33)   1.71)   0.61)
ritonavir 100 mg twice daily 400 mg single dose 10 0.76 0.84 0.99
(0.55, (0.70, (0.70,
                1.04)   1.01)   1.40)
tenofovir 300 mg daily 400 mg twice daily 9 1.64 1.49 1.03
(1.16, (1.15, (0.73,
                2.32)   1.94)   1.45)
tipranavir/ritonavir 500 mg/200 mg twice daily 400 mg twice daily 15 0.82 0.76 0.45
(14 for (0.46, (0.49, (0.31,
            C(min))   1.46)   1.19)   0.66)

12.4 Microbiology

Mechanism of Action

Raltegravir inhibits the catalytic activity of HIV-1 integrase, an HIV-1 encoded enzyme that is required for viral replication. Inhibition of integrase prevents the covalent insertion, or integration, of unintegrated linear HIV-1 DNA into the host cell genome preventing the formation of the HIV-1 provirus. The provirus is required to direct the production of progeny virus, so inhibiting integration prevents propagation of the viral infection. Raltegravir did not significantly inhibit human phosphoryltransferases including DNA polymerases α, β, and γ.

Antiviral Activity in Cell Culture

Raltegravir at concentrations of 31 +/- 20 nM resulted in 95% inhibition (EC95) of viral spread (relative to an untreated virus-infected culture) in human T-lymphoid cell cultures infected with the cell-line adapted HIV-1 variant H9IIIB. In addition, 5 clinical isolates of HIV-1 subtype B had EC95 values ranging from 9 to 19 nM in cultures of mitogen-activated human peripheral blood mononuclear cells. In a single-cycle infection assay, raltegravir inhibited infection of 23 HIV-1 isolates representing 5 non-B subtypes (A, C, D, F, and G) and 5 circulating recombinant forms (AE, AG, BF, BG, and cpx) with EC50 values ranging from 5 to 12 nM. Raltegravir also inhibited replication of an HIV-2 isolate when tested in CEMx174 cells (EC95 value = 6 nM). Additive to synergistic antiretroviral activity was observed when human T-lymphoid cells infected with the H9IIIB variant of HIV-1 were incubated with raltegravir in combination with non-nucleoside reverse transcriptase inhibitors (delavirdine, efavirenz, or nevirapine); nucleoside analog reverse transcriptase inhibitors (abacavir, didanosine, lamivudine, stavudine, tenofovir, zalcitabine, or zidovudine); protease inhibitors (amprenavir, atazanavir, indinavir, lopinavir, nelfinavir, ritonavir, or saquinavir); or the entry inhibitor enfuvirtide.

Resistance

The mutations observed in the HIV-1 integrase coding sequence that contributed to raltegravir resistance (evolved either in cell culture or in subjects treated with raltegravir) generally included an amino acid substitution at either Y143 (changed to C, H, or R) or Q148 (changed to H, K, or R) or N155 (changed to H) plus one or more additional substitutions (i.e., L74M, E92Q, T97A, E138A/K, G140A/S, V151I, G163R, H183P, Y226C/D/F/H, S230R, and D232N).

Treatment-Naïve Subjects: By Week 96 in the STARTMRK trial, the primary raltegravir resistance-associated substitutions were observed in 4 (2 with Y143H/R and 2 with Q148H/R) of the 10 virologic failure subjects with evaluable genotypic data from paired baseline and raltegravir treatment-failure isolates.

Treatment-Experienced Subjects: By Week 96 in the BENCHMRK trials, at least one of the primary raltegravir resistance-associated substitutions, Y143C/H/R, Q148H/K/R, and N155H, was observed in 76 of the 112 virologic failure subjects with evaluable genotypic data from paired baseline and raltegravir treatment-failure isolates. The emergence of the primary raltegravir resistance-associated substitutions was observed cumulatively in 70 subjects by Week 48 and 78 subjects by Week 96, 15.2% and 17% of the raltegravir recipients, respectively. Some (n=58) of those HIV-1 isolates harboring one or more of the primary raltegravir resistance-associated substitutions were evaluated for raltegravir susceptibility yielding a median decrease of 26.3-fold (mean 48.9 ± 44.8-fold decrease, ranging from 0.8- to 159-fold) compared to the wild-type reference.

13 NONCLINICAL TOXICOLOGY

13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility

Carcinogenicity studies of raltegravir in mice did not show any carcinogenic potential. At the highest dose levels, 400 mg/kg/day in females and 250 mg/kg/day in males, systemic exposure was 1.8-fold (females) or 1.2-fold (males) greater than the AUC (54 µM●hr) at the 400-mg twice daily human dose. Treatment-related squamous cell carcinoma of nose/nasopharynx was observed in female rats dosed with 600 mg/kg/day raltegravir for 104 weeks. These tumors were possibly the result of local irritation and inflammation due to local deposition and/or aspiration of drug in the mucosa of the nose/nasopharynx during dosing. No tumors of the nose/nasopharynx were observed in rats dosed with 150 mg/kg/day (males) and 50 mg/kg/day (females) and the systemic exposure in rats was 1.7-fold (males) to 1.4-fold (females) greater than the AUC (54 μM●hr) at the 400-mg twice daily human dose.

No evidence of mutagenicity or genotoxicity was observed in in vitro microbial mutagenesis (Ames) tests, in vitro alkaline elution assays for DNA breakage, and in vitro and in vivo chromosomal aberration studies.

No effect on fertility was seen in male and female rats at doses up to 600 mg/kg/day which resulted in a 3-fold exposure above the exposure at the recommended human dose.

14 CLINICAL STUDIES

Description of Clinical Studies

The evidence of durable efficacy of ISENTRESS is based on the analyses of 96-week data from an ongoing, randomized, double-blind, active-control trial, STARTMRK (Protocol 021) in antiretroviral treatment-naïve HIV-1 infected adult subjects and from 2 ongoing, randomized, double-blind, placebo-controlled studies, BENCHMRK 1 and BENCHMRK 2 (Protocols 018 and 019), in antiretroviral treatment-experienced HIV-1 infected adult subjects.

Treatment-Naïve Subjects

STARTMRK (Protocol 021) is a Phase 3 study to evaluate the safety and antiretroviral activity of ISENTRESS 400 mg twice daily + emtricitabine (+) tenofovir versus efavirenz 600 mg at bedtime plus emtricitabine (+) tenofovir in treatment-naïve HIV-1-infected subjects with HIV-1 RNA >5000 copies/mL. Randomization was stratified by screening HIV-1 RNA level (≤50,000 copies/mL; and >50,000 copies/mL) and by hepatitis status.

Table 8 shows the demographic characteristics of subjects in the group receiving ISENTRESS 400 mg twice daily and subjects in the comparator group.

     

Table 8: Baseline Characteristics

 
Randomized Study ISENTRESS Efavirenz
Protocol 021 400 mg Twice Daily 600 mg At Bedtime
      (N = 281)   (N = 282)
Gender
Male 81% 82%
  Female   19%   18%
Race
White 41% 44%
Black 12% 8%
Asian 13% 11%
Hispanic 21% 24%
Native American <1% <1%
  Multiracial   12%   13%
Region
Latin America 35% 34%
Southeast Asia 12% 10%
North America 29% 32%
  EU/Australia   23%   23%
Age (years)        

18-64

99% 99%
≥65 1% 1%
Mean (SD) 38 (9) 37 (10)
  Median (min, max)   37 (19 to 67)   36 (19 to 71)
CD4+ Cell Count (cells/microL)        
Mean (SD) 219 (124) 217 (134)
  Median (min, max)   212 (1 to 620)   204 (4 to 807)
Plasma HIV-1 RNA (log10 copies/mL)
Mean (SD) 5 (1) 5 (1)
  Median (min, max)   5 (3 to 6)   5 (4 to 6)
Plasma HIV-1 RNA (copies/mL)
Geometric Mean 103205 106215
  Median (min, max)   114000 (400 to 750000)   104000 (4410 to 750000)
History of AIDS*
  Yes   19%   21%
Viral Subtype
Clade B 78% 82%
  Non-Clade B   21%   17%
Baseline Plasma HIV-1 RNA
≤100,000 copies/mL 45% 49%
  >100,000 copies/mL   55%   51%
Baseline CD4+ Cell Counts
≤50 cells/mm3 10% 11%
>50 cells/mm3 and ≤200 cells/mm3 37% 37%
  >200 cells/mm3   53%   51%
Hepatitis Status
  Hepatitis B or C Positive   6%   6%
*Includes additional subjects identified as having a history of AIDS.
(†)Non-Clade B Subtypes (# of subjects): Clade A (4), A/C (1), A/G (2), A1 (1), AE (29), AG (12), BF (6), C (37), D (2), F (2), F1 (5), G (2), Complex (3).
(‡)Evidence of hepatitis B surface antigen or evidence of HCV RNA by polymerase chain reaction (PCR) quantitative test for hepatitis C Virus.
Notes:
ISENTRESS and Efavirenz were administered with emtricitabine (+) tenofovir
N = Number of subjects in each group.
 

Week 96 outcomes from Protocol 021 are shown in Table 9.

     

Table 9: Virologic Outcomes of Randomized Treatment of Protocol 021 at 96 Weeks

 
ISENTRESS Efavirenz Difference
400 mg 600 mg (ISENTRESS – Efavirenz) (CI)
Twice Daily At Bedtime
    (N = 281)   (N = 282)    
 
Subjects with HIV-1 RNA less than 50 copies/mL  

82%

 

78%

  3.8%

(-2.8%, 10.4%)

Virologic Failure*

 

9%

 

10%

   

No virologic data at Week 96

Window

 

Reasons

 
Discontinued study due to AE or death

4%

7%

Discontinued study for other reasons

5%

4%

Missing data during window but on study  

1%

 

1%

 
*Includes subjects who discontinued prior to Week 96 for lack of efficacy, subjects changed OBT due to lack of efficacy prior to Week 96, or subjects who are ≥50 copies in the 96 week window.
Includes subjects who discontinued due to AE or Death at any time point from Day 1 through the Week 96 window if this resulted in no virologic data on treatment during Week 96 visit window.
Other includes: withdrew consent, loss to follow-up, moved etc., if the viral load at the time of discontinuation was <50 copies/mL.
 

The mean changes in CD4 count from baseline were 217 cells/mm3 in the group receiving ISENTRESS 400 mg twice daily and 199 cells/mm3 in the group receiving Efavirenz 600 mg at bedtime.

Treatment-Experienced Subjects

BENCHMRK 1 and BENCHMRK 2 are Phase 3 studies to evaluate the safety and antiretroviral activity of ISENTRESS 400 mg twice daily in combination with an optimized background therapy (OBT), versus OBT alone, in HIV-1-infected subjects, 16 years or older, with documented resistance to at least 1 drug in each of 3 classes (NNRTIs, NRTIs, PIs) of antiretroviral therapies. Randomization was stratified by degree of resistance to PI (1PI vs. >1PI) and the use of enfuvirtide in the OBT. Prior to randomization, OBT was selected by the investigator based on genotypic/phenotypic resistance testing and prior ART history.

Table 10 shows the demographic characteristics of subjects in the group receiving ISENTRESS 400 mg twice daily and subjects in the placebo group.

   

Table 10: Baseline Characteristics

 
ISENTRESS 400 mg Twice
Daily Placebo
Randomized Studies + OBT + OBT
Protocol 018 and 019
    (N = 462)   (N = 237)
Gender        
Male 88% 89%
Female   12%   11%
Race        
White 65% 73%
Black 14% 11%
Asian 3% 3%
Hispanic 11% 8%
Others   6%   5%
Age (years)        
Median (min, max)   45 (16 to 74)   45 (17 to 70)
CD4+ Cell Count        
Median (min, max), cells/mm3

119 (1 to 792)

123 (0 to 759)
≤50 cells/mm3 32% 33%
>50 and ≤200 cells/mm3   37%   36%
Plasma HIV-1 RNA        
Median (min, max), log10 copies/mL 4.8 (2 to 6) 4.7 (2 to 6)
>100,000 copies/mL   36%   33%
History of AIDS        
Yes   92%   91%
Prior Use of ART, Median (1st Quartile, 3rd Quartile)
Years of ART Use 10 (7 to 12) 10 (8 to 12)
Number of ART   12 (9 to 15)   12 (9 to 14)
Hepatitis Co-infection*        
No Hepatitis B or C virus 83% 84%
Hepatitis B virus only 8% 3%
Hepatitis C virus only 8% 12%
Co-infection of Hepatitis B and C virus   1%   1%
Stratum        
Enfuvirtide in OBT 38% 38%
Resistant to ≥2 PI   97%   95%
*Hepatitis B virus surface antigen positive or hepatitis C virus antibody positive.
 

Table 11 compares the characteristics of optimized background therapy at baseline in the group receiving ISENTRESS 400 mg twice daily and subjects in the control group.

   

Table 11: Characteristics of Optimized Background Therapy at Baseline

 
Randomized Studies ISENTRESS 400 mg Twice Placebo + OBT
Protocol 018 and 019 Daily + OBT
    (N = 462)   (N = 237)
Number of ARTs in OBT        
Median (min, max)   4 (1 to 7)   4 (2 to 7)
Number of Active PI in OBT by Phenotypic
Resistance Test*        
0 36% 41%
1 or more   60%   58%
Phenotypic Sensitivity Score (PSS)        
0 15% 18%
1 31% 30%
2 31% 28%
3 or more   18%   20%
Genotypic Sensitivity Score (GSS)        
0 25% 27%
1 38% 40%
2 24% 21%
3 or more   11%   10%

*Darunavir use in OBT in darunavir-naïve subjects was counted as one active PI.

(†)The Phenotypic Sensitivity Score (PSS) and the Genotypic Sensitivity Score (GSS) were defined as the total oral ARTs in OBT to which a subject's viral isolate showed phenotypic sensitivity and genotypic sensitivity, respectively, based upon phenotypic and genotypic resistance tests. Enfuvirtide use in OBT in enfuvirtide-naïve subjects was counted as one active drug in OBT in the GSS and PSS. Similarly, darunavir use in OBT in darunavir-naïve subjects was counted as one active drug in OBT.

 

Week 96 outcomes for the 699 subjects randomized and treated with the recommended dose of ISENTRESS 400 mg twice daily or placebo in the pooled BENCHMRK 1 and 2 studies are shown in Table 12.

   
Table 12: Virologic Outcomes of Randomized Treatment of
Protocols 018 and 019 at 96 Weeks (Pooled Analysis)
 
ISENTRESS Placebo + OBT
400 mg Twice Daily + (N = 237)
OBT
    (N = 462)    
Subjects with HIV-1 RNA less than 50 copies/mL  

55%

 

27%

Virologic Failure*

 

35%

 

66%

No virologic data at Week 96

Window

 

Reasons

Discontinued study due to AE or death

3%

3%

Discontinued study for other reasons

4%

4%

Missing data during window but on study  

4%

 

<1%

*Includes subjects who switched to open-label raltegravir after Week 16 due to the protocol-defined virologic failure, subjects who discontinued prior to Week 96 for lack of efficacy, subjects changed OBT due to lack of efficacy prior to Week 96, or subjects who were ≥50 copies in the 96 week window.

 

Includes subjects who discontinued due to AE or Death at any time point from Day 1 through the Week 96 window if this resulted in no virologic data on treatment during the Week 96 window.
Other includes: withdrew consent, loss to follow-up, moved etc., if the viral load at the time of discontinuation was <50 copies/mL.
 

The mean changes in CD4 count from baseline were 118 cells/mm3 in the group receiving ISENTRESS 400 mg twice daily and 47 cells/mm3 for the control group.

Treatment-emergent CDC Category C events occurred in 4% of the group receiving ISENTRESS 400 mg twice daily and 5% of the control group.

Virologic responses at Week 96 by baseline genotypic and phenotypic sensitivity score are shown in Table 13.

 
Table 13: Virologic Response at 96 Week Window by Baseline
Genotypic/Phenotypic Sensitivity Score
 
Percent with HIV-1 RNA
50 copies/mL
At Week 96
  ISENTRESS     Placebo
400 mg + OBT
Twice Daily + OBT (N=237)
    n   (N = 462)   n    
Phenotypic Sensitivity Score (PSS)*
0 67 43 43 5
1 144 58 71 23
2 142 61 66 32
3 or more 85 48 48 42
Genotypic Sensitivity Score (GSS)*
0 116 39 65 5
1 177 62 95 26
2 111 61 49 53
3 or more   51   49   23   35

*The Phenotypic Sensitivity Score (PSS) and the Genotypic Sensitivity Score (GSS) were defined as the total oral ARTs in OBT to which a subject's viral isolate showed phenotypic sensitivity and genotypic sensitivity, respectively, based upon phenotypic and genotypic resistance tests. Enfuvirtide use in OBT in enfuvirtide-naïve subjects was counted as one active drug in OBT in the GSS and PSS. Similarly, darunavir use in OBT in darunavir-naïve subjects was counted as one active drug in OBT.

 

16 HOW SUPPLIED/STORAGE AND HANDLING

ISENTRESS tablets 400 mg are pink, oval-shaped, film-coated tablets with “227” on one side. They are supplied as follows:

NDC 0006-0227-61 unit-of-use bottles of 60.

No. 3894

Storage and Handling

Store at 20-25°C (68-77°F); excursions permitted to 15-30°C (59-86°F). See USP Controlled Room Temperature.

17 PATIENT COUNSELING INFORMATION

[See FDA-Approved Patient Labeling.]

Patients should be informed that ISENTRESS is not a cure for HIV infection or AIDS. They should also be told that people taking ISENTRESS may still get infections or other conditions common in people with HIV (opportunistic infections). Patients should also be told that it is very important that they stay under a physician's care during treatment with ISENTRESS.

Patients should be informed that ISENTRESS does not reduce the chance of passing HIV to others through sexual contact, sharing needles, or being exposed to blood. Patients should be advised to continue to practice safer sex and to use latex or polyurethane condoms or other barrier methods to lower the chance of sexual contact with any body fluids such as semen, vaginal secretions or blood. Patients should also be advised to never re-use or share needles.

Physicians should instruct their patients that if they miss a dose, they should take it as soon as they remember. If they do not remember until it is time for the next dose, they should be instructed to skip the missed dose and go back to the regular schedule. Patients should not take two tablets of ISENTRESS at the same time.

Physicians should instruct their patients to read the Patient Package Insert before starting ISENTRESS therapy and to reread each time the prescription is renewed. Patients should be instructed to inform their physician or pharmacist if they develop any unusual symptom, or if any known symptom persists or worsens.

Distributed by:

Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc.

Whitehouse Station, NJ 08889, USA

9795112

U.S. Patent Nos. US 7,169,780

1 Registered trademark of Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc. Copyright © 2007, 2009 Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc.

All rights reserved

Patient Information
ISENTRESS® (eye sen tris)
(raltegravir)
Tablets

Read the patient information that comes with ISENTRESS1 before you start taking it and each time you get a refill. There may be new information. This leaflet is a summary of the information for patients. Your doctor or pharmacist can give you additional information. This leaflet does not take the place of talking with your doctor about your medical condition or your treatment.

What is ISENTRESS?

  • ISENTRESS is an anti-HIV (antiretroviral) medicine used for the treatment of HIV. The term HIV stands for Human Immunodeficiency Virus. It is the virus that causes AIDS (Acquired Immune Deficiency Syndrome). ISENTRESS is used along with other anti-HIV medicines. ISENTRESS will NOT cure HIV infection.
  • People taking ISENTRESS may still develop infections, including opportunistic infections or other conditions that happen with HIV infection.
  • Stay under the care of your doctor during treatment with ISENTRESS.
  • The safety and effectiveness of ISENTRESS in children has not been studied.

ISENTRESS must be used with other anti-HIV medicines.

How does ISENTRESS work?

  • ISENTRESS blocks an enzyme which the virus (HIV) needs in order to make more virus. The enzyme that ISENTRESS blocks is called HIV integrase.
  • When used with other anti-HIV medicines, ISENTRESS may do two things:

1. Reduce the amount of HIV in your blood. This is called your "viral load".

2. Increase the number of white blood cells called CD4 (T) cells.

  • ISENTRESS may not have these effects in all patients.

Does ISENTRESS lower the chance of passing HIV to other people?

No. ISENTRESS does not reduce the chance of passing HIV to others through sexual contact, sharing needles, or being exposed to your blood.

  • Continue to practice safer sex.
  • Use latex or polyurethane condoms or other barrier methods to lower the chance of sexual contact with any body fluids. This includes semen from a man, vaginal secretions from a woman, or blood.
  • Never re-use or share needles.

Ask your doctor if you have any questions about safer sex or how to prevent passing HIV to other people.

What should I tell my doctor before and during treatment with ISENTRESS?

Tell your doctor about all of your medical conditions. Include any of the following that applies to you:

  • You have any allergies.
  • You are pregnant or plan to become pregnant.

- ISENTRESS is not recommended for use during pregnancy. ISENTRESS has not been studied in pregnant women. If you take ISENTRESS while you are pregnant, talk to your doctor about how you can be included in the Antiretroviral Pregnancy Registry.

  • You are breast-feeding or plan to breast-feed.

- It is recommended that HIV-infected women should not breast-feed their infants. This is because their babies could be infected with HIV through their breast milk.

- Talk with your doctor about the best way to feed your baby.

Tell your doctor about all the medicines you take. Include the following:

  • prescription medicines, including rifampin (a medicine used to treat some infections such as tuberculosis)
  • non-prescription medicines
  • vitamins
  • herbal supplements

Know the medicines you take.

  • Keep a list of your medicines. Show the list to your doctor and pharmacist when you get a new medicine.

How should I take ISENTRESS?

Take ISENTRESS exactly as your doctor has prescribed. The recommended dose is as follows:

  • Take only one 400-mg tablet at a time.
  • Take it twice a day.
  • Take it by mouth.
  • Take it with or without food.

Do not change your dose or stop taking ISENTRESS or your other anti-HIV medicines without first talking with your doctor.

IMPORTANT: Take ISENTRESS exactly as your doctor prescribed and at the right times of day because if you don't:

  • The amount of virus (HIV) in your blood may increase if the medicine is stopped for even a short period of time.
  • The virus may develop resistance to ISENTRESS and become harder to treat.
  • Your medicines may stop working to fight HIV.
  • The activity of ISENTRESS may be reduced (due to resistance).

If you fail to take ISENTRESS the way you should, here's what to do:

  • If you miss a dose, take it as soon as you remember. If you do not remember until it is time for your next dose, skip the missed dose and go back to your regular schedule. Do NOT take two tablets of ISENTRESS at the same time. In other words, do NOT take a double dose.
  • If you take too much ISENTRESS, call your doctor or local Poison Control Center.

Be sure to keep a supply of your anti-HIV medicines.

  • When your ISENTRESS supply starts to run low, get more from your doctor or pharmacy.
  • Do not wait until your medicine runs out to get more.

What are the possible side effects of ISENTRESS?

When ISENTRESS has been given with other anti-HIV drugs, side effects included:

  • nausea
  • headache
  • tiredness
  • weakness
  • trouble sleeping
  • stomach pain
  • dizziness
  • depression
  • suicidal thoughts and actions

Other side effects include: rash, severe skin reactions, feeling anxious, paranoia, low blood platelet count, diarrhea, liver failure.

A condition called Immune Reconstitution Syndrome can happen in some patients with advanced HIV infection (AIDS) when combination antiretroviral treatment is started. Signs and symptoms of inflammation from opportunistic infections that a person has or had may occur as the medicines work to treat the HIV infection and help to strengthen the immune system. Call your doctor right away if you notice any signs or symptoms of an infection after starting ISENTRESS with other anti-HIV medicines.

Contact your doctor promptly if you experience unexplained muscle pain, tenderness, or weakness while taking ISENTRESS. This is because on rare occasions, muscle problems can be serious and can lead to kidney damage.

Rash occurred more often in patients taking ISENTRESS and darunavir together than with either drug separately, but was generally mild.

Tell your doctor if you have any side effects that bother you.

These are not all the side effects of ISENTRESS. For more information, ask your doctor or pharmacist.

How should I store ISENTRESS?

  • Store ISENTRESS at room temperature (68 to 77°F).
  • Keep ISENTRESS and all medicines out of the reach of children.

General information about the use of ISENTRESS

Medicines are sometimes prescribed for conditions that are not mentioned in patient information leaflets.

  • Do not use ISENTRESS for a condition for which it was not prescribed.
  • Do not give ISENTRESS to other people, even if they have the same symptoms you have. It may harm them.

This leaflet gives you the most important information about ISENTRESS.

  • If you would like to know more, talk with your doctor.
  • You can ask your doctor or pharmacist for additional information about ISENTRESS that is written for health professionals.
  • For more information go to www.ISENTRESS.com or call 1-800-622-4477.

What are the ingredients in ISENTRESS?

Active ingredient: Each film-coated tablet contains 400 mg of raltegravir.

Inactive ingredients: Microcrystalline cellulose, lactose monohydrate, calcium phosphate dibasic anhydrous, hypromellose 2208, poloxamer 407 (contains 0.01% butylated hydroxytoluene as antioxidant), sodium stearyl fumarate, magnesium stearate. In addition, the film coating contains the following inactive ingredients: polyvinyl alcohol, titanium dioxide, polyethylene glycol 3350, talc, red iron oxide and black iron oxide.

Distributed by:
Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc.
Whitehouse Station, NJ 08889, USA
Revised February 2011
9795112

U.S. Patent Nos. US 7,169,780

1 Registered trademark of Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc. Copyright © 2007, 2009 Merck Sharp & Dohme Corp., a subsidiary of Merck & Co., Inc.

All rights reserved

Contacts

Merck & Co., Inc.
Media:
Pamela Eisele, 908-423-5042
Robert Consalvo, 908-423-6595
or
Investors:
Joe Romanelli, 908-423-5088

Contacts

Merck & Co., Inc.
Media:
Pamela Eisele, 908-423-5042
Robert Consalvo, 908-423-6595
or
Investors:
Joe Romanelli, 908-423-5088