Peginterferon alfa-2a
003580
Categories, Drug
Classes, Brand Names & Cost Of Therapy
Categories: Hepatitis C; Pregnancy
Category X; FDA Approved 2002 Dec
Drug Classes: Antivirals;
Immunomodulators
Brand Names: Pegasys
Warning
Alpha interferons, including
peginterferon alfa-2a (peginterferon alfa-2a), may cause or aggravate fatal or
life-threatening neuropsychiatric, autoimmune, ischemic, and infectious
disorders. Patients should be monitored closely with periodic clinical and
laboratory evaluations. Therapy should be withdrawn in patients with
persistently severe or worsening signs or symptoms of these conditions. In
many, but not all cases, these disorders resolve after stopping peginterferon
alfa-2a therapy (see WARNINGS and ADVERSE REACTIONS).
Use With Ribavirin
Ribavirin, including Copegus, may
cause birth defects and/or death of the fetus. Extreme care must be taken to
avoid pregnancy in female patients and in female partners of male patients.
Ribavirin causes hemolytic anemia. The anemia associated with ribavirin therapy
may result in a worsening of cardiac disease. Ribavirin is genotoxic and
mutagenic and should be considered a potential carcinogen (see ribavirin
package insert for additional information and other warnings).
DescriptionPeginterferon alfa-2a, is a
covalent conjugate of recombinant alfa-2a interferon (approximate molecular
weight [MW] 20,000 daltons) with a single branched bis-monomethoxy polyethylene
glycol (PEG) chain (approximate MW 40,000 daltons). The PEG moiety is linked at
a single site to the interferon alfa moiety via a stable amide bond to lysine.
Peginterferon alfa-2a has an approximate molecular weight of 60,000 daltons.
Interferon alfa-2a is produced using recombinant DNA technology in which a
cloned human leukocyte interferon gene is inserted into and expressed in
Escherichia coli.
Each vial contains approximately 1.2 ml of solution
to deliver 1.0 ml of drug product. Subcutaneous (SC) administration of 1.0 ml
delivers 180 µg of drug product (expressed as the amount of interferon
alfa-2a), 8.0 mg sodium chloride, 0.05 mg polysorbate 80, 10.0 mg benzyl
alcohol, 2.62 mg sodium acetate trihydrate, and 0.05 mg acetic acid. The
solution is colorless to light yellow and the pH is 6.0 ± 0.01.
Clinical PharmacologyPharmacodynamics
Interferons bind to specific receptors on the
cell surface initiating intracellular signaling via a complex cascade of
protein-protein interactions leading to rapid activation of gene transcription.
Interferon-stimulated genes modulate many biological effects including the
inhibition of viral replication in infected cells, inhibition of cell
proliferation, and immunomodulation. The clinical relevance of these in vitro
activities is not known.
Peginterferon alfa-2a stimulates the
production of effector proteins such as serum neopterin and 2′,
5′-oligoadenylate synthetase.
Pharmacokinetics
Maximal serum concentrations (Cmax)
occur between 72-96 hours post dose. The Cmax and AUC measurements
of peginterferon alfa-2a increase in a dose-related manner. Week 48 mean trough
concentrations (16 ng/ml; range 4-28) at 168 hours post dose are approximately
2-fold higher than week 1 mean trough concentrations (8 ng/ml; range 0-15).
Steady-state serum levels are reached within 5-8 weeks of once weekly dosing.
The peak to trough ratio at week 48 is approximately 2.0.
The mean systemic clearance in healthy
subjects given peginterferon alfa-2a was 94 ml/h, which is 48 approximately
100- fold lower than that for interferon alfa-2a (interferon alfa-2b). The mean
terminal half- life after SC dosing in patients with chronic hepatitis C was 80
hours (range 50-140 hours) compared to 5.1 hours (range 3.7-8.5 hours) for
interferon alfa-2b.
Special Populations
Gender and
Age
Peginterferon alfa-2a administration yielded
similar pharmacokinetics in male and female healthy subjects. The AUC was
increased from 1295-1663 ng·h/ml in subjects older than 62 years taking
180 µg peginterferon alfa-2a, but peak concentrations were similar (9 vs
10 ng/ml) in those older and younger than 62 years.
Pediatric
Patients
The pharmacokinetics of peginterferon alfa-2a
have not been adequately studied in pediatric patients.
Renal
Dysfunction
In patients with end stage renal disease
undergoing hemodialysis, there is a 25-45% reduction in peginterferon alfa-2a
clearance (see PRECAUTIONS, Renal Impairment).
The pharmacokinetics of ribavirin following
administration of ribavirin have not been studied in patients with renal
impairment and there are limited data from clinical trials on administration of
ribavirin in patients with creatinine clearance <50 ml/min. Therefore,
patients with creatinine clearance <50 ml/min should not be treated with
ribavirin (see WARNINGS and DOSAGE AND ADMINISTRATION).
Effect of Food on
Absorption of Ribavirin
Bioavailability of a single oral dose of
ribavirin was increased by co-administration with a high-fat meal. The
absorption was slowed (Tmax was doubled) and the AUC(0-192h) and
Cmax increased by 42% and 66%, respectively, when ribavirin was
taken with a high-fat meal compared with fasting conditions (see DOSAGE AND
ADMINISTRATION).
Drug InteractionsDrug Interactions
Nucleoside
Analogues
Ribavirin has been shown in vitro to inhibit
phosphorylation of zidovudine and stavudine which could lead to decreased
anti-retroviral activity. Exposure to didanosine or its active metabolite
(dideoxyadenosine 5′-triphosphate) is increased when didanosine is
co-administered with ribavirin (see DRUG INTERACTIONS).
Clinical StudiesPeginterferon alfa-2a
Monotherapy (Studies 1, 2, and 3)
The safety and effectiveness of peginterferon
alfa-2a for the treatment of hepatitis C virus infection were assessed in three
randomized, open- label, active-controlled clinical studies. All patients were
adults, had compensated liver disease, detectable hepatitis C virus (HCV),
liver biopsy diagnosis of chronic hepatitis, and were previously untreated with
interferon. All patients received therapy by SC injection for 48 weeks, and
were followed for an additional 24 weeks to assess the durability of response.
In studies 1 and 2, approximately 20% of subjects had cirrhosis or bridging
fibrosis. Study 3 enrolled patients with a histological diagnosis of cirrhosis
(78%) or bridging fibrosis (22%).
In study 1 (n=630), patients received either
interferon alfa-2a 3 MIU 3 times/week (TIW), peginterferon alfa-2a 135 µg
once each week (qw) or peginterferon alfa-2a 180 µg qw. In study 2
(n=526), patients received either interferon alfa-2b 6 MIU TIW for 12 weeks
followed by 3 MIU TIW for 36 weeks or peginterferon alfa-2a 180 µg qw. In
study 3 (n=269), patients received interferon alfa-2b 3 MIU TIW, peginterferon
alfa-2a 90 µg qw or peginterferon alfa-2a 180 µg once each
week.
In all three studies, treatment with
peginterferon alfa-2a 180 µg resulted in significantly more patients who
experienced a sustained response (defined as undetectable HCV RNA and
normalization of ALT on or after study week 68) compared to treatment with
interferon alfa-2b. In study 1, response to peginterferon alfa-2a 135 µg
was not different from response to 180 µg. In study 3, response to
peginterferon alfa-2a 90 µg was intermediate between peginterferon
alfa-2a 180 µg and interferon alfa-2b.
TABLE 1 Sustained Response to Monotherapy
Treatment
| |
|
n |
Combined Virologic and Biologic
Sustained Response |
Sustained Virologic
Response† |
|
Study 1 |
| |
Interferon alfa-2b 3 MIU |
207 |
11% |
11% |
| |
Peginterferon alfa-2a 180 µg
|
208 |
24% |
26% |
| |
Diff* (95% CI) |
|
12 (6, 20) |
15 (8, 23) |
|
Study 2 |
| |
Interferon alfa-2b 6/3 MIU |
261 |
17% |
19% |
| |
Peginterferon alfa-2a 180 µg
|
265 |
35% |
38% |
| |
Diff* (95% CI) |
|
18 (11, 25) |
19 (11, 26) |
|
Study 3 |
| |
Interferon alfa-2b 3 MIU |
86 |
7% |
8% |
| |
Peginterferon alfa-2a 180 µg
|
87 |
23% |
30% |
| |
Diff* (95% CI) |
|
16 (6, 26) |
22 (11, 33) |
|
*
Percent difference between peginterferon
alfa-2a and Roferon-A treatment. |
|
†
Cobas Amplicor HCVTest, version 2.0.
|
Matched pre- and post-treatment liver biopsies
were obtained in approximately 70% of 109 patients. Similar modest reductions
in inflammation compared to baseline were observed in all treatment
groups.
Of the patients who did not demonstrate either
undetectable HCV RNA or at least a 2-log10 drop in HCV RNA titer from baseline
by 12 weeks of peginterferon alfa-2a 180 µg therapy, 2% (3/156) achieved
a sustained virologic response (see DOSAGE AND ADMINISTRATION).
Averaged over study 1, study 2, and study 3,
response rates to peginterferon alfa-2a were 23% among patients with viral
genotype 1 and 48% in patients with other viral genotypes. The treatment
response rates were similar in men and women.
Peginterferon
alfa-2a/Ribavirin Combination Therapy (Studies 4 and 5)
The safety and effectiveness of peginterferon
alfa-2a in combination with ribavirin for the treatment of hepatitis C virus
infection were assessed in two randomized controlled clinical trials. All
patients were adults, had compensated liver disease, detectable hepatitis C
virus, liver biopsy diagnosis of chronic hepatitis, and were previously
untreated with interferon. Approximately 20% of patients in both studies had
compensated cirrhosis (Child-Pugh class A).
In study 4, patients were randomized to
receive either peginterferon alfa-2a 180 µg SC once weekly (qw) with an
oral placebo, peginterferon alfa-2a 180 µg qw with ribavirin 1000 mg PO
(body weight <75 kg) or 1200 mg PO (body weight ≥75 kg) or interferon
alfa-2b 3 MIU SC TIW plus ribavirin 1000 mg or 1200 mg PO. All patients
received 48 weeks of therapy followed by 24 weeks of treatment-free follow-up.
Ribavirin or placebo treatment assignment was blinded. Peginterferon alfa-2a in
combination with ribavirin resulted in a higher SVR (defined as undetectable
HCV RNA at the end of the 24 week treatment-free follow-up period) compared to
peginterferon alfa-2a alone or interferon alfa-2b and ribavirin (TABLE 2). In
all treatment arms, patients with viral genotype 1 regardless of viral load,
had a lower response rate compared to patients with other viral
genotypes.
TABLE 2 Sustained Virologic Response to Combination
Therapy (Study 4)
| |
Interferon alfa-2b +
|
Peginterferon alfa-2a +
|
Peginterferon alfa-2a +
|
| |
Ribavirin 1000 mg or 1200 mg
|
Placebo |
Ribavirin 1000 mg or 1200 mg
|
|
All patients |
197/444 (44%) |
65/224 (29%) |
241/453 (53%) |
|
Genotype 1 |
103/285 (36%) |
29/145 (20%) |
132/298 (44%) |
|
Genotypes 2-6 |
94/159 (59%) |
36/79 (46%) |
109/155 (70%) |
|
Difference in overall treatment response
(peginterferon alfa-2a/ribavirin Interferon alfa -2b/ribavirin) was 9% (95% CI
2.3, 15.3). |
In study 5, all patients received
peginterferon alfa-2a 180 µg SC qw and were randomized to treatment for
either 24 or 48 weeks and to a ribavirin dose of either 800 mg or 1000 mg/1200
mg (for body weight <75 kg / ≥75 kg). Assignment to the four treatment
arms was stratified by viral genotype and baseline HCV viral titer. Patients
with genotype 1 and high viral titer (defined as >2 × 10
6
HCV RNA copies/ml serum) were preferentially assigned to treatment for 48
weeks.
Genotype 1
Irrespective of baseline viral titer,
treatment for 48 weeks with peginterferon alfa-2a and 1000 mg or 1200 mg of
ribavirin resulted in higher SVR (defined as undetectable HCV RNA at the end of
the 24 week treatment-free follow-up period) compared to shorter treatment (24
weeks) and/or 800 mg ribavirin.
Genotype
Non-1
Irrespective of baseline viral titer,
treatment for 24 weeks with peginterferon alfa-2a and 800 mg of ribavirin
resulted in a similar SVR compared to longer treatment (48 weeks) and/or 1000
mg or 1200 mg of ribavirin (see TABLE 3).
TABLE 3 Sustained Virologic Response as a Function of
Genotype (Study 5)
| |
24 Weeks Treatment |
48 Weeks Treatment |
| |
Peginterferon alfa-2a +
Copegus |
Peginterferon alfa-2a +
Copegus |
| |
800 mg |
1000 mg or 1200 mg*
|
800 mg |
1000 mg or 1200 mg*
|
| |
(n=207) |
(n=280) |
(n=361) |
(n=436) |
|
Genotype 1 |
29/101 (29%) |
48/118 (41%) |
99/250 (40%) |
138/271 (51%) |
|
Genotype 2-3 |
79/96 (82%) |
116/144 (81%) |
75/99 (76%) |
117/153 (76%) |
|
*
1000 mg for body weight <75 kg; 1200 mg for
body weight ≥75 kg. |
Among the 36 patients with genotype 4,
response rates were similar to those observed in patients with genotype 1 (data
not shown). The numbers of patients with genotype 5 and 6 were too few to allow
for meaningful assessment.
Treatment
Response in Patient Subgroups
Treatment response rates are lower in patients
with poor prognostic factors receiving pegylated interferon alpha therapy. In
studies 4 and 5, treatment response rates were lower in patients older than 40
years (50% vs 66%), in patients with cirrhosis (47% vs 59%), in patients
weighing over 85 kg (49% vs 60%), and in patients with genotype 1 with high
versus low viral load (43% vs 56%). African American patients had lower
response rates compared to Caucasians.
Paired liver biopsies were performed on
approximately 20% of patients in Studies 4 and 5. Modest reductions in
inflammation compared to baseline were seen in all treatment groups.
In studies 4 and 5, lack of early virologic
response at 12 weeks (defined as HCV RNA undetectable or >2log10 lower than
baseline) was grounds for discontinuation of treatment. Of patients who lacked
an early viral response at 12 weeks and completed a recommended course of
therapy despite a protocol-defined option to discontinue therapy, 5/39 (13%)
achieved an SVR. Of patients who lacked an early viral response at 24 weeks, 19
completed a full course of therapy and none achieved an SVR.
Indications And UsagePeginterferon
alfa-2a, alone or in combination with ribavirin, is indicated for the treatment
of adults with chronic hepatitis C virus infection who have compensated liver
disease and have not been previously treated with interferon alpha.
ContraindicationsPeginterferon alfa-2a is
contraindicated in patients with:
|
Hypersensitivity to peginterferon alfa-2a or
any of its components. |
|
Hepatic decompensation (Child-Pugh class B and
C) before or during treatment. |
Peginterferon alfa-2a is contraindicated in
neonates and infants because it contains benzyl alcohol. Benzyl alcohol is
associated with an increased incidence of neurologic and other complications in
neonates and infants, which are sometimes fatal.
Peginterferon alfa-2a and ribavirin
combination therapy is additionally contraindicated in:
|
Patients with known hypersensitivity to
ribavirin or to any component of the tablet. |
|
Men whose female partners are pregnant.
|
|
Patients with hemoglobinopathies (e.g., thalassemia major, sickle-cell anemia).
|
WarningsGeneral
Patients should be monitored for the following
serious conditions, some of which may become life threatening. Patients with
persistently severe or worsening signs or symptoms should have their therapy
withdrawn (see BOXED WARNING).
Neuropsychiatric
Life-threatening or fatal neuropsychiatric
reactions may manifest in patients receiving therapy with peginterferon alfa-2a
and include suicide, suicidal ideation, depression, relapse of drug addiction
and drug overdose. These reactions may occur in patients with and without
previous psychiatric illness.
Peginterferon alfa-2a should be used with
extreme caution in patients who report a history of depression.
Neuropsychiatric adverse events observed with alpha interferon treatment
include aggressive behavior, psychoses, hallucinations, bipolar disorders and
mania. Physicians should monitor all patients for evidence of depression and
other psychiatric symptoms. Patients should be advised to report any sign or
symptom of depression or suicidal ideation to their prescribing physicians. In
severe cases, therapy should be stopped immediately and psychiatric
intervention instituted (see ADVERSE REACTIONS and DOSAGE AND
ADMINISTRATION).
Infections
Serious and severe bacterial infections, some
fatal, have been observed in patients treated with alpha interferons including
peginterferon alfa-2a. Some of the infections have been associated with
neutropenia. Peginterferon alfa-2a should be discontinued in patients who
develop severe infections and appropriate antibiotic therapy instituted.
Bone Marrow
Toxicity
Peginterferon alfa-2a suppresses bone marrow
function and may result in severe cytopenias. Ribavirin may potentiate the
neutropenia and lymphopenia induced by alpha interferons including
peginterferon alfa-2a. Very rarely alpha interferons may be associated with
aplastic anemia. It is advised that complete blood counts (CBC) be obtained
pre-treatment and monitored routinely during therapy (see PRECAUTIONS,
Laboratory Tests).
Peginterferon alfa-2a and ribavirin should be
used with caution in patients with baseline neutrophil counts <1500
cells/mm3 ,
with baseline platelet counts <90,000 cells/mm3
or
baseline hemoglobin <10 g/dl. Peginterferon alfa-2a therapy should be
discontinued, at least temporarily, in patients who develop severe decreases in
neutrophil and/or platelet counts (see DOSAGE AND ADMINISTRATION, Dose
Modification).
Cardiovascular Disorders
Hypertension, supraventricular arrhythmias,
chest pain, and myocardial infarction have been observed in patients treated
with peginterferon alfa-2a.
Peginterferon alfa-2a should be administered
with caution to patients with preexisting cardiac disease. Because cardiac
disease may be worsened by ribavirin- induced anemia, patients with a history
of significant or unstable cardiac disease should not use ribavirin (see
WARNINGS, Anemia and the ribavirin package insert).
Hypersensitivity
Severe acute hypersensitivity reactions (e.g., urticaria, angioedema,
bronchoconstriction, anaphylaxis) have been rarely observed during alpha
interferon and ribavirin therapy. If such reaction occurs, therapy with
peginterferon alfa-2a and ribavirin should be discontinued and appropriate
medical therapy immediately instituted.
Endocrine
Disorders
Peginterferon alfa-2a causes or aggravates
hypothyroidism and hyperthyroidism. Hyperglycemia, hypoglycemia, and diabetes
mellitus have been observed to develop in patients treated with peginterferon
alfa-2a. Patients with these conditions at baseline who cannot be effectively
treated by medication should not begin peginterferon alfa-2a therapy. Patients
who develop these conditions during treatment and cannot be controlled with
medication may require discontinuation of peginterferon alfa-2a therapy.
Autoimmune
Disorders
Development or exacerbation of autoimmune
disorders including myositis, hepatitis, ITP, psoriasis, rheumatoid arthritis,
interstitial nephritis, thyroiditis, and systemic lupus erythematosus have been
reported in patients receiving alpha interferon. Peginterferon alfa-2a should
be used with caution in patients with autoimmune disorders.
Pulmonary
Disorders
Dyspnea, pulmonary infiltrates, pneumonia,
bronchiolitis obliterans, interstitial pneumonitis and sarcoidosis, some
resulting in respiratory failure and/or patient deaths, may be induced or
aggravated by peginterferon alfa-2a or alpha interferon therapy. Patients who
develop persistent or unexplained pulmonary infiltrates or pulmonary function
impairment should discontinue treatment with peginterferon alfa-2a.
Colitis
Ulcerative, and hemorrhagic/ischemic colitis,
sometimes fatal, have been observed within 12 weeks of starting alpha
interferon treatment. Abdominal pain, bloody diarrhea, and fever are the
typical manifestations of colitis. Peginterferon alfa-2a should be discontinued
immediately if these symptoms develop. The colitis usually resolves within 1-3
weeks of discontinuation of alpha interferon.
Pancreatitis
Pancreatitis, sometimes fatal, has occurred
during alpha interferon and ribavirin treatment. Peginterferon alfa-2a and
ribavirin should be suspended if symptoms or signs suggestive of pancreatitis
are observed. Peginterferon alfa-2a and ribavirin should be discontinued in
patients diagnosed with pancreatitis.
Ophthalmologic Disorders
Decrease or loss of vision, retinopathy
including macular edema, retinal artery or vein thrombosis, retinal hemorrhages
and cotton wool spots, optic neuritis, and papilledema are induced or
aggravated by treatment with peginterferon alfa-2a or other alpha interferons.
All patients should receive an eye examination at baseline. Patients with
preexisting ophthalmologic disorders (e.g., diabetic or hypertensive retinopathy)
should receive periodic ophthalmologic exams during interferon alpha treatment.
Any patient who develops ocular symptoms should receive a prompt and complete
eye examination. Peginterferon alfa-2a treatment should be discontinued in
patients who develop new or worsening ophthalmologic disorders.
Use With
Ribavirin
Also, see ribavirin package insert.
Ribavirin may cause birth defects
and/or death of the exposed fetus. Extreme care must be taken to avoid
pregnancy in female patients and in female partners of male patients taking
peginterferon alfa-2a and ribavirin combination therapy. RIBAVIRIN THERAPY
SHOULD NOT BE STARTED UNLESS A REPORT OF A NEGATIVE PREGNANCY TEST HAS BEEN
OBTAINED IMMEDIATELY PRIOR TO INITIATION OF THERAPY. Women of childbearing
potential and men must use 2 forms of effective contraception during treatment
and for at least 6 months after treatment has concluded. Routine monthly
pregnancy tests must be performed during this time (see BOXED WARNING,
CONTRAINDICATIONS, PRECAUTIONS, Information for the Patient, and the ribavirin
package insert).
Anemia
The primary toxicity of ribavirin is hemolytic
anemia. Hemoglobin <10 g/dl was observed in approximately 13% of ribavirin
and peginterferon alfa-2a treated patients in clinical trials (see PRECAUTIONS,
Laboratory Tests). The anemia associated with ribavirin occurs within 1-2 weeks
of initiation of therapy with maximum drop in hemoglobin observed during the
first 8 weeks. BECAUSE THE INITIAL DROP IN HEMOGLOBIN MAY BE SIGNIFICANT, IT IS
ADVISED THAT HEMOGLOBIN OR HEMATOCRIT BE OBTAINED PRETREATMENT AND AT WEEK 2
AND WEEK 4 OF THERAPY OR MORE FREQUENTLY IF CLINICALLY INDICATED. Patients
should then be followed as clinically appropriate.
Fatal and nonfatal myocardial infarctions have
been reported in patients with anemia caused by ribavirin. Patients should be
assessed for underlying cardiac disease before initiation of ribavirin therapy.
Patients with pre-existing cardiac disease should have electrocardiograms
administered before treatment, and should be appropriately monitored during
therapy. If there is any deterioration of cardiovascular status, therapy should
be suspended or discontinued (see DOSAGE AND ADMINISTRATION, Dose Modification,
Ribavirin). Because cardiac disease may be worsened by drug-induced anemia,
patients with a history of significant or unstable cardiac disease should not
use ribavirin (see ribavirin package insert).
Renal
It is recommended that renal function be
evaluated in all patients started on ribavirin. Ribavirin should not be
administered to patients with creatinine clearance <50 ml/min (see CLINICAL
PHARMACOLOGY, Special Populations).
PrecautionsGeneral
The safety and efficacy of peginterferon
alfa-2a alone or in combination with ribavirin for the treatment of hepatitis C
have not been established in:
|
Patients who have failed other alpha
interferon treatments. |
|
Liver or other organ transplant
recipients. |
|
Patients co-infected with human
immunodeficiency virus (HIV) or hepatitis B virus (HBV). |
Renal Impairment
A 25-45% higher exposure to peginterferon
alfa-2a is seen in subjects undergoing hemodialysis. In patients with impaired
renal function, signs and symptoms of interferon toxicity should be closely
monitored. Doses of peginterferon alfa-2a should be adjusted accordingly.
Peginterferon alfa-2a should be used with caution in patients with creatinine
clearance <50 ml/min (see DOSAGE AND ADMINISTRATION, Dose
Modification).
Information for the Patient
Patients receiving peginterferon alfa-2a alone
or in combination with ribavirin should be directed in its appropriate use,
informed of the benefits and risks associated with treatment, and referred to
the peginterferon alfa-2a and, if applicable, ribavirin medication
guides.
Peginterferon alfa-2a and ribavirin
combination therapy must not be used by women who are pregnant or by men whose
female partners are pregnant. Ribavirin therapy should not be initiated until a
report of a negative pregnancy test has been obtained immediately before
starting therapy. Female patients of childbearing potential and male patients
with female partners of childbearing potential must be advised of the
teratogenic/embryocidal risks and must be instructed to practice effective
contraception during ribavirin therapy and for 6 months posttherapy. Patients
should be advised to notify the physician immediately in the event of a
pregnancy (see CONTRAINDICATIONS and WARNINGS).
Women of childbearing potential and men must
use 2 forms of effective contraception during treatment and during the 6 months
after treatment has concluded; routine monthly pregnancy tests must be
performed during this time (see CONTRAINDICATIONS and ribavirin package
insert).
If pregnancy does occur during treatment or
during 6 months post-therapy, the patient must be advised of the significant
teratogenic risk of ribavirin therapy to the fetus. To monitor maternal-fetal
outcomes of pregnant women exposed to ribavirin, the Copegus Pregnancy Registry
has been established. Physicians and patients are strongly encouraged to
register by calling 1-800-526-6367.
Patients should be advised that laboratory
evaluations are required before starting therapy and periodically thereafter
(see Laboratory Tests). Patients should be instructed to remain well hydrated,
especially during the initial stages of treatment. Patients should be advised
to take ribavirin with food.
Patients should be informed that it is not
known if therapy with peginterferon alfa-2a alone or in combination with
ribavirin will prevent transmission of HCV infection to others or prevent
cirrhosis, liver failure or liver cancer that might result from HCV infection.
Patients who develop dizziness, confusion, somnolence, and fatigue should be
cautioned to avoid driving or operating machinery.
If home use is prescribed, a
puncture-resistant container for the disposal of used needles and syringes
should be supplied to the patients. Patients should be thoroughly instructed in
the importance of proper disposal and cautioned against any reuse of any
needles and syringes. The full container should be disposed of according to the
directions provided by the physician (see medication guide that comes with the
prescription).
Laboratory Tests
Before beginning peginterferon alfa-2a or
peginterferon alfa-2a and ribavirin combination therapy, standard hematological
and biochemical laboratory tests are recommended for all patients. Pregnancy
screening for women of childbearing potential must be performed.
After initiation of therapy, hematological
tests should be performed at 2 weeks and 4 weeks and biochemical tests should
be performed at 4 weeks. Additional testing should be performed periodically
during therapy. In the clinical studies, the CBC (including hemoglobin level
and white blood cell and platelet counts) and chemistries (including liver
function tests and uric acid) were measured at 1, 2, 4, 6, and 8, and then
every 4 weeks or more frequently if abnormalities were found. Thyroid
stimulating hormone (TSH) was measured every 12 weeks. Monthly pregnancy
testing should be performed during combination therapy and for 6 months after
discontinuing therapy.
The entrance criteria used for the clinical
studies of peginterferon alfa-2a may be considered as a guideline to acceptable
baseline values for initiation of treatment:
|
Platelet count ≥90,000
cells/mm3 (as
low as 75,000 cells/mm3
in
patients with cirrhosis). |
|
Caution should be exercised in initiating
treatment in any patient with baseline risk of severe anemia (e.g., spherocytosis, history of GI bleeding).
|
|
Absolute neutrophil count (ANC) ≥1500
cells/mm3 . |
|
Serum creatinine concentration <1.5 ×
upper limit of normal. |
|
TSH and T4 within normal limits or adequately
controlled thyroid function. |
Peginterferon alfa-2a treatment was associated
with decreases in WBC, ANC, lymphocytes and platelet counts often starting
within the first 2 weeks of treatment (see ADVERSE REACTIONS). Dose reduction
is recommended in patients with hematologic abnormalities (see DOSAGE AND
ADMINISTRATION, Dose Modification).
While fever is commonly caused by
peginterferon alfa-2a therapy, other causes of persistent fever must be ruled
out, particularly in patients with neutropenia (see WARNINGS,
Infections).
Transient elevations in ALT (2- to 5-fold
above baseline) were observed in some patients receiving peginterferon alfa-2a,
and were not associated with deterioration of other liver function tests. When
the increase in ALT levels is progressive despite dose reduction or is
accompanied by increased bilirubin, peginterferon alfa-2a therapy should be
discontinued (see DOSAGE AND ADMINISTRATION, Dose Modification).
Carcinogenesis, Mutagenesis, and
Impairment of Fertility
Carcinogenesis
Peginterferon alfa-2a has not been tested for
its carcinogenic potential.
Mutagenesis
Peginterferon alfa-2a did not cause DNA damage
when tested in the Ames bacterial mutagenicity assay and in the
in vitro chromosomal aberration assay
in human lymphocytes, either in the presence or absence of metabolic
activation.
Use With
Ribavirin
Ribavirin is genotoxic and mutagenic. The
carcinogenic potential of ribavirin has not been fully determined. In a p53
(+/-) mouse carcinogenicity study at doses up to the maximum tolerated dose of
100 mg/kg/day ribavirin was not oncogenic. However, on a body surface area
basis, this dose was 0.5 times maximum recommended human 24 hour dose of
ribavirin. A study in rats to assess the carcinogenic potential of ribavirin is
ongoing.
Mutagenesis
See ribavirin package insert.
Impairment of
Fertility
Peginterferon alfa-2a may impair fertility in
women. Prolonged menstrual cycles and/or 437 amenorrhea were observed in female
cynomolgus monkeys given SC injections of 600 µg/kg/dose (7200
µg/m 2 /dose) of peginterferon alfa-2a every other day for
1 month, at approximately 180 times the recommended weekly human dose for a 60
kg person (based on body surface area). Menstrual cycle irregularities were
accompanied by both a decrease and delay in the peak 17β-estradiol and
progesterone levels following administration of peginterferon alfa-2a to female
monkeys. A return to normal menstrual rhythm followed cessation of treatment.
Every other day dosing with 100 µg/kg (1200 µg/m
2 )
peginterferon alfa-2a (equivalent to approximately 30 times the recommended
human dose) had no effects on cycle duration or reproductive hormone
status.
The effects of peginterferon alfa-2a on male
fertility have not been studied. However, no adverse effects on fertility were
observed in male Rhesus monkeys treated with non-pegylated interferon alfa-2a
for 5 months at doses up to 25 × 10
6
IU/kg/day (see ribavirin package insert).
Pregnancy
Category C
Peginterferon alfa-2a has not been studied for
its teratogenic effect. Non-pegylated interferon alfa-2a treatment of pregnant
Rhesus monkeys at approximately 20-500 times the human weekly dose resulted in
a statistically significant increase in abortions. No teratogenic effects were
seen in the offspring delivered at term. Peginterferon alfa-2a should be
assumed to have abortifacient potential. There are no adequate and
well-controlled studies of peginterferon alfa-2a in pregnant women.
Peginterferon alfa-2a is to be used during pregnancy only if the potential
benefit justifies the potential risk to the fetus. Peginterferon alfa-2a is
recommended for use in women of childbearing potential only when they are using
effective contraception during therapy.
Pregnancy
Category X: Use With Ribavirin
Significant teratogenic and/or
embryocidal effects have been demonstrated in all animal species exposed to
ribavirin. Ribavirin therapy is contraindicated in women who are pregnant and
in the male partners of women who are pregnant (see CONTRAINDICATIONS,
WARNINGS, and the ribavirin package insert).
If pregnancy occurs in a patient or partner of
a patient during treatment or during the 6 months after treatment cessation,
such cases should be reported to the Copegus Pregnancy Registry at
1-800-526-6367.
Nursing
Mothers
It is not known whether peginterferon or
ribavirin or its components are excreted in human milk. The effect of orally
ingested peginterferon or ribavirin from breast milk on the nursing infant has
not been evaluated. Because of the potential for adverse reactions from the
drugs in nursing infants, a decision must be made whether to discontinue
nursing or discontinue peginterferon alfa-2a and ribavirin treatment.
Pediatric
Use
The safety and effectiveness of peginterferon
alfa-2a, alone or in combination with ribavirin in patients below the age of 18
years have not been established.
Peginterferon alfa-2a contains benzyl alcohol.
Benzyl alcohol has been reported to be associated with an increased incidence
of neurological and other complications in neonates and infants, which are
sometimes fatal (see CONTRAINDICATIONS).
Geriatric
Use
Younger patients have higher virologic
response rates than older patients. Clinical studies of peginterferon alfa-2a
alone or in combination with ribavirin did not include sufficient numbers of
subjects aged 65 or over to determine whether they respond differently from
younger subjects. Adverse reactions related to alpha interferons, such as CNS,
cardiac, and systemic (e.g., flu- like)
effects may be more severe in the elderly and caution should be exercised in
the use of peginterferon alfa-2a in this population. Peginterferon alfa-2a and
ribavirin are excreted by the kidney, and the risk of toxic reactions to this
therapy may be greater in patients with impaired renal function. Because
elderly patients are more likely to have decreased renal func tion, care should
be taken in dose selection and it may be useful to monitor renal function.
Peginterferon alfa-2a should be used with caution in patients with creatinine
clearance <50 ml/min and ribavirin should not be administered to patients
with creatinine clearance <50 ml/min.
Drug InteractionsTreatment with
peginterferon alfa-2a once weekly for 4 weeks in healthy subjects was
associated with an inhibition of P450 1A2 and a 25% increase in theophylline
AUC. Theophylline serum levels should be monitored and appropriate dose
adjustments considered for patients given both theophylline and peginterferon
alfa-2a (see PRECAUTIONS). There was no effect on the pharmacokinetics of
representative drugs metabolized by CYP 2C9, CYP 2C19, CYP 2D6 or CYP 3A4. In
patients with chronic hepatitis C treated with peginterferon alfa-2a in
combination with ribavirin, peginterferon alfa-2a treatment did not affect
ribavirin distribution or clearance.
Nucleoside
Analogues
Didanosine
Co-administration of ribavirin and didanosine
is not recommended. Reports of fatal hepatic failure, as well as peripheral
neuropathy, pancreatitis, and symptomatic hyperlactatemia/lactic acidosis have
been reported in clinical trials (see CLINICAL PHARMACOLOGY, Drug
Interactions).
Stavudine and
Zidovudine
Ribavirin can antagonize the in vitro
antiviral activity of stavudine and zidovudine against HIV. Therefore,
concomitant use of ribavirin with either of these drugs should be
avoided.
Adverse ReactionsPeginterferon alfa-2a
alone or in combination with ribavirin causes a broad variety of serious
adverse reactions (see BOXED WARNING and WARNINGS). In all studies, one or more
serious adverse reactions occurred in 10% of patients receiving peginterferon
alfa-2a alone or in combination with ribavirin.
The most common life-threatening or fatal
events induced or aggravated by peginterferon alfa-2a and ribavirin were
depression, suicide, relapse of drug abuse/overdose, and bacterial infections;
each occurred at a frequency of <1%.
Nearly all patients in clinical trials
experienced one or more adverse events. The most commonly reported adverse
reactions were psychiatric reactions, including depression, irritability,
anxiety, and flu-like symptoms such as fatigue, pyrexia, myalgia, headache and
rigors.
Overall 11% of patients receiving 48 weeks of
therapy with peginterferon alfa-2a either alone (7%) or in combination with
ribavirin (10%) discontinued therapy. The most common reasons for
discontinuation of therapy were psychiatric, flu-like syndrome (e.g., lethargy, fatigue, headache),
dermatologic and gastrointestinal disorders.
The most common reason for dose modification in
patients receiving combination therapy was for laboratory abnormalities;
neutropenia (20%) and thrombocytopenia (4%) for peginterferon alfa-2a and
anemia (22%) for ribavirin. Peginterferon alfa-2a dose was reduced in 12% of
patients receiving 1000-1200 mg ribavirin for 48 weeks and in 7% of patients
receiving 800 mg ribavirin for 24 weeks. ribavirin dose was reduced in 21% of
patients receiving 1000-1200 mg ribavirin for 48 weeks and 12% in patients
receiving 800 mg ribavirin for 24 weeks.
Because clinical trials are
conducted under widely varying and controlled conditions, adverse reaction
rates observed in clinical trials of a drug cannot be directly compared to
rates in the clinical trials of another drug. Also, the adverse event rates
listed here may not predict the rates observed in a broader patient population
in clinical practice.
TABLE 4 Adverse Reactions Occurring in ≥5% of
Patients in Hepatitis C Clinical Trials (Pooled Studies 1, 2, 3, and Study
4)
| |
|
Peginterferon alfa-2a
|
|
Peginterferon alfa-2a 180 µg
+ |
Intron A + |
| |
|
180 µg |
|
1000 mg or 1200 mg Copegus
|
1000 mg or 1200 mg Rebetol
|
| |
|
48 wk† |
Roferon-A*† |
48 wk‡ |
48 wk‡ |
| |
|
n=559 |
n=554 |
n=451 |
n=443 |
|
Application Site Disorders
|
| |
Injection site reaction |
22% |
18% |
23% |
16% |
|
Endocrine Disorders
|
| |
Hypothyroidism |
3% |
2% |
4% |
5% |
|
Flu-Like Symptoms and Signs
|
| |
Fatigue/asthenia |
56% |
57% |
65% |
68% |
| |
Pyrexia |
37% |
41% |
41% |
55% |
| |
Rigors |
35% |
44% |
25% |
37% |
| |
Pain |
11% |
12% |
10% |
9% |
|
Gastrointestinal |
| |
Nausea/vomiting |
24% |
33% |
25% |
29% |
| |
Diarrhea |
16% |
16% |
11% |
10% |
| |
Abdominal pain |
15% |
15% |
8% |
9% |
| |
Dry mouth |
6% |
3% |
4% |
7% |
| |
Dyspepsia |
<1% |
1% |
6% |
5% |
|
Hematologic
§ |
| |
Lymphopenia |
3% |
5% |
14% |
12% |
| |
Anemia |
2% |
1% |
11% |
11% |
| |
Neutropenia |
21% |
8% |
27% |
8% |
| |
Thrombocytopenia |
5% |
2% |
5% |
<1% |
|
Metobolic and Nutritional
|
| |
Anorexia |
17% |
17% |
24% |
26% |
| |
Weight decrease |
4% |
3% |
10% |
10% |
|
Musculoskeletal, Connective Tissue
and Bone |
| |
Myalgia |
37% |
38% |
40% |
49% |
| |
Arthralgia |
28% |
29% |
22% |
23% |
| |
Back pain |
9% |
10% |
5% |
5% |
|
Neurological |
| |
Headache |
54% |
58% |
43% |
49% |
| |
Dizziness (excluding vertigo)
|
16% |
12% |
14% |
14% |
| |
Memory impairment |
5% |
4% |
6% |
5% |
|
Psychiatric |
| |
Irritability/anxiety/nervousness
|
19% |
22% |
33% |
38% |
| |
Insomnia |
19% |
23% |
30% |
37% |
| |
Deprssion |
18% |
19% |
20% |
28% |
| |
Concentration impairment |
8% |
10% |
10% |
13% |
| |
Mood alteration |
3% |
2% |
5% |
6% |
|
Resistance Mechanism
Disorders |
| |
Overall |
10% |
6% |
12% |
10% |
|
Respiratory, Thoracic and
Mediastinal |
| |
Dyspnea |
4% |
2% |
13% |
14% |
| |
Cough |
4% |
3% |
10% |
7% |
| |
Dyspnea exertional |
<1% |
<1% |
4% |
7% |
|
Skin and Subcutaneous Tissue
|
| |
Alopecia |
23% |
30% |
28% |
33% |
| |
Pruritus |
12% |
8% |
19% |
18% |
| |
Dermatitis |
8% |
3% |
16% |
13% |
| |
Dry skin |
4% |
3% |
10% |
13% |
| |
Rash |
5% |
4% |
8% |
5% |
| |
Sweating increased |
6% |
7% |
6% |
5% |
| |
Eczema |
1% |
1% |
5% |
4% |
|
Visual Disorders |
| |
Vision blurred |
4% |
2% |
5% |
2% |
|
*
Pooled studies 1, 2, and 3. |
|
†
Either 3 MIU or 6/3 MIU of interferon
alfa-2b. |
|
‡
Study 4. |
|
§
Severe hematologic abnormalities.
|
Patients treated for 24 weeks with
peginterferon alfa-2a and 800 mg ribavirin were observed to have lower
incidence of serious adverse events (3% vs 10%), Hgb <10g/dl (3% vs 15%),
dose modification of peginterferon alfa-2a (30% vs 36%) and ribavirin (19% vs
38%) and of withdrawal from treatment (5% vs 15%) compared to patients treated
for 48 weeks with peginterferon alfa-2a and 1000 or 1200 mg ribavirin. On the
other hand the overall incidence of adverse events appeared to be similar in
the 2 treatment groups.
The most common serious adverse event (3%) was
bacterial infection (e.g., sepsis,
osteomyelitis, endocarditis, pyelonephritis, pneumonia). Other SAEs occurred at
a frequency of <1% and included: suicide, suicidal ideation, psychosis,
aggression, anxiety, drug abuse and drug overdose, angina, hepatic dysfunction,
fatty liver, cholangitis, arrhythmia, diabetes mellitus, autoimmune phenomena (
e.g., hyperthyroidism, hypothyroidism,
sarcoidosis, systemic lupus erythematosis, rheumatoid arthritis) peripheral
neuropathy, aplastic anemia, peptic ulcer, gastrointestinal bleeding,
pancreatitis, colitis, corneal ulcer, pulmo nary embolism, coma, myositis, and
cerebral hemorrhage.
Laboratory Test
Values
Hemoglobin
The hemoglobin concentration decreased below
12g/dl in 17% (median Hgb drop = 2.2 g/dl) of monotherapy and 52% (median Hgb
drop = 3.7 g/dl) of combination therapy patients. Severe anemia (Hgb <10
g/dl) was encountered in 13% of patients receiving combination therapy and 2%
of monotherapy recipients. Dose modification for anemia was required in 22% of
ribavirin recipients treated for 48 weeks. Hemoglobin decreases in
peginterferon alfa-2a monotherapy were generally mild and did not require dose
modification (see DOSAGE AND ADMINISTRATION, Dose Modification).
Neutrophils
Decreases in neutrophil count below normal
were observed in 95% of patients treated with peginterferon alfa-2a either
alone or in combination with ribavirin. Severe potentially life-threatening
neutropenia (ANC <0.5 × 10
9 /L)
occurred in approximately 5% of patients receiving peginterferon alfa-2a either
alone or in combination with ribavirin. Seventeen percent (17%) of patients
receiving peginterferon alfa-2a monotherapy and 20-24% of patients receiving
peginterferon alfa-2a/ribavirin combination therapy required modification of
interferon dosage for neutropenia. Two percent of patients required permanent
reductions of peginterferon alfa-2a dosage and <1% required permanent
discontinuation. Median neutrophil counts return to pre-treatment levels 4
weeks after cessation of therapy (see DOSAGE AND ADMINISTRATION, Dose
Modification).
Lymphocytes
Decreases in lymphocyte count are induced by
interferon alpha therapy. Lymphopenia was observed during both monotherapy
(86%) and combination therapy with peginterferon alfa-2a and ribavirin (94%).
Severe lymphopenia (<0.5 x 10
9 /L)
occurred in approximately 5% of monotherapy patients and 14% of combination
peginterferon alfa-2a and ribavirin therapy recipients. Dose adjustments were
not required by protocol. Median lymphocyte counts return to pre-treatment
levels after 4-12 weeks of the cessation of therapy. The clinical significance
of the lymphopenia is not known.
Platelets
Platelet counts decreased in 52% of patients
treated with peginterferon alfa-2a alone (median drop 45% from baseline), 33%
of patients receiving combination with ribavirin (median drop 30% from
baseline). Median platelet counts return to pretreatment levels 4 weeks after
the cessation of therapy.
Triglycerides
Triglyceride levels are elevated in patients
receiving alfa interferon therapy and were elevated in the majority of patients
participating in clinical studies receiving either peginterferon alfa-2a alone
or in combination with ribavirin. Random levels higher ≥400 mg/dl were
observed in about 20% of patients.
| 