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Generic: nevirapine


Boxed Warning

Warning: Life-threatening (including Fatal) Hepatotoxicity And Skin Reactions

HEPATOTOXICITY: Severe, life-threatening, and in some cases fatal hepatotoxicity, particularly in the first 18 weeks, has been reported in patients treated with nevirapine. In some cases, patients presented with non-specific prodromal signs or symptoms of hepatitis and progressed to hepatic failure. These events are often associated with rash. Female gender and higher CD4+ cell counts at initiation of therapy place patients at increased risk; women with CD4+ cell counts greater than 250 cells/mm3, including pregnant women receiving nevirapine in combination with other antiretrovirals for the treatment of HIV-1 infection, are at the greatest risk. However, hepatotoxicity associated with nevirapine use can occur in both genders, all CD4+ cell counts and at any time during treatment. Hepatic failure has also been reported in patients without HIV taking nevirapine for post-exposure prophylaxis (PEP). Use of nevirapine for occupational and non-occupational PEP is contraindicated [see Contraindications (4.2)] . Patients with signs or symptoms of hepatitis, or with increased transaminases combined with rash or other systemic symptoms, must discontinue nevirapine and seek medical evaluation immediately [see Warnings and Precautions (5.1)] . SKIN REACTIONS: Severe, life-threatening skin reactions, including fatal cases, have occurred in patients treated with nevirapine. These have included cases of Stevens-Johnson syndrome, toxic epidermal necrolysis, and hypersensitivity reactions characterized by rash, constitutional findings, and organ dysfunction. Patients developing signs or symptoms of severe skin reactions or hypersensitivity reactions must discontinue nevirapine and seek medical evaluation immediately. Transaminase levels should be checked immediately for all patients who develop a rash in the first 18 weeks of treatment. The 14-day lead-in period with nevirapine 200 mg daily dosing has been observed to decrease the incidence of rash and must be followed [see Warnings and Precautions (5.2)] . MONITORING: Patients must be monitored intensively during the first 18 weeks of therapy with Nevirapine to detect potentially life-threatening hepatotoxicity or skin reactions. Extra vigilance is warranted during the first 6 weeks of therapy, which is the period of greatest risk of these events. Do not restart Nevirapine following severe hepatic, skin or hypersensitivity reactions. In some cases, hepatic injury has progressed despite discontinuation of treatment. WARNING: LIFE-THREATENING (INCLUDING FATAL) HEPATOTOXICITY and SKIN REACTIONS See full prescribing information for complete boxed warning.
  • Fatal and non-fatal hepatotoxicity (5.1)
  • Fatal and non-fatal skin reactions (5.2)
  Discontinue immediately if experiencing:
  • Signs or symptoms of hepatitis (5.1)
  • Increased transaminases combined with rash or other systemic symptoms (5.1)
  • Severe skin or hypersensitivity reactions (5.2)
  • Any rash with systemic symptoms (5.2)
Monitoring during the first 18 weeks of therapy is essential. Extra vigilance is warranted during the first 6 weeks of therapy, which is the period of greatest risk of these events (5) .


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Recent Major Changes Section



Indications and Usage 11/2012 Warnings and Precautions Immune Reconstitution Syndrome ( 5.5 ) 11/2012

Warning: Life-threatening (including Fatal) Hepatotoxicity And Skin Reactions


HEPATOTOXICITY:

Severe, life-threatening, and in some cases fatal hepatotoxicity, particularly in the first 18 weeks, has been reported in patients treated with nevirapine. In some cases, patients presented with non-specific prodromal signs or symptoms of hepatitis and progressed to hepatic failure. These events are often associated with rash. Female gender and higher CD4+ cell counts at initiation of therapy place patients at increased risk; women with CD4+ cell counts greater than 250 cells/mm3, including pregnant women receiving nevirapine in combination with other antiretrovirals for the treatment of HIV-1 infection, are at the greatest risk. However, hepatotoxicity associated with nevirapine use can occur in both genders, all CD4+ cell counts and at any time during treatment. Hepatic failure has also been reported in patients without HIV taking nevirapine for post-exposure prophylaxis (PEP). Use of nevirapine for occupational and non-occupational PEP is contraindicated [see Contraindications (4.2)] . Patients with signs or symptoms of hepatitis, or with increased transaminases combined with rash or other systemic symptoms, must discontinue nevirapine and seek medical evaluation immediately [see Warnings and Precautions (5.1)] .

SKIN REACTIONS:

Severe, life-threatening skin reactions, including fatal cases, have occurred in patients treated with nevirapine. These have included cases of Stevens-Johnson syndrome, toxic epidermal necrolysis, and hypersensitivity reactions characterized by rash, constitutional findings, and organ dysfunction. Patients developing signs or symptoms of severe skin reactions or hypersensitivity reactions must discontinue nevirapine and seek medical evaluation immediately. Transaminase levels should be checked immediately for all patients who develop a rash in the first 18 weeks of treatment. The 14-day lead-in period with nevirapine 200 mg daily dosing has been observed to decrease the incidence of rash and must be followed [see Warnings and Precautions (5.2)] .

MONITORING:

Patients must be monitored intensively during the first 18 weeks of therapy with Nevirapine to detect potentially life-threatening hepatotoxicity or skin reactions. Extra vigilance is warranted during the first 6 weeks of therapy, which is the period of greatest risk of these events. Do not restart Nevirapine following severe hepatic, skin or hypersensitivity reactions. In some cases, hepatic injury has progressed despite discontinuation of treatment.


WARNING: LIFE-THREATENING (INCLUDING FATAL) HEPATOTOXICITY and SKIN REACTIONS

See full prescribing information for complete boxed warning.
  • Fatal and non-fatal hepatotoxicity (5.1)
  • Fatal and non-fatal skin reactions (5.2)

 

Discontinue immediately if experiencing:
  • Signs or symptoms of hepatitis (5.1)
  • Increased transaminases combined with rash or other systemic symptoms (5.1)
  • Severe skin or hypersensitivity reactions (5.2)
  • Any rash with systemic symptoms (5.2)

Monitoring during the first 18 weeks of therapy is essential. Extra vigilance is warranted during the first 6 weeks of therapy, which is the period of greatest risk of these events (5) .

1 Indications And Usage


Nevirapine is indicated for combination antiretroviral treatment of HIV-1 infection in adults and in pediatrics patients 15 days and older [see Clinical Studies (14.1),14.2)] Additional important information regarding the use of nevirapine tablets, USP for the treatment of HIV-1 infection:
  • Based on serious and life-threatening hepatotoxicity observed in controlled and uncontrolled trials, nevirapine tablets, USP should not be initiated in adult females with CD4+ cell counts greater than 250 cells/mm3 or in adult males with CD4+ cell counts greater than 400 cells/mm3 unless the benefit outweighs the risk [see Boxed Warning and Warnings and Precautions (5.1)] .
  • The 14-day lead-in period with nevirapine tablets USP, 200 mg daily dosing must be strictly followed; it has been demonstrated to reduce the frequency of rash [see Dosage and Administration (2.4) and Warnings and Precautions (5.2)] .
  • If rash persists beyond the 14-day lead-in period, do not dose escalate to 200 mg twice daily. The 200 mg once-daily dosing regimen should not be continued beyond 28 days, at which point an alternative regimen should be sought.

  • Nevirapine is an NNRTI indicated for combination antiretroviral treatment of HIV-1 infection (1)

Important Considerations:
  • Initiation of treatment is not recommended in the following populations unless the benefits outweigh the risks (1, 5.1)
    • adult females with CD4 + cell counts >250 cells/mm 3
    • adult males with CD4 + cell counts >400 cells/mm 3
  • The 14-day lead-in period must be strictly followed; it may reduce the frequency of rash (2.4, 5.2)

2 Dosage And Administration


  • Any patient experiencing rash during the 14-day lead-in period should not increase dose until the rash has resolved. The lead-in dosing regimen should not be continued beyond 28 days (2.4)
  • If dosing interrupted for >7 days, restart 14-day lead-in dosing (2.4)

2.1 Adults


The recommended dose for nevirapine is one 200 mg tablet daily for the first 14 days, followed by one 200 mg tablet twice daily, in combination with other antiretroviral agents. The lead-in period has been observed to decrease the incidence of rash. For concomitantly administered antiretroviral therapy, the manufacturer’s recommended dosage and monitoring should be followed.

2.2 Pediatric Patients


The recommended oral dose for pediatric patients 15 days and older is 150 mg/m 2 once daily for 14 days followed by 150 mg/m 2 twice daily thereafter. The total daily dose should not exceed 400 mg for any patient.

2.3 Monitoring of Patients


Intensive clinical and laboratory monitoring, including liver enzyme tests, is essential at baseline and during the first 18 weeks of treatment with Nevirapine. The optimal frequency of monitoring during this period has not been established. Some experts recommend clinical and laboratory monitoring more often than once per month, and in particular, would include monitoring of liver enzyme tests at baseline, prior to dose escalation, and at two weeks post-dose escalation. After the initial 18-week period, frequent clinical and laboratory monitoring should continue throughout Nevirapine treatment [ see Warnings and Precautions (5) ]. In some cases, hepatic injury has progressed despite discontinuation of treatment.

2.4 Dosage Adjustment


Patients with Rash Discontinue nevirapine tablets if a patient experiences severe rash or any rash accompanied by constitutional findings [see Boxed Warning, Warnings and Precautions (5.2), and Patient Counseling Information (17.1)] . Do not increase nevirapine tablets dose if a patient experiences mild to moderate rash without constitutional symptoms during the 14-day lead-in period of 200 mg/day (150 mg/m2/day in pediatric patients) until the rash has resolved [see Warnings and Precautions (5.2) and Patient Counseling Information (17.1)] . The total duration of the once daily lead-in dosing period should not exceed 28 days at which point an alternative regimen should be sought. Patients with Hepatic Events If a clinical (symptomatic) hepatic event occurs, permanently discontinued nevirapine tablets. Do not restart nevirapine tablets after recovery [see Warnings and Precautions (5.1)] . Patients with Dose Interruption For patients who interrupt nevirapine tablets dosing for more than 7 days, restart the recommended dosing, using one 200 mg tablet daily (150 mg/m2/day in pediatric patients) for the first 14 days (lead-in) followed by one 200 mg tablet twice daily (150 mg/m2 twice daily for pediatric patients). Patients with Renal Impairment Patients with CrCL greater than or equal to 20 mL per min do not require an adjustment in nevirapine tablets dosing. The pharmacokinetics of nevirapine have not been evaluated in patients with CrCL less than 20 mL per min. An additional 200 mg dose of nevirapine tablets following each dialysis treatment is indicated in patients requiring dialysis. Nevirapine metabolites may accumulate in patients receiving dialysis; however, the clinical significance of this accumulation is not known [see Clinical Pharmacology (12.3)] .

3 Dosage Forms And Strengths


Tablets: 200 mg, white modified capsule shaped, biconvex tablets. One side is debossed with S on the left side of bisect and G on the right side of bisect and the other side with 1 on the left side of bisect 00 on the right side of bisect.

  • Tablets: 200 mg (3)

4 Contraindications


  • Patients with moderate or severe (Child-Pugh Class B or C, respectively) hepatic impairment (4, 5.1, 8.7)
  • Use as part of occupational and non-occupational post-exposure prophylaxis (PEP) regimens, an unapproved use (4.2, 5.1)

4.1 Hepatic Impairment


Nevirapine is contraindicated in patients with moderate or severe (Child-Pugh Class B or C, respectively) hepatic impairment [see Warnings and Precautions (5.1) and Use in Specific Populations (8.7)].

4.2 Post-Exposure Prophylaxis


Nevirapine is contraindicated for use as part of occupational and non-occupational post-exposure prophylaxis (PEP) regimens [ see Warnings and Precautions (5.1)].

5 Warnings And Precautions


The most serious adverse reactions associated with Nevirapine are hepatitis/hepatic failure, Stevens-Johnson syndrome, toxic epidermal necrolysis, and hypersensitivity reactions. Hepatitis/hepatic failure may be associated with signs of hypersensitivity which can include severe rash or rash accompanied by fever, general malaise, fatigue, muscle or joint aches, bulers, oral lesions, conjunctivitis, facial edema, eosinophilia, granulocytopenia, lymphadenopathy, or renal dysfunction.

The first 18 weeks of therapy with Nevirapine are a critical period during which intensive clinical and laboratory monitoring of patients is required to detect potentially life-threatening hepatic events and skin reactions. The optimal frequency of monitoring during this time period has not been established. Some experts recommend clinical and laboratory monitoring more often than once per month, and in particular, would include monitoring of liver enzyme tests at baseline, prior to dose escalation and at two weeks post-dose escalation. After the initial 18-week period, frequent clinical and laboratory monitoring should continue throughout Nevirapine treatment. In addition, the 14-day lead-in period with Nevirapine 200 mg daily dosing has been demonstrated to reduce the frequency of rash [see Dosage and Administration (2.1)] ..

  • Hepatotoxicity: Fatal and non-fatal hepatotoxicity has been reported. Monitor liver function tests before and during therapy. Permanently discontinue nevirapine if clinical hepatitis or transaminase elevations combined with rash or other systemic symptoms occur. Do not restart nevirapine after recovery. (5.1)
  • Rash: Fatal and non-fatal skin reactions, including Stevens-Johnson syndrome, toxic epidermal necrolysis, and hypersensitivity reactions, have been reported. Permanently discontinue nevirapine if severe skin reactions or hypersensitivity reactions occur. Check transaminase immediately for all patients who develop a rash in the first 18 weeks of treatment. (5.2)
  • Monitor patients for immune reconstitution syndrome and fat redistribution. (5.5, 5.6)

5.1 Hepatotoxicity and Hepatic Impairment


Severe, life-threatening, and in some cases fatal hepatotoxicity, including fulminant and cholestatic hepatitis, hepatic necrosis and hepatic failure, have been reported in patients treated with Nevirapine. In controlled clinical trials, symptomatic hepatic events regardless of severity occurred in 4% (range 0% to 11.0%) of patients who received Nevirapine and 1.2% of patients in control groups.

The risk of symptomatic hepatic events regardless of severity was greatest in the first 6 weeks of therapy. The risk continued to be greater in the Nevirapine groups compared to controls through 18 weeks of treatment. However, hepatic events may occur at any time during treatment. In some cases, patients presented with non-specific, prodromal signs or symptoms of fatigue, malaise, anorexia, nausea, jaundice, liver tenderness or hepatomegaly, with or without initially abnormal serum transaminase levels. Rash was observed in approximately half of the patients with symptomatic hepatic adverse events. Fever and flu-like symptoms accompanied some of these hepatic events. Some events, particularly those with rash and other symptoms, have progressed to hepatic failure with transaminase elevation, with or without hyperbilirubinemia, hepatic encephalopathy, prolonged partial thromboplastin time, or eosinophilia. Rhabdomyolysis has been observed in some patients experiencing skin and/or liver reactions associated with Nevirapine use. Patients with signs or symptoms of hepatitis must be advised to discontinue Nevirapine and immediately seek medical evaluation, which should include liver enzyme tests.

Transaminases should be checked immediately if a patient experiences signs or symptoms suggestive of hepatitis and/or hypersensitivity reaction. Transaminases should also be checked immediately for all patients who develop a rash in the first 18 weeks of treatment. Physicians and patients should be vigilant for the appearance of signs or symptoms of hepatitis, such as fatigue, malaise, anorexia, nausea, jaundice, bilirubinuria, acholic stools, liver tenderness or hepatomegaly. The diagnosis of hepatotoxicity should be considered in this setting, even if transaminases are initially normal or alternative diagnoses are possible [see Boxed Warning, Dosage and Administration (2.3), and Patient Counseling Information (17.1)] .

If clinical hepatitis or transaminase elevations combined with rash or other systemic symptoms occur permanently discontinue nevirapine. Do not restart Nevirapine after recovery. In some cases, hepatic injury progresses despite discontinuation of treatment.

The patients at greatest risk of hepatic events, including potentially fatal events, are women with high CD4 + cell counts. In general, during the first 6 weeks of treatment, women have a three-fold higher risk than men for symptomatic, often rash-associated, hepatic events (5.8% versus 2.2%), and patients with higher CD4 + cell counts at initiation of Nevirapine therapy are at higher risk for symptomatic hepatic events with Nevirapine. In a retrospective review, women with CD4 + cell counts >250 cells/mm 3 had a 12-fold higher risk of symptomatic hepatic adverse events compared to women with CD4 + cell counts <250 cells/mm 3 (11.0% versus 1%). An increased risk was observed in men with CD4 + cell counts >400 cells/mm 3 (6.3% versus 1% for men with CD4 + cell counts <400 cells/mm 3). However, all patients, regardless of gender, CD4 + cell count, or antiretroviral treatment history, should be monitored for hepatotoxicity since symptomatic hepatic adverse events have been reported at all CD4 + cell counts. Co-infection with hepatitis B or C and/or increased transaminase elevations at the start of therapy with Nevirapine are associated with a greater risk of later symptomatic events (6 weeks or more after starting nevirapine) and asymptomatic increases in AST or ALT.

In addition, serious hepatotoxicity (including liver failure requiring transplantation in one instance) has been reported in HIV-1 uninfected individuals receiving multiple doses of Nevirapine in the setting of post-exposure prophylaxis, an unapproved use. Use of nevirapine for occupational and non-occupational PEP is contraindicated [see Contraindications (4.2)].

Increased nevirapine trough concentrations have been observed in some patients with hepatic fibrosis or cirrhosis. Therefore, carefully monitor patients with either hepatic fibrosis or cirrhosis for evidence of drug-induced toxicity. Do not be administered nevirapine to patients with moderate or severe (Child-Pugh Class B or C, respectively) hepatic impairment [see Contraindications (4.1), Use in Specific Populations (8.7), and Clinical Pharmacology (12.3)] .

5.2 Skin Reactions


Severe and life-threatening skin reactions, including fatal cases, have been reported, occurring most frequently during the first 6 weeks of therapy. These have included cases of Stevens-Johnson syndrome, toxic epidermal necrolysis, and hypersensitivity reactions characterized by rash, constitutional findings, and organ dysfunction including hepatic failure. Rhabdomyolysis has been observed in some patients experiencing skin and/or liver reactions associated with Nevirapine use. In controlled clinical trials, Grade 3 and 4 rashes were reported during the first 6 weeks in 2% of Nevirapine recipients compared to less than 1% of placebo subjects.

Patients developing signs or symptoms of severe skin reactions or hypersensitivity reactions (including, but not limited to, severe rash or rash accompanied by fever, general malaise, fatigue, muscle or joint aches, bulers, oral lesions, conjunctivitis, facial edema, and/or hepatitis, eosinophilia, granulocytopenia, lymphadenopathy, and renal dysfunction) must permanently discontinue Nevirapine and seek medical evaluation immediately [see Boxed Warning and Patient Counseling Information (17.1)] . Do not restart Nevirapine following severe skin rash, skin rash combined with increased transaminases or other symptoms, or hypersensitivity reaction.

If patients present with a suspected nevirapine-associated rash, measure transaminases immediately. Permanently discontinue niverapine in patients with rash-associated transaminase elevations see Warnings and Precautions (5.1)] .

Therapy with Nevirapine must be initiated with a 14-day lead-in period of 200 mg/day (150 mg/m 2/day in pediatric patients), which has been shown to reduce the frequency of rash. Discontinue nevirapine if a patient experiences severe rash or any rash accompanied by constitutional findings. Do not increase nevirapine dose to a patient experiencing a mild to moderate rash without constitutional symptoms during the 14-day lead-in period of 200 mg/day (150 mg/m2/day in pediatric patients) until the rash has resolved. The total duration of the once-daily lead-in dosing period must not exceed 28 days at which point an alternative regimen should be sought [see Dosage and Administration (2.4)] . Patients must be monitored closely if isolated rash of any severity occurs. Delay in stopping Nevirapine treatment after the onset of rash may result in a more serious reaction.

Women appear to be at higher risk than men of developing rash with Nevirapine.

In a clinical trial, concomitant prednisone use (40 mg/day for the first 14 days of Nevirapine administration) was associated with an increase in incidence and severity of rash during the first 6 weeks of Nevirapine therapy. Therefore, use of prednisone to prevent nevirapine-associated rash is not recommended.

5.3 Resistance


Nevirapine must not be used as a single agent to treat HIV-1 or added on as a sole agent to a failing regimen. Resistant virus emerges rapidly when nevirapine is administered as monotherapy. The choice of new antiretroviral agents to be used in combination with nevirapine should take into consideration the potential for cross resistance. When discontinuing an antiretroviral regimen containing nevirapine, the long half-life of nevirapine should be taken into account; if antiretrovirals with shorter half-lives than nevirapine are stopped concurrently, low plasma concentrations of nevirapine alone may persist for a week or longer and virus resistance may subsequently develop [see Microbiology (12.4) ].

5.4 Drug Interactions


See Table 3 for ulings of established and potential drug interactions [see Drug Interactions (7)] .

Concomitant use of St. John's Wort ( Hypericum perforatum) or St. John's wort-containing products and nevirapine is not recommended. Co-administration of St. John’s Wort with non-nucleoside reverse transcriptase inhibitors (NNRTIs), including nevirapine, is expected to substantially decrease NNRTI concentrations and may result in sub-optimal levels of nevirapine and lead to loss of virologic response and possible resistance to nevirapine or to the class of NNRTIs. Co-administration of nevirapine and efavirenz is not recommended as this combination has been associated with an increase in adverse reactions and no improvement in efficacy.

5.5 Immune Reconstitution Syndrome


Immune reconstitution syndrome has been reported in patients treated with combination antiretroviral therapy, including Nevirapine. During the initial phase of combination antiretroviral treatment, patients whose immune system responds may develop an inflammatory response to indolent or residual opportunistic infections (such as Mycobacterium avium infection, cytomegalovirus, Pneumocystis jirovecipneumonia (PCP), or tuberculosis), which may necessitate further evaluation and treatment.

5.6 Fat Redistribution


Redistribution/accumulation of body fat including central obesity, dorsocervical fat enlargement (buffalo hump), peripheral wasting, facial wasting, breast enlargement, and "cushingoid appearance" have been observed in patients receiving antiretroviral therapy. The mechanism and long-term consequences of these events are currently unknown. A causal relationship has not been established.

6 Adverse Reactions


  • The most common adverse reaction is rash. In adults the incidence of rash is 14.8% vs 5.9% with placebo, with Grade 3/4 rash occurring in 1.5% of patients (6.1)
  • In pediatric patients the incidence of rash (all causality) was 21% (6.2)

To report SUSPECTED ADVERSE REACTIONS, contact GSMS, Inc. at 1-800-284-8633 or FDA at 1-800-FDA-1088 or www.fda.gov/medwatch.

6.1 Clinical Trial Experience in Adult Patients


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

The most serious adverse reactions associated with nevirapine are hepatitis, hepatic failure, Stevens-Johnson syndrome, toxic epidermal necrolysis, and hypersensitivity reactions. Hepatitis/hepatic failure may be isolated or associated with signs of hypersensitivity which may include severe rash or rash accompanied by fever, general malaise, fatigue, muscle or joint aches, bulers, oral lesions, conjunctivitis, facial edema, eosinophilia, granulocytopenia, lymphadenopathy, or renal dysfunction [see Boxed Warning and Warnings and Precautions (5.1, 5.2)].


Hepatic Reaction

In controlled clinical trials, symptomatic hepatic events regardless of severity occurred in 4% (range 0% to 11.%) of patients who received nevirapine and 1% of patients in control groups. Female gender and higher CD4 + cell counts (>250 cells/mm 3 in women and >400 cells/mm 3 in men) place patients at increased risk of these events see Boxed Warning and Warnings and Precautions (5.1, 5.2)].

Asymptomatic transaminase elevations (AST or ALT >5X ULN) were observed in 6% (range 0% to 9%) of patients who received nevirapine and 5.5% of patients in control groups. Co-infection with hepatitis B or C and/or increased transaminase elevations at the start of therapy with nevirapine are associated with a greater risk of later symptomatic events (6 weeks or more after starting nevirapine) and asymptomatic increases in AST or ALT.

Liver enzyme abnormalities (AST, ALT, GGT) were observed more frequently in patients receiving nevirapine than in controls (see Table 2).


Skin Reaction

The most common clinical toxicity of nevirapine is rash, which can be severe or life-threatening see Boxed Warning and Warnings and Precautions (5.1, 5.2)]. Rash occurs most frequently within the first 6 weeks of therapy. Rashes are usually mild to moderate, maculopapular erythematous cutaneous eruptions, with or without pruritus, located on the trunk, face and extremities. In controlled clinical trials (Trials 1037, 1038, 1046, and 1090), Grade 1 and 2 rashes were reported in 13% of patients receiving nevirapine compared to 6% receiving placebo during the first 6 weeks of therapy. Grade 3 and 4 rashes were reported in 2% of nevirapine recipients compared to less than 1% of subjects receiving placebo. Women tend to be at higher risk for development of nevirapine-associated rash see Boxed Warning and Warnings and Precautions (5.1, 5.2)].

Treatment-related, adverse experiences of moderate or severe intensity observed in greater than 2% of patients receiving Nevirapine in placebo-controlled trials are shown in Table 1.
Table 1 Percentage of Subjects with Moderate or Severe Drug-Related Events in Adult Placebo-Controlled Trials

Trial 1090 1

Trial 1037, 1038, 1046 2

Nevirapine

Placebo

Nevirapine

Placebo

(n=1121)

(n=1128)

(n=253)

(n=203)

Median exposure (weeks)

58

52

28

28

Any adverse event

15%

11%

32%

13%

Rash

5

2

7

2

Nausea

1

1

9

4

Granulocytopenia

2

3

<1

0

Headache

1

<1

4

1

Fatigue

<1

<1

5

4

Diarrhea

<1

1

2

1

Abdominal pain

<1

<1

2

0

Myalgia

<1

0

1

2

1Background therapy included 3TC for all subjects and combinations of NRTIs and PIs. Subjects had CD4 + cell counts less than 200 cell/mm 3.

2Background therapy included ZDV and ZDV=ddI; nevirapine monotherapy was administered in some subjects. Subjects had CD4 + cell count greater than or equal to 200 cells/mm 3.


Laboratory Abnormalities

Liver enzyme test abnormalities (AST, ALT) were observed more frequently in patients receiving nevirapine than in controls (Table 2). Asymptomatic elevations in GGT occur frequently but are not a contraindication to continue nevirapine therapy in the absence of elevations in other liver enzyme tests. Other laboratory abnormalities (bilirubin, anemia, neutropenia, thrombocytopenia) were observed with similar frequencies in clinical trials comparing nevirapine and control regimens (see Table 2).
Table 2 Percentage of Adult Subjects with Laboratory Abnormalities

Trial 1090 1

Trial 1037, 1038, 1046 2

Nevirapine

Placebo

Nevirapine

Placebo

Laboratory Abnormalities

(n=1121)

(n=1128)

(n=253)

(n=203)

Blood Chemistry

SGPT (ALT) >250 U/L

5

4

14

4

SGOT (AST) >250 U/L

4

3

8

2

Bilirubin >2.5 mg/dL

2

2

2

2

Hematology

Hemoglobin <8.0 g/dL

3

4

0

0

Platelets <50,000/mm 3

1

1

<1

2

Neutrophils <750/mm 2

13

14

4

1

1Background therapy included 3TC for all subjects and combinations of NRTIs and PIs. Subjects had CD4 + cell counts less than 200 cell/mm 3.

2Background therapy included ZDV and ZDV=ddI; Nevirapine monotherapy was administered in some subjects. Subjects had CD4 + cell count greater than or equal to 200 cells/mm 3.

6.2 Clinical Trial Experience in Pediatric Patients


Adverse events were assessed in BI Trial 1100.1032 (ACTG 245), a double-blind, placebo-controlled trial of nevirapine (n=305) in which pediatric subjects received combination treatment with nevirapine. In this trial two subjects were reported to experience Stevens-Johnson syndrome or Stevens-Johnson/toxic epidermal necrolysis transition syndrome. Safety was also assessed in trial BI 1100.882 (ACTG 180), an open-label trial of nevirapine (n=37) in which subjects were followed for a mean duration of 33.9 months (range: 6.8 months to 5.3 years, including long-term follow-up in 29 of these subjects in trial BI 1100.892). The most frequently reported adverse events related to nevirapine in pediatric subjects were similar to those observed in adults, with the exception of granulocytopenia, which was more commonly observed in children receiving both zidovudine and nevirapine. Cases of allergic reaction, including one case of anaphylaxis, were also reported.

The safety of nevirapine was also examined in BI Trial 1100.1368, an open-label, randomized clinical trial performed in South Africa in which 123 HIV-1 infected treatment-naĂŻve subjects between 3 months and 16 years of age received combination treatment with nevirapine oral suspension, lamivudine and zidovudine for 48 weeks [see Use In Specific Populations (8.4) and Clinical Pharmacology (12.3)]. Rash (all causality) was reported in 21% of the subjects, 4 (3%) of whom discontinued drug due to rash. All 4 subjects experienced the rash early in the course of therapy (less than 4 weeks) and resolved upon nevirapine discontinuation. Other clinically important adverse events (all causality) include neutropenia (9%), anemia (7%), and hepatotoxicity (2%) [see Use in Specific Populations (8.4)and Clinical Studies (14.2)].

Safety information on use of nevirapine in combination therapy in pediatric subjects 2 weeks to less than 3 months of age was assessed in 36 subjects from the BI 1100.1222 (PACTG 356) trial. No unexpected safety findings were observed although granulocytopenia was reported more frequently in this age group compared to the older pediatric age groups and adults.

6.3 Post-Marketing Experience


In addition to the adverse events identified during clinical trials, the following adverse reactions have been identified during post-approval use of Nevirapine. 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.
  • Body as a Whole: fever, somnolence, drug withdrawal [see Drug Interactions (7)], redistribution/accumulation of body fat [see Warnings and Precautions (5.6)]
  • Gastrointestinal: vomiting
  • Liver and Biliary: jaundice, fulminant and cholestatic hepatitis, hepatic necrosis, hepatic failure
  • Hematology:anemia, eosinophilia, neutropenia
  • Musculoskeletal: arthralgia, rhabdomyolysis associated with skin and/or liver reactions
  • Neurologic: paraesthesia
  • Skin and Appendages: allergic reactions including anaphylaxis, angioedema, bullous eruptions, ulcerative stomatitis and urticaria have all been reported. In addition, hypersensitivity syndrome and hypersensitivity reactions with rash associated with constitutional findings such as fever, bulering, oral lesions, conjunctivitis, facial edema, muscle or joint aches, general malaise, fatigue or significant hepatic abnormalities [see Warnings and Precautions (5.1)] plus one or more of the following: hepatitis, eosinophilia, granulocytopenia, lymphadenopathy and/or renal dysfunction have been reported.

In post-marketing surveillance anemia has been more commonly observed in children although development of anemia due to concomitant medication use cannot be ruled out.

7 Drug Interactions


Nevirapine is principally metabolized by the liver via the cytochrome P450 isoenzymes, 3A and 2B6. Nevirapine is known to be an inducer of these enzymes. As a result, drugs that are metabolized by these enzyme systems may have lower than expected plasma levels when co-administered with nevirapine.

The specific pharmacokinetic changes that occur with co-administration of nevirapine and other drugs are uled in [Clinical Pharmacology (12.3)] , Table 4. Clinical comments about possible dosage modifications based on established drug interactions are uled in Table 3. The data in Tables 3 and 4 are based on the results of drug interaction studies conducted in HIV-1 seropositive subjects unless otherwise indicated. In addition to established drug interactions, there may be potential pharmacokinetic interactions between nevirapine and other drug classes that are metabolized by the cytochrome P450 system. These potential drug interactions are also uled in Table 3. Although specific drug interaction studies in HIV-1 seropositive subjects have not been conducted for some classes of drugs uled in Table 3, additional clinical monitoring may be warranted when co-administering these drugs.

The in vitro interaction between nevirapine and the antithrombotic agent warfarin is complex. As a result, when giving these drugs concomitantly, plasma warfarin levels may change with the potential for increases in coagulation time. When warfarin is co-administered with nevirapine, anticoagulation levels should be monitored frequently.

Table 3 Established and Potential Drug Interactions: Use With Caution, Alteration in Dose or Regimen May Be Needed Due to Drug Interaction Established Drug Interactions: See Clinical Pharmacology (12.3), Table 4 for Magnitude of Interaction.

* The interaction between nevirapine and the drug was evaluated in a clinical study. All other drug interactions shown are predicted.

Drug Name

Effect on Concentration of Nevirapine or Concomitant Drug

Clinical Comment

HIV Antiviral Agents: Protease Inhibitors (PIs)

Atazanavir/Ritonavir*

↓ Atazanavir ↑ Nevirapine

Do not co-administer nevirapine with atazanavir because nevirapine substantially decreases atazanavir exposure and there is a potential risk for nevirapine-associated toxicity due to increased nevirapine exposures.

Fosamprenavir* Fosamprenavir/Ritonavir*

↓Amprenavir ↑Nevirapine ↓Amprenavir ↑Nevirapine

Co-administration of nevirapine and fosamprenavir without ritonavir is not recommended. No dosing adjustments are required when nevirapine is co-administered with 700/100 mg of fosamprenavir/ritonavir twice daily. The combination of nevirapine administered with fosamprenavir/ritonavir once daily has not been studied.

Indinavir*

↓ Indinavir

The appropriate doses of this combination of indinavir and nevirapine with respect to efficacy and safety have not been established.

Lopinavir/Ritonavir*

↓ Lopinavir

Dosing in adult patients: A dose adjustment of lopinavir/ritonavir to 500/125 mg tablets twice daily or 533/133 mg (6.5 mL) oral solution twice daily is recommended when used in combination with nevirapine. Neither lopinavir/ritonavir tablets nor oral solution should be administered once daily in combination with nevirapine. Dosing in pediatric patients: Please refer to the Kaletra® prescribing information for dosing recommendations based on body surface area and body weight. Neither lopinavir/ritonavir tablets nor oral solution should be administered once daily in combination with nevirapine.

Nelfinavir*

↓Nelfinavir M8 Metabolite ↓Nelfinavir Cmin

The appropriate doses of the combination of nevirapine and nelfinavir with respect to safety and efficacy have not been established.

Saquinavir/ritonavir

The interaction between nevirapine and saquinavir/ritonavir has not been evaluated

The appropriate doses of the combination of nevirapine and saquinavir/ritonavir with respect to safety and efficacy have not been established.

HIV Antiviral Agents: Non-Nucleoside Reverse Transcriptase Inhibitors (NNRTIs)

Efavirenz* Delavirdine Etravirine Rilpivirine

↓Efavirenz

The appropriate doses of these combinations with respect to safety and efficacy have not been established. Plasma concentrations may be altered. Nevirapine should not be coadministered with another NNRTI as this combination has not been shown to be beneficial.

Other Agents

Analgesics: Methadone*

↓Methadone

Methadone levels were decreased; increased dosages may be required to prevent symptoms of opiate withdrawal. Methadone-maintained patients beginning nevirapine therapy should be monitored for evidence of withdrawal and methadone dose should be adjusted accordingly.

Antiarrhythmics: Amiodarone, disopyramide, lidocaine

Plasma concentrations may be decreased.

Appropriate doses for this combination have not been established.

Antibiotics: Clarithromycin* Rifabutin* Rifampin*

↓Clarithromycin ↑14-OH clarithromycin ↑Rifabutin ↓ Nevirapine

Clarithromycin exposure was significantly decreased by nevirapine; however, 14-OH metabolite concentrations were increased. Because clarithromycin active metabolite has reduced activity against Mycobacterium aviumintracellulare complex, overall activity against this pathogen may be altered. Alternatives to clarithromycin, such as azithromycin, should be considered. Rifabutin and its metabolite concentrations were moderately increased. Due to high intersubject variability, however, some patients may experience large increases in rifabutin exposure and may be at higher risk for rifabutin toxicity. Therefore, caution should be used in concomitant administration. Nevirapine and rifampin should not be administered concomitantly because decreases in nevirapine plasma concentrations may reduce the efficacy of the drug. Physicians needing to treat patients co-infected with tuberculosis and using a nevirapine-containing regimen may use rifabutin instead.

Anticonvulsants: Carbamazepine, clonazepam, ethosuximide

Plasma concentrations of nevirapine and the anticonvulsant may be decreased.

Use with caution and monitor virologic response and levels of anticonvulsants.

Antifungals: Fluconazole* Ketoconazole* Itraconazole

↑Nevirapine ↓ Ketoconazole ↓ Itraconazole

Because of the risk of increased exposure to nevirapine, caution should be used in concomitant administration, and patients should be monitored closely for nevirapine-associated adverse events. Nevirapine and ketoconazole should not be administered concomitantly because decreases in ketoconazole plasma concentrations may reduce the efficacy of the drug. Nevirapine and itraconazole should not be administered concomitantly due to potential decreases in itraconazole plasma concentrations that may reduce efficacy of the drug.

Antithrombotics: Warfarin

Plasma concentrations may be increased.

Potential effect on anticoagulation. Monitoring of anticoagulation levels is recommended.

Calcium channel blockers: Diltiazem, nifedipine, verapamil

Plasma concentrations may be decreased.

Appropriate doses for these combinations have not been established.

Cancer chemotherapy: Cyclophosphamide

Plasma concentrations may be decreased.

Appropriate doses for this combination have not been established.

Ergot alkaloids: Ergotamine

Plasma concentrations may be decreased.

Appropriate doses for this combination have not been established.

Immunosuppressants: Cyclosporine, tacrolimus, sirolimus

Plasma concentrations may be decreased.

Appropriate doses for these combinations have not been established.

Motility agents: Cisapride

Plasma concentrations may be decreased.

Appropriate doses for this combination have not been established.

Opiate agonists: Fentanyl

Plasma concentrations may be decreased.

Appropriate doses for this combination have not been established.

Oral contraceptives: Ethinyl estradiol and Norethindrone*

↓ Ethinyl estradiol ↓ Norethindrone

Oral contraceptives and other hormonal methods of birth control should not be used as the sole method of contraception in women taking nevirapine, since nevirapine may lower the plasma levels of these medications. An alternative or additional method of contraception is recommended.

* The interaction between nevirapine and the drug was evaluated in a clinical study. All other drug interations shown are predicted.


Co-administration of Nevirapine can alter the concentrations of other drugs and other drugs may alter the concentration of nevirapine. The potential for drug interactions must be considered prior to and during therapy (5.4, 7, 12.3)

8 Use In Specific Populations


  • Monitor patients with hepatic fibrosis or cirrhosis carefully for evidence of drug induced toxicity. Do not administer neveriapine to patients with Child-Pugh B or C. (5.1, 8.7)
  • No dose adjustment is required for patients with renal impairment with a creatinine clearance greater than or equal to 20 mL per min. Patients on dialysis receive an additional dose of 200 mg following each dialysis treatment (2.4, 8.6)

8.1 Pregnancy

Teratogenic Effects, Pregnancy Category B

There are no adequate and well-controlled trials of nevirapine in pregnant women. The Antiretroviral Pregnancy Registry, which has been surveying pregnancy outcomes since January 1989, has not found an increased risk of birth defects following first trimester exposures to nevirapine. The prevalence of birth defects after any trimester exposure to nevirapine is comparable to the prevalence observed in the general population. Severe hepatic events, including fatalities, have been reported in pregnant women receiving chronic nevirapine therapy as part of combination treatment of HIV-1 infection. Regardless of pregnancy status, women with CD4+ cell counts greater than 250 cells/mm3 should not initiate nevirapine unless the benefit outweighs the risk. It is unclear if pregnancy augments the risk observed in non-pregnant women [see Boxed Warning] . Nevirapine should be used during pregnancy only if the potential benefit justifies the potential risk to the fetus. Antiretroviral Pregnancy Registry To monitor maternal-fetal outcomes of pregnant women exposed to nevirapine, an Antiretroviral Pregnancy Registry has been established. Physicians are encouraged to register patients by calling (800) 258-4263. Animal Data No observable teratogenicity was detected in reproductive studies performed in pregnant rats and rabbits. The maternal and developmental no-observable-effect level dosages produced systemic exposures approximately equivalent to or approximately 50% higher in rats and rabbits, respectively, than those seen at the recommended daily human dose (based on AUC). In rats, decreased fetal body weights were observed due to administration of a maternally toxic dose (exposures approximately 50% higher than that seen at the recommended human clinical dose).

8.3 Nursing Mothers


The Centers for Disease Control and Prevention recommend that HIV-1 infected mothers not breastfeed their infants to avoid risking postnatal transmission of HIV-1. Nevirapine is excreted in breast milk. Because of both the potential for HIV-1 transmission and the potential for serious adverse reactions in nursing infants, mothers should be instructed not to breastfeed if they are receiving nevirapine.

8.4 Pediatric Use


The safety, pharmacokinetic profile, and virologic and immunologic responses of nevirapine have been evaluated in HIV-1 infected pediatric subjects age 3 months to 18 years [see Adverse Reactions (6.2) and Clinical Studies (14.2)] . The safety and pharmacokinetic profile of nevirapine has been evaluated in HIV-1 infected pediatric subjects age 15 days to less than 3 months [see Adverse Reactions (6.2) and Clinical Studies (14.2)] . The most frequently reported adverse events related to nevirapine in pediatric subjects were similar to those observed in adults, with the exception of granulocytopenia, which was more commonly observed in children receiving both zidovudine and nevirapine [see Adverse Reactions (6.2) and Clinical Studies (14.2)] .

8.5 Geriatric Use


Clinical studies of Nevirapine did not include sufficient numbers of subjects aged 65 and older to determine whether elderly subjects respond differently from 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 Renal Impairment


In subjects with renal impairment (mild, moderate or severe), there were no significant changes in the pharmacokinetics of nevirapine. Nevirapine is extensively metabolized by the liver and nevirapine metabolites are extensively eliminated by the kidney. Nevirapine metabolites may accumulate in patients receiving dialysis; however, the clinical significance of this accumulation is not known. No adjustment in nevirapine dosing is required in patients with CrCL greater than or equal to 20 mL/min. In patients undergoing chronic hemodialysis, an additional 200 mg dose following each dialysis treatment is indicated [see Dosage and Administration (2.4) and Clinical Pharmacology (12.3)].

8.7 Hepatic Impairment


Because increased nevirapine levels and nevirapine accumulation may be observed in patients with serious liver disease, do not administer Nevirapine to patients with moderate or severe (Child-Pugh Class B or C, respectively) hepatic impairment [see Contraindications (4.1), Warnings and Precautions (5.1), and Clinical Pharmacology (12.3)] .

10 Overdosage


There is no known antidote for nevirapine overdosage. Cases of nevirapine overdose at doses ranging from 800 to 1800 mg per day for up to 15 days have been reported. Patients have experienced events including edema, erythema nodosum, fatigue, fever, headache, insomnia, nausea, pulmonary infiltrates, rash, vertigo, vomiting and weight decrease. All events subsided following discontinuation of nevirapine.

11 Description


Nevirapine is a non-nucleoside reverse transcriptase inhibitor (NNRTI) with activity against Human Immunodeficiency Virus Type 1 (HIV-1). Nevirapine is structurally a member of the dipyridodiazepinone chemical class of compounds.

The chemical name of nevirapine is 11-cyclopropyl-5,11-dihydro-4-methyl-6H-dipyrido [3,2-b:2’,3’-e][1,4] diazepin-6-one. Nevirapine is a white to off-white crystalline powder with the molecular weight of 266.30 and the molecular formula C15H14N4O. Nevirapine has the following structural formula:

Nevirapine Tablets are for oral administration. Each tablet contains 200 mg of nevirapine and the inactive ingredients microcrystalline cellulose, lactose monohydrate, povidone, sodium starch glycolate, colloidal silicon dioxide and magnesium stearate.

Nevirapine Oral Suspension is for oral administration. Each 5 mL of Nevirapine suspension contains 50 mg of nevirapine (as nevirapine hemihydrate). The suspension also contains the following excipients: carbomer 934P, methylparaben, propylparaben, sorbitol, sucrose, polysorbate 80, sodium hydroxide and purified water.

12 Clinical Pharmacology


12.1 Mechanism of Action


Nevirapine is an antiviral drug [see Microbiology (12.4)] .

12.3 Pharmacokinetics


Adults


Absorption and Bioavailability

Nevirapine is readily absorbed (>90%) after oral administration in healthy volunteers and in adults with HIV-1 infection. Absolute bioavailability in 12 healthy adults following single-dose administration was 93 ± 9% (mean ± SD) for a 50 mg tablet and 91 ± 8% for an oral solution. Peak plasma nevirapine concentrations of 2 ± 0.4 μg/mL (7.5 μM) were attained by 4 hours following a single 200 mg dose. Following multiple doses, nevirapine peak concentrations appear to increase linearly in the dose range of 200 to 400 mg/day. Steady-state trough nevirapine concentrations of 4.5 ± 1.9 μg/mL (17 ± 7 μM), (n = 242) were attained at 400 mg/day. Nevirapine tablets and suspension have been shown to be comparably bioavailable and interchangeable at doses up to 200 mg. When nevirapine (200 mg) was administered to 24 healthy adults (12 female, 12 male), with either a high-fat breakfast (857 kcal, 50 g fat, 53% of calories from fat) or antacid (Maalox ® 30 mL), the extent of nevirapine absorption (AUC) was comparable to that observed under fasting conditions. In a separate study in HIV-1 infected patients (n=6), nevirapine steady-state systemic exposure (AUC τ) was not significantly altered by didanosine, which is formulated with an alkaline buffering agent. Nevirapine may be administered with or without food, antacid or didanosine.


Distribution

Nevirapine is highly lipophilic and is essentially nonionized at physiologic pH. Following intravenous administration to healthy adults, the apparent volume of distribution (Vdss) of nevirapine was 1.21 ± 0.09 L/kg, suggesting that nevirapine is widely distributed in humans. Nevirapine readily crosses the placenta and is also found in breast milk [ see Use in Specific Populations (8.3)] . Nevirapine is about 60% bound to plasma proteins in the plasma concentration range of 1-10 μg/mL. Nevirapine concentrations in human cerebrospinal fluid (n=6) were 45% (±5%) of the concentrations in plasma; this ratio is approximately equal to the fraction not bound to plasma protein.


Metabolism/Elimination

In vivo studies in humans and in vitro studies with human liver microsomes have shown that nevirapine is extensively biotransformed via cytochrome P450 (oxidative) metabolism to several hydroxylated metabolites. In vitro studies with human liver microsomes suggest that oxidative metabolism of nevirapine is mediated primarily by cytochrome P450 (CYP) isozymes from the CYP3A and CYP2B6 families, although other isozymes may have a secondary role. In a mass balance/excretion study in eight healthy male volunteers dosed to steady state with nevirapine 200 mg given twice daily followed by a single 50 mg dose of 14C-nevirapine, approximately 91.4 ± 10.5% of the radiolabeled dose was recovered, with urine (81.3 ± 11.1%) representing the primary route of excretion compared to feces (10.1 ± 1.5%). Greater than 80% of the radioactivity in urine was made up of glucuronide conjugates of hydroxylated metabolites. Thus cytochrome P450 metabolism, glucuronide conjugation, and urinary excretion of glucuronidated metabolites represent the primary route of nevirapine biotransformation and elimination in humans. Only a small fraction (<5%) of the radioactivity in urine (representing <3% of the total dose) was made up of parent compound; therefore, renal excretion plays a minor role in elimination of the parent compound.

Nevirapine is an inducer of hepatic cytochrome P450 (CYP) metabolic enzymes 3A and 2B6. Nevirapine induces CYP3A and CYP2B6 by approximately 20-25%, as indicated by erythromycin breath test results and urine metabolites. Autoinduction of CYP3A and CYP2B6 mediated metabolism leads to an approximately 1.5- to 2-fold increase in the apparent oral clearance of nevirapine as treatment continues from a single dose to two-to-four weeks of dosing with 200-400 mg/day. Autoinduction also results in a corresponding decrease in the terminal phase half-life of nevirapine in plasma, from approximately 45 hours (single dose) to approximately 25-30 hours following multiple dosing with 200-400 mg/day.

Specific Populations


Renal Impairment

HIV-1 seronegative adults with mild (CrCL 50-79 mL/min; n=7), moderate (CrCL 30-49 mL/min; n=6), or severe (CrCL <30 mL/min; n=4) renal impairment received a single 200 mg dose of nevirapine in a pharmacokinetic study. These subjects did not require dialysis. The study included six additional subjects with renal failure requiring dialysis.

In subjects with renal impairment (mild, moderate or severe), there were no significant changes in the pharmacokinetics of nevirapine. However, subjects requiring dialysis exhibited a 44% reduction in nevirapine AUC over a one-week exposure period. There was also evidence of accumulation of nevirapine hydroxy-metabolites in plasma in subjects requiring dialysis. An additional 200 mg dose following each dialysis treatment is indicated [see Dosage and Administration (2.4) and Use in Specific Populations (8.6)] .


Hepatic Impairment

In a steady-state study comparing 46 patients with mild (n=17; expansion of some portal areas; Ishak Score 1-2), moderate (n=20; expansion of most portal areas with occasional portal-to-portal and portal-to-central bridging; Ishak Score 3-4), or severe (n=9; marked bridging with occasional cirrhosis without decompensation indicating Child-Pugh A; Ishak Score 5-6) fibrosis as a measure of hepatic impairment, the multiple dose pharmacokinetic disposition of nevirapine and its five oxidative metabolites were not altered. However, approximately 15% of these patients with hepatic fibrosis had nevirapine trough concentrations above 9,000 ÎĽg/mL (2-fold the usual mean trough). Therefore, patients with hepatic impairment should be monitored carefully for evidence of drug-induced toxicity [see Warnings and Precautions (5.1)] . The patients studied were receiving antiretroviral therapy containing nevirapine 200 mg twice daily for at least 6 weeks prior to pharmacokinetic sampling, with a median duration of therapy of 3.4 years.

In a pharmacokinetic study where HIV-1 negative cirrhotic patients with mild (Child-Pugh A; n=6) or moderate (Child-Pugh B; n=4) hepatic impairment received a single 200 mg dose of nevirapine, a significant increase in the AUC of nevirapine was observed in one patient with Child-Pugh B and ascites suggesting that patients with worsening hepatic function and ascites may be at risk of accumulating nevirapine in the systemic circulation. Because nevirapine induces its own metabolism with multiple dosing, this single-dose study may not reflect the impact of hepatic impairment on multiple-dose pharmacokinetics.

Do not administer nevirapine to patients with moderate or severe (Child-Pugh Class B or C, respectively) hepatic impairment see Contraindications (4), Warnings and Precautions (5.1), and Use in Specific Populations (8.7)] .


Gender

In the multinational 2NN study, a population pharmacokinetic substudy of 1077 patients was performed that included 391 females. Female patients showed a 13.8% lower clearance of nevirapine than did men. Since neither body weight nor Body Mass Index (BMI) had an influence on the clearance of nevirapine, the effect of gender cannot solely be explained by body size.


Race

An evaluation of nevirapine plasma concentrations (pooled data from several clinical trials) from HIV-1-infected patients (27 Black, 24 Hispanic, 189 Caucasian) revealed no marked difference in nevirapine steady-state trough concentrations (median C minss = 4.7 ÎĽg/mL Black, 3.8 ÎĽg/mL Hispanic, 4.3 ÎĽg/mL Caucasian) with long-term nevirapine treatment at 400 mg/day. However, the pharmacokinetics of nevirapine have not been evaluated specifically for the effects of ethnicity.

Black subjects (n=80/group) in Trial 1100.1486 showed approximately 30% to 35% higher trough concentrations than Caucasian subjects (250 to 325 subjects/group) in both immediate-release nevirapine and nevirapine extended-release treatment groups over 96 weeks of treatment at 400 mg per day.


Geriatric Patients

Nevirapine pharmacokinetics in HIV-1-infected adults do not appear to change with age (range 18–68 years); however, nevirapine has not been extensively evaluated in patients beyond the age of 55 years [see Use in Specific Populations (8.5)] .


Pediatric Patients

Pharmacokinetic data for nevirapine have been derived from two sources: a 48-week pediatric trial in South Africa (BI Trial 1100.1368) involving 123 HIV-1 positive, antiretroviral-naĂŻve patients aged 3 months to 16 years; and a consolidated analysis of five Pediatric AIDS Clinical Trials Group (PACTG) protocols comprising 495 patients aged 14 days to 19 years.

BI Trial 1100.1368 studied the safety, efficacy, and pharmacokinetics of a weight-based and a body surface area (BSA)-based dosing regimen of nevirapine. In the weight-based regimen, pediatric patients up to 8 years of age received a dose of 4 mg/kg once daily for two weeks followed by 7 mg/kg twice daily thereafter. Patients 8 years and older were dosed 4 mg/kg once daily for two weeks followed by 4 mg/kg twice daily thereafter. In the BSA regimen, all pediatric patients received 150 mg/m 2 once daily for two weeks followed by 150 mg/m 2 twice daily thereafter [see Use in Specific Populations (8.4) and Adverse Reactions (6.2)] . Dosing of nevirapine at 150 mg/m 2 BID (after a two-week lead-in of 150 mg/m 2 QD) produced geometric mean or mean trough nevirapine concentrations between 4-6 ÎĽg/mL (as targeted from adult data). In addition, the observed trough nevirapine concentrations were comparable between the two dosing regimens studied (BSA- and weight-based methods).

The consolidated analysis of Pediatric AIDS Clinical Trials Group (PACTG) protocols 245, 356, 366, 377, and 403 allowed for the evaluation of pediatric patients less than 3 months of age (n=17). The plasma nevirapine concentrations observed were within the range observed in adults and the remainder of the pediatric population, but were more variable between patients, particularly in the second month of age. For dose recommendations for pediatric patients see Dosage and Administration (2.2)].


Drug Interactions [see Drug Interactions (7)]

Nevirapine induces hepatic cytochrome P450 metabolic isoenzymes 3A and 2B6. Co-administration of Nevirapine and drugs primarily metabolized by CYP3A or CYP2B6 may result in decreased plasma concentrations of these drugs and attenuate their therapeutic effects.

While primarily an inducer of cytochrome P450 3A and 2B6 enzymes, nevirapine may also inhibit this system. Among human hepatic cytochrome P450s, nevirapine was capable in vitro of inhibiting the 10-hydroxylation of (R)-warfarin (CYP3A). The estimated K i for the inhibition of CYP3A was 270 ÎĽM, a concentration that is unlikely to be achieved in patients as the therapeutic range is <25 ÎĽM. Therefore, nevirapine may have minimal inhibitory effect on other substrates of CYP3A.

Nevirapine does not appear to affect the plasma concentrations of drugs that are substrates of other CYP450 enzyme systems, such as 1A2, 2D6, 2A6, 2E1, 2C9 or 2C19.

Table 4 (see below) contains the results of drug interaction studies performed with Nevirapine and other drugs likely to be co-administered. The effects of Nevirapine on the AUC, C max, and C min of co-administered drugs are summarized.

Table 4 Drug Interactions: Changes in Pharmacokinetic Parameters for Co-administered Drug in the Presence of Nevirapine (All interaction trials were conducted in HIV-1 positive subjects)

Co-administered Drug

Dose of Co-administered Drug

Dose Regimen of Nevirapine

n

% Change of Co-administered Drug Pharmacokinetic Parameters (90% CI)

Antiretrovirals

AUC

Cmax

Cmin

Atazanavir/ Ritonavira, d

300/100 mg QD day 4 to 13, then 400/100 mg QD, day 14 to 23

200 mg BID day 1 to 23. Subjects were treated with nevirapine prior to trial entry.

23

Atazanavir 300/100 mg ↓42 (↓52 to ↓29)

Atazanavir 300/100 mg ↓28 (↓40 to ↓14)

Atazanavir 300/100 mg ↓72 (↓80 to ↓60)

Atazanavir 400/100 mg ↓19 (↓35 to ↑2)

Atazanavir 400/100 mg ↑2 (↓15 to ↑24)

Atazanavir 400/100 mg ↓59 (↓73 to ↓40)

Darunavir/ Ritonavire

400/100 mg BID

200 mg BID

8

↑24 (↓3 to ↑57)

↑40 (↑14 to ↑73)

↑2 (↓21 to ↑32)

Didanosine

100 to 150 mg BID

200 mg QD x 14 days; 200 mg BID x 14 days

18

#

#

§

Efavirenza

600 mg QD

200 mg QD x 14 days; 400 mg QD x 14 days

17

↓28 (↓34 to ↓14)

↓12 (↓23 to ↑1)

↓32 (↓35 to ↓19)

Fosamprenavir

1400 mg BID

200 mg BID. Subjects were treated with nevirapine prior to trial entry.

17

↓33 (↓45 to ↓20)

↓25 (↓37 to ↓10)

↓35 (↓50 to ↓15)

Fosamprenavir/ Ritonavir

700/100 mg BID

200 mg BID. Subjects were treated with nevirapine prior to trial entry

17

↓11 (↓23 to ↑3)

#

↓19 (↓32 to ↓4)

Indinavira

800 mg q 8 H

200 mg QD x 14 days; 200 mg BID x 14 days

19

↓31 (↓39 to ↓22)

↓15 (↓24 to ↓4)

↓44 (↓53 to ↓33)

Lopinavira, b

300/75 mg/m2 (lopinavir/ ritonavir)b

7 mg/kg or 4 mg/kg QD x 2 weeks; BID x 1 week

12, 15c

↓22 (↓44 to ↑9)

↓14 (↓36 to ↑16)

↓55 (↓75 to ↓19)

Lopinavira

400/100 mg BID (lopinavir/ ritonavir)

200 mg QD x 14 days; 200 mg BID >1 year

22, 19c

↓27 (↓47 to ↓2)

↓19 (↓38 to ↑5)

↓51 (↓72 to ↓26)

Maravirocf

300 mg SD

200 mg BID

8

↑1 (↓35 to ↑55)

↑54 (↓6 to ↑151)

#

Nelfinavira Nelfinavir-M8 metabolite

750 mg TID

200 mg QD x 14 days; 200 mg BID x 14 days

23

#

#

↓32 (↓50 to ↑5)

↓62 (↓70 to ↓53)

↓59 (↓68 to ↓48)

↓66 (↓74 to ↓55)

Ritonavir

600 mg BID

200 mg QD x 14 days; 200 mg BID x 14 days

18

#

#

#

Stavudine

30 to 40 mg BID

200 mg QD x 14 days; 200 mg BID x 14 days

22

#

#

§

Zalcitabine

0.125 to 0.25 mg TID

200 mg QD x 14 days; 200 mg BID x 14 days

6

#

#

§

Zidovudine

100 to 200 mg TID

200 mg QD x 14 days; 200 mg BID x 14 days

11

↓28 (↓40 to ↓4)

↓30 (↓51 to ↑14)

§

Other Medications

AUC

Cmax

Cmin

Clarithromycina Metabolite 14-OH-clarithromycin

500 mg BID

200 mg QD x 14 days; 200 mg BID x 14 days

15

↓31 (↓38 to ↓24)

↓23 (↓31 to ↓14)

↓56 (↓70 to ↓36)

↑42 (↑16 to ↑73)

↑47 (↑21 to ↑80)

#

Ethinyl estradiola and Norethindronea

0.035 mg (as Ortho-Novum® 1/35) 1 mg (as Ortho-Novum® 1/35)

200 mg QD x 14 days; 200 mg BID x 14 days

10

↓20 (↓33 to ↓3)

#

§

↓19 (↓30 to ↓7)

↓16 (↓27 to ↓3)

§

Depomedroxy- progesterone acetate

150 mg every 3 months

200 mg QD x 14 days; 200 mg BID x 14 days

32

#

#

#

Fluconazole

200 mg QD

200 mg QD x 14 days; 200 mg BID x 14 days

19

#

#

#

Ketoconazolea

400 mg QD

200 mg QD x 14 days; 200 mg BID x 14 days

21

↓72 (↓80 to ↓60)

↓44 (↓58 to ↓27)

§

Methadonea

Individual Subject Dosing

200 mg QD x 14 days; 200 mg BID ≥7 days

9

In a controlled pharmacokinetic trial with 9 subjects receiving chronic methadone to whom steady-state nevirapine therapy was added, the clearance of methadone was increased by 3-fold, resulting in symptoms of withdrawal, requiring dose adjustments in 10 mg segments, in 7 of the 9 subjects. Methadone did not have any effect on nevirapine clearance.

Rifabutina Metabolite 25-O-desacetyl-rifabutin

150 or 300 mg QD

200 mg QD x 14 days; 200 mg BID x 14 days

19

↑17 (↓2 to ↑40)

↑28 (↑9 to ↑51)

#

↑24 (↓16 to ↑84)

↑29 (↓2 to ↑68)

↑22 (↓14 to ↑74)

Rifampina

600 mg QD

200 mg QD x 14 days; 200 mg BID x 14 days

14

↑11 (�4 to ↑28)

#

§

§ = Cmin below detectable level of the assay ↑ = Increase, ↓ = Decrease, # = No Effect a For information regarding clinical recommendations, see Drug Interactions (7). b Pediatric subjects ranging in age from 6 months to 12 years. c Parallel group design; n for nevirapine+lopinavir/ritonavir, n for lopinavir/ritonavir alone. d Parallel group design; n=23 for atazanavir/ritonavir + nevirapine, n=22 for atazanavir/ritonavir without nevirapine. Changes in atazanavir PK are relative to atazanavir/ritonavir 300/100 mg alone. e Based on between-trial comparison. f Based on historical controls

Because of the design of the drug interaction trials (addition of 28 days of Nevirapine therapy to existing HIV-1 therapy), the effect of the concomitant drug on plasma nevirapine steady-state concentrations was estimated by comparison to historical controls.

Administration of rifampin had a clinically significant effect on nevirapine pharmacokinetics, decreasing AUC and C max by greater than 50%. Administration of fluconazole resulted in an approximate 100% increase in nevirapine exposure, based on a comparison to historic data Drug Interactions (7) . The effect of other drugs uled in Table 4 on nevirapine pharmacokinetics was not significant. No significant interaction was observed when tipranavir was co-administered with low-dose ritonavir and nevirapine.

12.4 Microbiology


Mechanism of Action


Nevirapine is a non-nucleoside reverse transcriptase inhibitor (NNRTI) of HIV-1. Nevirapine binds directly to reverse transcriptase (RT) and blocks the RNA-dependent and DNA-dependent DNA polymerase activities by causing a disruption of the enzyme's catalytic site. The activity of nevirapine does not compete with template or nucleoside triphosphates. HIV-2 RT and eukaryotic DNA polymerases (such as human DNA polymerases α, β, γ, or δ) are not inhibited by nevirapine.

Antiviral Activity


The antiviral activity of nevirapine has been measured in a variety of cell lines including peripheral blood mononuclear cells, monocyte-derived macrophages, and lymphoblastoid cell lines. In an assay using human embryonic kidney 293 cells, the median EC 50 value (50% inhibitory concentration) of nevirapine was 90 nM against a panel of 2923 isolates of HIV-1 that were primarily (93%) clade B clinical isolates from the United States. The 99 th percentile EC 50 value was 470 nM in this study. The median EC 50 value was 63 nM (range 14-302 nM, n=29) against clinical isolates of HIV-1 clades A, B, C, D, F, G, and H, and circulating recombinant forms CRF01_AE, CRF02_AG and CRF12_BF. Nevirapine had no antiviral activity in cell culture against group O HIV-1 isolates (n=3) or HIV-2 isolates (n=3) replicating in cord blood mononuclear cells. Nevirapine in combination with efavirenz exhibited strong antagonistic anti-HIV-1 activity in cell culture and was additive to antagonistic with the protease inhibitor ritonavir or the fusion inhibitor enfuvirtide. Nevirapine exhibited additive to synergistic anti-HIV-1 activity in combination with the protease inhibitors amprenavir, atazanavir, indinavir, lopinavir, nelfinavir, saquinavir and tipranavir, and the NRTIs abacavir, didanosine, emtricitabine, lamivudine, stavudine, tenofovir and zidovudine. The anti-HIV-1 activity of nevirapine was antagonized by the anti-HBV drug adefovir and by the anti-HCV drug ribavirin in cell culture.

Resistance


HIV-1 isolates with reduced susceptibility (100- to 250-fold) to nevirapine emerge in cell culture. Genotypic analysis showed mutations in the HIV-1 RT gene encoding Y181C and/or V106A substitutions depending upon the virus strain and cell line employed. Time to emergence of nevirapine resistance in cell culture was not altered when selection included nevirapine in combination with several other NNRTIs.

Phenotypic and genotypic changes in HIV-1 isolates from treatment-naïve patients receiving either nevirapine (n=24) or nevirapine and ZDV (n=14) were monitored in Phase 1 and 2 trials over 1 to ≥12 weeks. After 1 week of nevirapine monotherapy, isolates from 3/3 patients had decreased susceptibility to nevirapine in cell culture. One or more of the RT mutations resulting in amino acid substitutions K103N, V106A, V108I, Y181C, Y188C and G190A were detected in HIV-1 isolates from some patients as early as 2 weeks after therapy initiation. By week eight of nevirapine monotherapy, 100% of the patients tested (n=24) had HIV-1 isolates with a >100-fold decrease in susceptibility to nevirapine in cell culture compared to baseline, and had one or more of the nevirapine-associated RT resistance substitutions. Nineteen of these patients (80%) had isolates with Y181C substitutions regardless of dose.

Genotypic analysis of isolates from antiretroviral-naĂŻve patients experiencing virologic failure (n=71) receiving nevirapine once daily (n=25) or twice daily (n=46) in combination with lamivudine and stavudine (study 2NN) for 48 weeks showed that isolates from 8/25 and 23/46 patients, respectively, contained one or more of the following NNRTI resistance-associated substitutions: Y181C, K101E, G190A/S, K103N, V106A/M, V108I, Y188C/L, A98G, F227L and M230L.

For trial 1100.1486, genotypic analysis was performed for baseline and on-therapy isolates from 23 and 34 subjects who experienced virologic failure in the nevirapine extended-release tablets and immediate-release nevirapine treatment group, respectively. Nevirapine resistance-associated substitutions developed in the on-therapy isolates of 78% (18/23) of the subjects who had virologic failures in the nevirapine extended-release tablets treatment group and 88% (30/34) of the subjects in the immediate-release nevirapine treatment group, respectively. The Y181C nevirapine resistance-associated substitution was found alone or in combination with other nevirapine resistance-associated substitutions (K101E, K103N, V106A, V108I, V179D/E/I, Y188 C/F/H/L/N, G190A, P225H, F227L, M230L) in isolates from 14 subjects failing nevirapine extended-release tablets treatment and 25 subjects failing immediate-release nevirapine treatment. On-therapy isolates from 1 subject in nevirapine extended-release tablets treatment group developed a novel amino acid substitution Y181I and isolates from another subject in the immediate-release nevirapine treatment group developed a novel amino acid substitution Y188N. Phenotypic analysis showed that Y188N and Y181I substitutions conferred 103- and 22-fold reductions in susceptibility to nevirapine, respectively.

Cross-resistance


Rapid emergence of HIV-1 strains which are cross-resistant to NNRTIs has been observed in cell culture. Nevirapine-resistant HIV-1 isolates were cross-resistant to the NNRTIs delavirdine, efavirenz and etravirine. The Y188N conferred 22- and 7-fold reductions in susceptibility to delavirdine and efavirenz, respectively, but showed no decrease in susceptibility to etravirine. Similarly, the Y181I substitution reduced susceptibility to delavirdine and etravirine 3-and 8-fold, respectively, but did not reduce susceptibility to efavirenz. However, nevirapine-resistant isolates were susceptible to the NRTIs ddI and ZDV. Similarly, ZDV-resistant isolates were susceptible to nevirapine in cell culture.

13 Nonclinical Toxicology


13.1 Carcinogenesis, Mutagenesis, Impairment of Fertility


Carcinogenesis

Long-term carcinogenicity studies in mice and rats were carried out with nevirapine. Mice were dosed with 0, 50, 375 or 750 mg/kg/day for two years. Hepatocellular adenomas and carcinomas were increased at all doses in males and at the two high doses in females. In studies in which rats were administered nevirapine at doses of 0, 3.5, 17.5 or 35 mg/kg/day for two years, an increase in hepatocellular adenomas was seen in males at all doses and in females at the high dose. The systemic exposure (based on AUCs) at all doses in the two animal studies was lower than that measured in humans at the 200 mg twice daily dose. The mechanism of the carcinogenic potential is unknown. Mutagenesis However, in genetic toxicology assays, nevirapine showed no evidence of mutagenic or clastogenic activity in a battery of in vitro and in vivo studies. These included microbial assays for gene mutation (Ames: Salmonella strains and E. coli), mammalian cell gene mutation assay (CHO/HGPRT), cytogenetic assays using a Chinese hamster ovary cell line and a mouse bone marrow micronucleus assay following oral administration. Given the lack of genotoxic activity of nevirapine, the relevance to humans of hepatocellular neoplasms in nevirapine-treated mice and rats is not known. Impairment of Fertility In reproductive toxicology studies, evidence of impaired fertility was seen in female rats at doses providing systemic exposure, based on AUC, approximately equivalent to that provided with the recommended clinical dose of nevirapine.

13.2 Animal Toxicology and/or Pharmacology


Animal studies have shown that nevirapine is widely distributed to nearly all tissues and readily crosses the blood-brain barrier.

14 Clinical Studies


14.1 Clinical Studies in Adults


Trial BI 1090 was a placebo-controlled, double-blind, randomized trial in 2249 HIV-1 infected patients with <200 CD4 + cells/mm 3 at screening. Initiated in 1995, BI 1090 compared treatment with Nevirapine + lamivudine + background therapy versus lamivudine + background therapy in NNRTI-naĂŻve patients. Treatment doses were Nevirapine, 200 mg daily for two weeks followed by 200 mg twice daily or placebo, and lamivudine, 150 mg twice daily. Other antiretroviral agents were given at approved doses. Initial background therapy (in addition to lamivudine) was one NRTI in 1309 patients (58%), two or more NRTIs in 771 (34%), and PIs and NRTIs in 169 (8%). The patients (median age 36.5 years, 70% Caucasian, 79% male) had advanced HIV-1 infection, with a median baseline CD4 + cell count of 96 cells/mm 3 and a baseline HIV-1 RNA of 4.58 log 10 copies/mL (38,291 copies/mL). Prior to entering the trial, 45% had previously experienced an AIDS-defining clinical event. Eighty-nine percent had antiretroviral treatment prior to entering the trial. BI 1090 was originally designed as a clinical endpoint study. Prior to unblinding the trial, the primary endpoint was changed to proportion of patients with HIV-1 RNA <50 copies/mL and not previously failed at 48 weeks. Treatment response and outcomes are shown in Table 5.
Table 5 BI 1090 Outcomes Through 48 Weeks
1 including change to open-label nevirapine 2 includes withdrawal of consent, lost to follow-up, non-compliance with protocol, other administrative reasons

Outcome

Nevirapine (N=1121) %

Placebo (N=1128) %

Responders at 48 weeks: HIV-1 RNA <50 copies/mL

18

2

Treatment Failure

82

98

    Never suppressed viral load

 

45

 

66

    Virologic failure after response

 

7

 

4

    CDC category C event or death

 

10

 

11

    Added antiretroviral therapy 1 while <50 copies/mL

 

5

 

1

    Discontinued trial therapy due to AE

 

7

 

6

    Discontinued trial <48 weeks 2

 

9

 

10

The change from baseline in CD4 + cell count through one year of therapy was significantly greater for the Nevirapine group compared to the placebo group for the overall study population (64 cells/mm 3 vs 22 cells/mm 3, respectively), as well as for patients who entered the trial as treatment naĂŻve or having received only ZDV (85 cells/mm 3 vs 25 cells/mm 3, respectively).

At two years into the study, 16% of subjects on Nevirapine had experienced class C CDC events as compared to 21% of subjects on the control arm.

Trial BI 1046 (INCAS) was a double-blind, placebo-controlled, randomized, three-arm trial with 151 HIV-1 infected patients with CD4 + cell counts of 200-600 cells/mm 3 at baseline. BI 1046 compared treatment with nevirapine+zidovudine+didanosine to nevirapine+zidovudine and zidovudine+didanosine. Treatment doses were Nevirapine at 200 mg daily for two weeks followed by 200 mg twice daily or placebo, zidovudine at 200 mg three times daily, and didanosine at 125 or 200 mg twice daily (depending on body weight). The patients had mean baseline HIV-1 RNA of 4.41 log 10 copies/mL (25,704 copies/mL) and mean baseline CD4 + cell count of 376 cells/mm 3. The primary endpoint was the proportion of patients with HIV-1 RNA <400 copies/mL and not previously failed at 48 weeks. The virologic responder rates at 48 weeks were 45% for patients treated with nevirapine+zidovudine+didanosine, 19% for patients treated with zidovudine+didanosine, and 0% for patients treated with nevirapine+zidovudine.

CD4 + cell counts in the nevirapine+ZDV+ddI group increased above baseline by a mean of 139 cells/mm 3 at one year, significantly greater than the increase of 87 cells/mm 3 in the ZDV+ddI patients. The nevirapine+ZDV group mean decreased by 6 cells/mm 3 below baseline.

14.2 Clinical Studies in Pediatric Patients


The pediatric safety and efficacy of Nevirapine was examined in BI Trial 1100.1368, an open-label, randomized clinical study performed in South Africa in which 123 HIV-1 infected treatment-naïve patients between 3 months and 16 years of age received Nevirapine oral suspension for 48 weeks. Patients were divided into 4 age groups (3 months to <2 years, 2 to <7 years, 7 to <12 years, and 12 to ≤16 years) and randomized to receive one of two Nevirapine doses, determined by 2 different dosing methods [body surface area (150 mg/m 2) and weight-based dosing (4 or 7 mg/kg)] in combination with zidovudine and lamivudine [see Adverse Reactions (6.2), Use in Specific Populations (8.4), and Clinical Pharmacology (12.3)] . The total daily dose of Nevirapine did not exceed 400 mg in either regimen. There were 66 patients in the body surface area (BSA) dosing group and 57 patients in the weight-based (BW) dosing group.

Baseline demographics included: 49% male; 81% Black and 19% Caucasian; 4% had previous exposure to ARVs. Patients had a median baseline HIV-1 RNA of 5.45 log 10 copies/mL and a median baseline CD4 + cell count of 527 cells/mm 3 (range 37-2279). One hundred and five (85%) completed the 48-week period while 18 (15%) discontinued prematurely. Of the patients who discontinued prematurely, 9 (7%) discontinued due to adverse reactions and 3 (2%) discontinued due to virologic failure. Overall the proportion of patients who achieved and maintained an HIV-1 RNA <400 copies/mL at 48 weeks was 47% (58/123).

16 How Supplied/storage And Handling


Nevirapine tablets, 200 mg, are white modified capsule shaped, biconvex tablets. One side is debossed with S on the left side of bisect and G on the right side of bisect and the other side with 1 on the left side of bisect 00 on the right side of bisect.

Nevirapine tablets are supplied in bottles of 60 (NDC 60429-298-60).

How Supplied/Storage and Handling


Nevirapine Tablets, USP should be stored at 20° to 25° C (68° to 77° F); excursions permitted to 15° to 30° C (59° to 86° F) [see USP Controlled Room Temperature]. Store in a safe place out of the reach of children.

Manufactured by: ScieGen Pharmaceuticals, Inc. Hauppauge, NY 11788 USA

Marketed/ Packaged by:  GSMS, Inc.   Camarillo, CA 93012

Rev. 6/14

17 Patient Counseling Information


“See FDA-approved patient labeling (Medication Guide)”

The Medication Guide provides written information for the patient, and should be dispensed with each new prescription and refill.

A Medication Guide is supplied as a tear-off following the full prescribing information.

ATTENTION PHARMACISTS: Detach "Medication Guide" and dispense with the product.

17.1 Hepatotoxicity and Skin Reactions


Inform patients of the possibility of severe liver disease or skin reactions associated with Nevirapine that may result in death. Instruct patients developing signs or symptoms of liver disease or severe skin reactions to discontinue Nevirapine and seek medical attention immediately, including performance of laboratory monitoring. Symptoms of liver disease include fatigue, malaise, anorexia, nausea, jaundice, acholic stools, liver tenderness or hepatomegaly. Symptoms of severe skin or hypersensitivity reactions include rash accompanied by fever, general malaise, fatigue, muscle or joint aches, bulers, oral lesions, conjunctivitis, facial edema and/or hepatitis.

Intensive clinical and laboratory monitoring, including liver enzymes, is essential during the first 18 weeks of therapy with Nevirapine to detect potentially life-threatening hepatotoxicity and skin reactions. However, liver disease can occur after this period; therefore, monitoring should continue at frequent intervals throughout Nevirapine treatment. Extra vigilance is warranted during the first 6 weeks of therapy, which is the period of greatest risk of hepatic events and skin reactions. Advise patients with signs and symptoms of hepatitis to discontinue Nevirapine and seek medical evaluation immediately. If Nevirapine is discontinued due to hepatotoxicity, do not restart it. Patients, particularly women, with increased CD4 + cell count at initiation of Nevirapine therapy (greater than 250 cells/mm 3 in women and greater than 400 cells/mm 3 in men) are at substantially higher risk for development of symptomatic hepatic events, often associated with rash. Advise patients that co-infection with hepatitis B or C and/or increased transaminases at the start of therapy with Nevirapine are associated with a greater risk of later symptomatic events (6 weeks or more after starting nevirapine) and asymptomatic increases in AST or ALT [see Boxed Warning and Warnings and Precautions (5.1)] .

The majority of rashes associated with Nevirapine occur within the first 6 weeks of initiation of therapy. Instruct patients that if any rash occurs during the two-week lead-in period, do not escalate the nevirapinr dose until the rash resolves. The total duration of the once-daily lead-in dosing period should not exceed 28 days, at which point an alternative regimen may need to be started. Any patient experiencing a rash should have their liver enzymes (AST, ALT) evaluated immediately. Patients with severe rash or hypersensitivity reactions should discontinue Nevirapine immediately and consult a physician. Nevirapine should not be restarted following severe skin rash or hypersensitivity reaction. Women tend to be at higher risk for development of nevirapine-associated rash [see Boxed Warning and Warnings and Precautions (5.2)] .

17.2 Administration


Inform patients to take nevirapine every day as prescribed. Patients should not alter the dose without consulting their doctor. If a dose is missed, patients should take the next dose as soon as possible. However, if a dose is skipped, the patient should not double the next dose. Advise patients to report to their doctor the use of any other medications.

Inform patients that it is not known whether nevirapine therapy reduces the risk of transmission of HIV-1 to others through sexual contact. Effective treatment combined with safer sex practices may reduce the chance of passing HIV to others through sexual contact. Patients should be advised to continue to practice safer sex and to use latex or polyurethane condoms to lower the chance of sexual contact with any body fluids such as semen, vaginal secretions or blood. Patients should be advised never to re-use or share needles.

Nevirapine is not a cure for HIV-1 infection; patients may continue to experience illnesses associated with advanced HIV-1 infection, including opportunistic infections. Advise patients to remain under the care of a physician when using nevirapine.

Advise patients taking nevirapine oral suspension to ask their pharmacist for a dosing cup or syringe if they do not have one.

Inform patients that they should not take nevirapine tablets or nevirapine oral suspension and nevirapine extended release tablets at the same time.

17.3 Drug Interactions


Nevirapine may interact with some drugs; therefore, patients should be advised to report to their doctor the use of any other prescription, non-prescription medication or herbal products, particularly St. John's wort [ see Warnings and Precautions (5.4) and Drug Interactions (7) ].

17.4 Contraceptives


Hormonal methods of birth control, other than depomedroxy-progesterone acetate (DMPA), should not be used as the sole method of contraception in women taking Nevirapine, since Nevirapine may lower the plasma levels of these medications. Additionally, when oral contraceptives are used for hormonal regulation during Nevirapine therapy, the therapeutic effect of the hormonal therapy should be monitored [ see Drug Interactions (7)] .

17.5 Methadone


Nevirapine may decrease plasma concentrations of methadone by increasing its hepatic metabolism. Narcotic withdrawal syndrome has been reported in patients treated with Nevirapine and methadone concomitantly. Methadone-maintained patients beginning nevirapine therapy should be monitored for evidence of withdrawal and methadone dose should be adjusted accordingly [ see Drug Interactions (7) ].

17.6 Fat Redistribution


Patients should be informed that redistribution or accumulation of body fat may occur in patients receiving antiretroviral therapy and that the cause and long-term health effects of these conditions are not known at this time [see Warnings and Precautions (5.6)] .

Manufactured by: ScieGen Pharmaceuticals, Inc.

Hauppaugee, NY 11788 USA

Manufactured for: GSMS, Inc. Camarillo, CA 93010

Rev: 06/14

Medication Guide


Nevirapine Tablets, USP Read this Medication Guide before you start taking nevirapine and each time you get a refill. There may be new information. This information does not take the place of talking to your doctor about your medical condition or treatment.

What is the most important information I should know about nevirapine?

Nevirapine can cause serious side effects. These include severe liver and skin problems which can cause death. These problems can happen at any time during treatment, but your risk is highest during the first 18 weeks of treatment.

1. Severe liver problems: Anyone who takes Nevirapine may get severe liver problems. In some cases, these liver problems can lead to liver failure and the need for a liver transplant, or death. People who have a higher CD4+ cell count when they begin nevirapine treatment have a higher risk of liver problems, especially:
  • • Women with CD4+ counts higher than 250 cells/mm3. This group has the highest risk.
  • • Men with CD4+ counts higher than 400 cells/mm3. 

If you are a woman with CD4+ counts higher than 250 cells/mm3 or a man with CD4+ counts higher than 400 cells/mm3, you and your doctor will decide whether starting nevirapine is right for you.

In general, women have a higher risk of liver problems compared to men. People who have abnormal liver test results before starting nevirapine treatment and people with hepatitis B or C also have a greater chance of getting liver problems.

You may get a rash if you have liver problems.

Stop taking nevirapine and call your doctor right away if you have anyof the following symptoms of liver problems:
  • • dark (tea colored) urine
  • • yellowing of your skin or whites of your eyes
  • • light-colored bowel movements (stools)
  • • fever
  • • nausea (feeling sick to your stomach)
  • • feel unwell or like you have the flu
  • • pain or tenderness on your right side below your ribs
  • • tiredness
  • • loss of appetite

Your doctor should see you and do blood tests often to check your liver function during the first 18 weeks of treatment with nevirapine. You should continue to have your liver checked regularly during your treatment with nevirapine. It is important for you to keep all of your doctor appointments.

2. Severe rash and skin reactions: Skin rash is the most common side  effect of nevirapine. Most rashes happen in the first 6 weeks of taking nevirapine. Rashes and skin reactions may be severe, life-threatening,and in some people, may lead to death. Stop using nevirapine and callyour doctor right away if you get a rash with any of the following symptoms:
  • • bulers
  • • mouth sores
  • • red or inflamed eyes, like "pink eye" (conjunctivitis)
  • • liver problems (see symptoms of liver problems above)
  • • swelling of your face
  • • feel unwell or like you have the flu
  • • fever
  • • tiredness
  • • muscle or joint aches

If your doctor tells you to stop treatment with nevirapine because you have had any of the serious liver or skin problems described above, you should never take nevirapine again.

See the section " What are the possible side effects of nevirapine?" for more information.

What is nevirapine?
  • • Nevirapine tablets are prescription HIV medicines used with other HIV medicines to treat HIV (Human Immunodeficiency Virus). HIV is the virus that causes AIDS (Acquired Immune Deficiency Syndrome).
  • • Nevirapine tablets are a type of HIV medicine called a non-nucleoside reverse transcriptase inhibitor (NNRTI).

When used with other HIV medicines, nevirapine may:
  • 1. Reduce the amount of HIV in your blood (called “viral load”)
  • 2. Help increase the number of CD4 (T) cells in your blood which help fight off other infections.

Reducing the amount of HIV and increasing the CD4 (T) cell count may improve your immune system. This may reduce your risk of death or infections that can happen when your immune system is weak (opportunistic infections).

Nevirapine does not cure HIV infection or AIDS.

Nevirapine does not cure HIV or AIDS and you may continue to experience illnesses associated with HIV-1 infection, including opportunistic infections.

You should remain under the care of a doctor when using nevirapine.
  • • You must stay on continuous HIV therapy to control HIV infection and decrease HIV-related illnesses.

Avoid doing things that can spread HIV-1 infection to others:
  • • Do not share needles or other injection equipment.
  • • Do not share personal lis that can have blood or body fluids on them, like toothbrushes and razor blades.
  • • Do not have any kind of sex without protection. Always practice safe sex by using a latex or polyurethane condom to lower the chance of sexual contact with semen, vaginal secretions, or blood.

Ask your doctor if you have any questions on how to prevent passing HIV to other people.

Who should not take Nevirapine? Tell your doctor if you have or have had liver problems. Your doctor may tell you not to take Nevirapine if you have certain liver problems.

Nevirapine is only for people diagnosed with HIV. If you have not been diagnosed as HIV positive, then do not take nevirapine.

What should I tell my doctor before taking nevirapine? 

Before you take nevirapine, tell your doctor if you:
  • • have or have had hepatitis (inflammation of your liver) or problems with your liver. See "What is the most important information I should know about nevirapine?" and "Who should not take nevirapine ?"
  • • receive dialysis
  • • have skin problems, such as a rash
  • • are pregnant or plan to become pregnant. It is not known if nevirapine will harm your unborn baby.
  • Pregnancy Registry: There is a pregnancy registry for women who take antiviral medicines during pregnancy. The purpose of the registry is to collect information about the health of you and your baby. Talk to your doctor about how you can take part in this registry.
  • • are breast-feeding or plan to breast-feed. Nevirapine can pass into your breast milk and may harm your baby. You should not breastfeed if you have HIV because of the risk of passing HIV to your baby. Do not breastfeed during treatment with nevirapine. Talk to your doctor about the best way to feed your baby.

Tell your doctor and pharmacist about all the medicines you take, including prescription and non-prescription medicines, vitamins and herbal supplements. Nevirapine may affect the way other medicines work, and other medicines may affect how Nevirapine works.

You should not take nevirapine if you also take:
  • • St. John's Wort. St. John's Wort can lower the amount of nevirapine in your body.
  • • efavirenz (Sustiva®, Atripla®). Efavirenz may cause you to have an increased chance of side effects.
  • • atazanavir (Reyataz®)
  • • lopinavir and ritonavir (Kaletra®)
  • • fosamprenavir calcium (Lexiva®)
  • • itraconazole (Sporanox®)
  • • ketoconazole (Nizoral®)
  • • rifampin (Rifadin®, Rifamate®, Rifater®)
  • • Birth control pills. Birth control pills taken by mouth (oral contraceptives) and other hormone types of birth control may not work to prevent pregnancy. Talk with your doctor about other types of birth control that you can use to prevent pregnancy during treatment with nevirapine.

Also tell your doctor if you take:
  • • clarithromycin (Biaxin®)
  • • fluconazole (Diflucan®)
  • • indinavir sulfate (Crixivan®)
  • • methadone
  • • nelfinavir mesylate (Viracept®)
  • • rifabutin (Mycobutin®)
  • • warfarin (Coumadin®, Jantoven ®)
  • • saquinavir mesylate (Invirase®)
  • • amiodarone, disopyramide (Norpace®), lidocaine
  • • carbamazepine, clonazepam (Klonopin®), ethosuximide (Zarontin®)
  • • diltiazem, nifedipine, verapamil
  • • cyclophosphamide
  • • ergotamine
  • • cyclosporine, tacrolimus, sirolimus (Rapamune®)
  • • cisapride (Propulsid®)
  • • fentanyl

If you are not sure if you take a medicine above, ask your doctor or pharmacist.

Know the medicines you take. Keep a ul of them to show your doctor or pharmacist when you get a new medicine.

How should I take nevirapine?
  • • Nevirapine is always taken in combination with other anti-HIV medications.
  • • Take nevirapine exactly as your doctor tells you to take it. Do not change your dose unless your doctor tells you to.
  • • You should never take more than one form of nevirapine at the same time. Talk to your doctor if you have any questions.
  • • If your child is prescribed nevirapine, your child’s doctor will tell you exactly how nevirapine should be taken.
  • • You may take nevirapine with or without food.
  • • Do not miss a dose of nevirapine. If you miss a dose of nevirapine, take the missed dose as soon as you remember. If it is almost time for your next dose, do not take the missed dose, just take the next dose at your regular time. Do not take two doses at the same time.
  • • If you stop taking nevirapine for more than 7 days, ask your doctor how much to take before you start taking it again. You may need to begin taking the nevirapine starting dose again, which is taken 1 time each day for 14 days.
  • Starting nevirapine tablets:

1. Your doctor should start you with 1 dose each day to lower your chance of getting a serious rash. It is important that you only take1 dose of nevirapine each day for the first 14 days.
  • • Call your doctor right away if you get a skin rash during the first14 days of nevirapine treatment and do not increase your dose to 2 times a day.
  • • You should never take your starting dose for longer than 28 days. If after 28 days you are still receiving this starting dose because you have a rash, you and your doctor should talk about prescribing another HIV medicine for you instead of nevirapine.
  • • Do not increase your dose to 2 times a day if you have a rash.

2. Day 15, you will take 1 nevirapine tablet two times a day.

Starting nevirapine extended-release tablets and this is the first time you are taking any form of nevirapine:

1. Your doctor should start you with 1 dose of nevirapine tablets each day to lower your chance of getting a serious rash. It is important thatyou only take 1 dose of nevirapine each day for the first 14 days.
  • • Call your doctor right away if you get a skin rash during the first14 days of nevirapine treatment and do not increase your dose to 2 times a day.
  • • You should never take your starting dose for longer than 28 days. If after 28 days you are still receiving this starting dose because you have a rash, you and your doctor should talk about prescribing another HIV medicine for you instead of nevirapine.
  • • Do not start nevirapine extended-release tablets if you have a rash.

2. Day 15, you will take 1 nevirapine extended-release tablet each day.

Switching from nevirapine tablets to nevirapine extended-release tablets:

1. Take nevirapine extended-release tablet 1 time a day.

What are the possible side effects of nevirapine?

Nevirapine may cause serious side effects, including:

• See " What is the most important information I should know about nevirapine?"
    • Changes in your immune system (Immune Reconstitution Syndrome) can happen when you start taking HIV medicines. Your immune system may get stronger and begin to fight infections that have been hidden in your body for a long time. Tell your doctor if you start having new symptoms after starting your HIV medicine.
    • Changes in body fat can happen in some people who take antiretroviral therapy. These changes may include increased amount of fat in the upper back and neck ("buffalo hump"), breast, and around the middle of your body (trunk). Loss of fat from your legs, arms, and face can also happen. The cause and long-term health effects of these problems are not known at this time.
  • The most common side effect of nevirapine is rash.
  • Tell your doctor if you have any side effect that bothers you or that does not go away.
  • These are not all the possible side effects of nevirapine. For more information, ask your doctor or pharmacist.
  • Call your doctor for medical advice about side effects. You may report side effects to FDA at 1-800-FDA-1088.

How should I store nevirapine?
  • Store nevirapine tablets at 20° to 25°C (68° to 77°F). [See USP Controlled Room Temperature.].
  • Throw away nevirapine that is no longer needed or out-of-date.

Keep nevirapine and all medicines out of the reach of children.

General information about nevirapine

Medicines are sometimes prescribed for purposes other than those uled in a Medication Guide. Do not use nevirapine for a condition for which it was not prescribed. Do not give nevirapine to other people, even if they have the same condition you have. It may harm them.

This Medication Guide summarizes the most important information about nevirapine. If you would like more information, talk with your doctor. You can ask your pharmacist or doctor for information about nevirapine that is written for health professionals.

For more information, call ScieGen Pharmaceuticals, Inc., at 1-855-724-3436 or contact GSMS, Inc. at 1-800-284-8633.

What are the ingredients in nevirapine?

Active ingredient: nevirapine

Inactive ingredients:

Nevirapine Tablets: microcrystalline cellulose, lactose monohydrate, povidone, sodium starch glycolate, silicon dioxide and magnesium stearate.

This Medication Guide has been approved by the U.S. Food and Drug Administration

Manufactured by: ScieGen Pharmaceuticals, Inc. Hauppauge, NY 11788 USA

Manufactured for: GSMS, Inc. Camarillo, CA 83010

Rev: 06/14

The brands uled are trademarks of their respective owners and are not trademarks of ScieGen Pharmaceuticals, Inc. or GSMS, Inc. The makers of these brands are not affiliated with and do not endorse ScieGen Pharmaceuticals, Inc. or GSMS, Inc. or its products.

Principal Display Panel 200mg 60s


Nevirapine Tablets, USP

200 mg

60 Tablets

NDC 60429-298-60

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