Product Characteristics
ANNEX I
SUMMARY OF PRODUCT CHARACTERISTICS
NAME OF THE MEDICINAL PRODUCT
PegIntron 50 micrograms powder and solvent for solution for injection
QUALITATIVE AND QUANTITATIVE COMPOSITION
Each vial of PegIntron, powder contains 50 micrograms of peginterferon alfa-2b as measured on a protein
basis.
Each vial provides 50 micrograms/0.5 ml of peginterferon alfa-2b when reconstituted as recommended.
The active substance is a covalent conjugate of recombinant interferon alfa-2b* with monomethoxy
polyethylene glycol. The potency of this product should not be compared to that of another pegylated
or nonpegylated protein of the same therapeutic class (see section 5.1).
*produced by rDNA technology in
E.coli
cells harbouring a genetically engineered plasmid hybrid encompassing an interferon
alfa-2b gene from human leukocytes
Excipients:
PegIntron contains 40 mg of sucrose per 0.5 ml.
For a full list of excipients, see section 6.1.
Powder and solvent for solution for injection.
White powder.
Clear and colourless solvent.
4.1 Therapeutic indications
Adult patients:
PegIntron is indicated for the treatment of adult patients with chronic hepatitis C who are positive for
hepatitis C virus RNA (HCV-RNA), including patients with compensated cirrhosis and/or co-infected
with clinically stable HIV (see section 4.4).
The best way to use PegIntron in this indication is in combination with ribavirin.
This combination is indicated in naïve patients including patients with clinically stable HIV co-
infection and in patients who have failed previous treatment with interferon alpha (pegylated or
nonpegylated) and ribavirin combination therapy or interferon alpha monotherapy (see section 5.1).
Interferon monotherapy, including PegIntron, is indicated mainly in case of intolerance or
contraindication to ribavirin.
Paediatric patients 3 years of age and older:
PegIntron is indicated in a combination regimen with ribavirin for the treatment of children 3 years of
age and older and adolescents, who have chronic hepatitis C, not previously treated, without liver
decompensation, and who are positive for HCV-RNA.
When deciding not to defer treatment until adulthood, it is important to consider that the combination
therapy induced a growth inhibition. The reversibility of growth inhibition is uncertain. The decision
to treat should be made on a case by case basis (see section 4.4).
Please refer also to the ribavirin Summary of Product Characteristics (SPC) for capsules or oral
solution when PegIntron is to be used in combination with ribavirin.
4.2 Posology and method of administration
Treatment should be initiated and monitored only by a physician experienced in the management of
patients with hepatitis C.
•
Dose to be administered
PegIntron should be administered as a once weekly subcutaneous injection. The dose administered in
adults depends on whether it is used in combination with ribavirin or as monotherapy.
PegIntron and ribavirin combination therapy
PegIntron 1.5 micrograms/kg/week in combination with ribavirin capsules.
The intended dose of 1.5 μg/kg of PegIntron to be used in combination with ribavirin may be delivered
in weight categories with the pen/vial strengths according to
Table 1
. Ribavirin capsules are to be
administered orally each day in two divided doses with food (morning and evening).
Table 1 Dosing for combination therapy
Vial/Pen strength
(
μ
g/0.5ml)
Administer
once weekly
(ml)
Number of
capsules
(200 mg)
a: 2 morning, 2 evening
b: 2 morning, 3 evening
c: 3 morning, 3 evening
d: 3 morning, 4 evening
Duration of treatment – Naïve patients
Predictability of sustained virological response:
Patients infected with virus genotype 1 who fail to
achieve undetectable HCV-RNA or demonstrate adequate virological response at week 4 or 12 are
highly unlikely to become sustained virological responders and should be evaluated for
discontinuation (see also
section 5.1).
•
Genotype 1:
- Patients who have undetectable HCV-RNA at treatment week 12, treatment should be
continued for another nine month period (i.e., a total of 48 weeks).
- Patients with detectable but ≥ 2 log decrease in HCV-RNA level from baseline at treatment
week 12 should be reassessed at treatment week 24 and, if HCV-RNA is undetectable, they
should continue with full course of therapy (i.e. a total of 48 weeks). However, if HCV-RNA is
still detectable at treatment week 24, discontinuation of therapy should be considered.
- In the subset of patients with genotype 1 infection and low viral load (< 600,000 IU/ml) who
become HCV-RNA negative at treatment week 4 and remain HCV-RNA negative at week 24,
the treatment could either be stopped after this 24 week treatment course or pursued for an
additional 24 weeks (i.e. overall 48 weeks treatment duration). However, an overall 24 weeks
treatment duration may be associated with a higher risk of relapse than a 48 weeks treatment
duration (see section 5.1).
Genotypes 2 or 3:
It is recommended that all patients be treated for 24 weeks, except for HCV/HIV co-infected
patients who should receive 48 weeks of treatment.
Genotype 4:
In general, patients infected with genotype 4 are considered harder to treat and limited study
data (n=66) indicate they are compatible with a duration of treatment as for genotype 1.
Duration of treatment - HCV/HIV co-infection
The recommended duration of treatment for HCV/HIV co-infected patients is 48 weeks, regardless of
genotype.
Predictability of response and non-response in HCV/HIV co-infection
Early virological response by week 12, defined as a 2 log viral load decrease or undetectable levels of
HCV-RNA, has been shown to be predictive for sustained response. The negative predictive value for
sustained response in HCV/HIV co-infected patients treated with PegIntron in combination with
ribavirin was 99 % (67/68; Study 1) (see section 5.1). A positive predictive value of 50 % (52/104;
Study 1) was observed for HCV/HIV co-infected patients receiving combination therapy.
Duration of treatment - Retreatment
Predictability of sustained virological response
:
All patients, irrespective of genotype, who have
demonstrated serum HCV-RNA below the limits of detection at week 12 should receive 48 weeks of
therapy. Retreated patients who fail to achieve virological response (i.e. HCV-RNA below the limits
of detection) at week 12 are unlikely to become sustained virological responders after 48 weeks of
therapy (see also section 5.1).
Retreatment duration greater than 48
weeks in non
-
responder patients with genotype 1 has not been
studied with pegylated interferon alfa-2b and ribavirin combination therapy.
Paediatric patients 3 years of age and older :
Dosing for children and adolescent patients is determined by body surface area for PegIntron and by
body weight for ribavirin. The recommended dose of PegIntron is 60 μg/m
2
/week subcutaneously in
combination with ribavirin 15 mg/kg/day orally in two divided doses with food (morning and
evening).
Genotype 1:
The recommended duration of treatment is 1 year. By extrapolation from clinical data on
combination therapy with standard interferon in paediatric patients (negative predictive value
96 % for interferon alfa–2b/ribavirin), patients who fail to achieve virological response at 12
weeks are highly unlikely to become sustained virological responders. Therefore, it is
recommended that children and adolescent patients receiving PegIntron/ribavirin combination
be discontinued from therapy if their week 12 HCV-RNA dropped < 2 log
10
compared to
pretreatment or if they have detectable HCV-RNA at treatment week 24.
Genotype 2 or 3:
The recommended duration of treatment is 24 weeks.
Genotype 4:
Only 5 children and adolescents with Genotype 4 were treated in the PegIntron/ribavirin clinical
trial. The recommended duration of treatment is 1 year. It is recommended that children and
adolescent patients receiving PegIntron/ribavirin combination be discontinued from therapy if
their week 12 HCV-RNA dropped < 2 log
10
compared to pretreatment or if they have detectable
HCV-RNA at treatment week 24.
PegIntron monotherapy – Adults
As monotherapy the PegIntron regimen is 0.5 or 1.0 μg/kg/week. The lowest vial or pen strength
available is 50 μg/0.5 ml; therefore for patients prescribed 0.5 μg/kg/week,
doses must be adjusted by
volume as shown in
Table 2
. For the 1.0 μg/kg dose, similar volume adjustments can be made or
alternate vial strengths can be used as shown in
Table 2
. PegIntron monotherapy was not studied in
HCV/HIV co-infected patients.
Table 2 Monotherapy dosing
Vial/Pen
strength
(
μ
g/0.5ml)
Administer once
weekly
(ml)
Vial/Pen
strength
(
μ
g/0.5ml)
Administer once
weekly
(ml)
* Must use vial. Minimum delivery for pen is 0.3 ml.
** For patients > 120 kg, the PegIntron dose should be calculated based on the individual patient weight.
Duration of treatment
For patients who exhibit virological response at week 12, treatment should be continued for at least
another three-month period (i.e., a total of six months). The decision to extend therapy to one year of
treatment should be based on prognostic factors (e.g., genotype, age > 40 years, male gender, bridging
fibrosis).
•
Dose modification for all patients
If severe adverse reactions or laboratory abnormalities develop during treatment with PegIntron
monotherapy or PegIntron in combination with ribavirin, modify the
dosages of each product as
appropriate, until the adverse reactions abate. As adherence might be of importance for outcome of
therapy, the dose should be kept as close as possible to the recommended standard dose. Guidelines were
developed in clinical trials for dose modification.
Combination therapy dose reduction guidelines
Table 2a Dose modification guidelines for combination therapy (with ribavirin) based on
laboratory parameters
Laboratory values
Reduce only
ribavirin daily dose
(see note 1) if:
Reduce only PegIntron
dose (see note 2) if:
Discontinue
combination
therapy if:
Adults:Haemoglobin
in: Patients with
history of stable
cardiac disease
Children and
≥ 2 g/dl decrease in haemoglobin during any
four week period during treatment
(permanent dose reduction)
< 12 g/dl after four
weeks of dose
reduction
adolescents: not
applicable
Leukocytes
< 50 x 10
9
/l (adults)
<70 x 10
9
/l (children and
adolescents)
< 25 x 10
9
/l (adults)
< 50 x 10
9
/l
(children and
adolescents)
> 4 mg/dl
(for > 4 weeks)
Discontinue
ribavirin if
CrCL < 50ml/min
Alanine
aminotransferase
(ALT)
2 x baseline and
> 10 x ULN
*
2 x baseline and
> 10 x ULN
*
Aspartate
aminotransferase
(AST)
Note 1: In adult patients 1
st
dose reduction of ribavirin is by 200 mg/day (except in patients receiving
the 1,400 mg, dose reduction should be by 400 mg/day). If needed, 2
nd
dose reduction of
ribavirin is by an additional 200 mg/day. Patients whose dose of ribavirin
is reduced to
600 mg daily receive one 200 mg capsule in the morning and two 200 mg capsules in the
evening.
In children and adolescent patients 1
st
dose reduction of ribavirin is to 12 mg/kg/day, 2
nd
dose
reduction of ribavirin is to 8 mg/kg/day.
Note 2: In adult patients 1
st
dose reduction of PegIntron is to 1 µg/kg/week. If needed, 2
nd
dose
reduction of PegIntron is to 0.5 µg/kg/week. For patients on PegIntron monotherapy: refer to
monotherapy dose reduction guidelines section for dose reduction.
In children and adolescent patients 1
st
dose reduction of PegIntron is to 40 μg/m
2
/week, 2
nd
dose reduction of PegIntron is to 20 μg/m
2
/week.
Dose reduction of PegIntron in adults may be accomplished by reducing the prescribed volume or by
utilizing a lower dose strength as shown in
Table 2b
. Dose reduction of PegIntron in children and
adolescents is accomplished by modifying the recommended dose in a two-step process from the
original starting dose of 60 μg/m
2
/week, to 40 μg/m
2
/week, then to 20 μg/m
2
/week, if needed.
Table 2b Two-step dose reduction of PegIntron in combination therapy in adults
First dose reduction to PegIntron 1 µg/kg
Second dose reduction to PegIntron 0.5 µg/kg
PegIntron
strength
to use
Amount of
PegIntron
(µg) to
administer
Volume
(ml)
of
PegIntron
to
administer
PegIntron
strength to
use
Amount of
PegIntron
(µg) to
administer
Volume (ml)
of PegIntron
to
administer
* Must use vial. Minimum delivery for pen 0.3 ml
PegIntron monotherapy dose reduction guidelines in adults
Dose modification guidelines for adult patients who use PegIntron monotherapy are shown in
Table 3a.
Table 3a Dose modification guidelines for PegIntron monotherapy in adults
based on laboratory parameters
Laboratory values
Reduce PegIntron
to one-half dose if:
Discontinue PegIntron if:
Dose reduction for adult patients who use 0.5 μg/kg PegIntron monotherapy must be accomplished by
reducing the prescribed volume by one-half. The 50 μg/0.5 ml vial must be used if necessary since the
pen can only deliver a minimum volume of 0.3 ml.
For adult patients who use 1.0 μg/kg PegIntron monotherapy, dose reduction may be accomplished by
reducing the prescribed volume by one-half or by utilizing a lower dose strength as shown in
Table 3b
.
Table 3b Reduced PegIntron dose for the 1.0
μ
g/kg monotherapy regimen in adults
Target reduced
dose (
μ
g)
Vial/Pen
strength
(
μ
g/0.5ml)
Administer once
weekly
(ml)
*Must use vial. Minimum delivery for pen is 0.3 ml.
Use in renal impairment:
Monotherapy
:
PegIntron should be used with caution in patients with moderate to severe renal impairment. In patients
with moderate renal dysfunction (creatinine clearance 30-50 ml/minute), the starting dose of PegIntron
should be reduced by 25 %. Patients with severe renal dysfunction (creatinine clearance 15-
29 ml/minute) should have the starting dose of PegIntron reduced by 50 %. Data are not available for
the use of PegIntron in patients with creatinine clearance < 15 ml/minute (see section 5.2). Patients
with severe renal impairment, including those on hemodialysis, should be closely monitored. If renal
function decreases during treatment, PegIntron therapy should be discontinued.
Combination therapy
:
Patients with creatinine clearance < 50 ml/minute must not be treated with PegIntron in combination
with ribavirin (see ribavirin SPC). When administered in combination with ribavirin
,
subjects with
impaired renal function should be more carefully monitored with respect to the development of
anaemia.
Use in hepatic impairment:
The safety and efficacy of PegIntron therapy has not been evaluated in patients with severe hepatic
dysfunction, therefore PegIntron must not be used for these patients.
Use in the elderly (≥ 65 years of age):
There are no apparent age-related effects on the pharmacokinetics of PegIntron. Data from elderly patients
treated with a single dose of PegIntron suggest no alteration in PegIntron dose is necessary based on age
(see section 5.2).
Use in paediatric patients:
PegIntron can be used in combination with ribavirin in paediatric patients 3 years of age and older.
Hypersensitivity to the active substance or to any interferon or to any of the excipients;
A history of severe pre-existing cardiac disease, including unstable or uncontrolled cardiac disease
in the previous six months (see section 4.4);
Severe, debilitating medical conditions;
Autoimmune hepatitis or a history of autoimmune disease;
Severe hepatic dysfunction or decompensated cirrhosis of the liver;
Pre-existing thyroid disease unless it can be controlled with conventional treatment;
Epilepsy and/or compromised central nervous system (CNS) function;
HCV/HIV patients with cirrhosis and a Child-Pugh score ≥ 6.
Existence of, or history of severe psychiatric condition, particularly severe depression, suicidal
ideation or suicidal attempt.
Combination therapy with ribavirin
: Also see ribavirin Summary of the Product Characteristics (SPC)
if PegIntron is to be administered in combination with ribavirin in patients with chronic hepatitis C.
4.4 Special warnings and precautions for use
Psychiatric and Central Nervous System (CNS)
:
Severe CNS effects, particularly depression, suicidal ideation and attempted suicide have been observed in
some patients during PegIntron therapy, and even after treatment discontinuation mainly during the 6-
month follow-up period. Other CNS effects including aggressive behaviour (sometimes directed against
others such as homicidal ideation), bipolar disorders, mania, confusion and alterations of mental status
have been observed with alpha interferons. Patients should be closely monitored for any signs or
symptoms of psychiatric disorders. If such symptoms appear, the potential seriousness of these
undesirable effects must be borne in mind by the prescribing physician and the need for adequate
therapeutic management should be considered. If psychiatric symptoms persist or worsen, or suicidal
ideation is identified, it is recommended that treatment with PegIntron be discontinued, and the patient
followed, with psychiatric intervention as appropriate.
Patients with existence of, or history of severe psychiatric conditions:
If treatment with peginterferon
alfa-2b is judged necessary in patients with existence or history of severe psychiatric conditions, this
should only be initiated after having ensured appropriate individualised diagnostic and therapeutic
management of the psychiatric condition.
- The use of PegIntron in children and adolescents with existence of or history of severe psychiatric
conditions is contraindicated (see section 4.3). Among children and adolescents treated with interferon
alfa-2b in combination with ribavirin, suicidal ideation or attempts were reported more frequently
compared to adult patients (2.4 % vs 1 %) during treatment and during the 6-month follow-up after
treatment. As in adult patients, children and adolescents experienced other psychiatric adverse events
(e.g. depression, emotional lability, and somnolence).
Growth and development (children and adolescents):
During the course of therapy lasting up to 48 weeks in patients ages 3 through 17 years, weight loss
and growth inhibition were common (see sections 4.8 and 5.1). The longer term data available in
children treated with the combination therapy with standard interferon/ribavirin are also indicative of
substantial growth retardation (> 15 percentile decrease in height percentile as compared to baseline)
in 21 % of children despite being off treatment for more than 5 years.
Case by case benefit/risk assessment in children:
The expected benefit of treatment should be carefully weighed against the safety findings observed for
children and adolescents in the clinical trials (see sections 4.8 and 5.1).
-
It is important to consider that the combination therapy induced a growth inhibition, the
reversibility of which is uncertain.
This risk should be weighed against the disease characteristics of the child, such as evidence
of disease progression (notably fibrosis), co-morbidities that may negatively influence the
disease progression (such as HIV co-infection), as well as prognostic factors of response (HCV
genotype and viral load).
Whenever possible the child should be treated after the pubertal growth spurt, in order to reduce the
risk of growth inhibition. There are no data on long term effects on sexual maturation.
More significant obtundation and coma, including cases of encephalopathy, have been observed in
some patients, usually elderly, treated at higher doses for oncology indications. While these effects are
generally reversible, in a few patients full resolution took up to three weeks. Very rarely, seizures have
occurred with high doses of interferon alpha.
All patients in the selected chronic hepatitis C studies had a liver biopsy before inclusion, but in certain
cases (i.e. patients with genotype 2 and 3), treatment may be possible without histological confirmation.
Current treatment guidelines should be consulted as to whether a liver biopsy is needed prior to
commencing treatment.
Acute hypersensitivity
: Acute hypersensitivity reactions (e.g., urticaria, angioedema,
bronchoconstriction, anaphylaxis) have been observed rarely during interferon alfa-2b therapy. If such a
reaction develops during treatment with PegIntron, discontinue treatment and institute appropriate medical
therapy immediately. Transient rashes do not necessitate interruption of treatment.
Cardiovascular system
: As with interferon alfa-2b, adult patients with a history of congestive heart failure,
myocardial infarction and/or previous or current arrhythmic disorders, receiving PegIntron therapy require
close monitoring. It is recommended that patients who have pre-existing cardiac abnormalities have
electrocardiograms taken prior to and during the course of treatment. Cardiac arrhythmias (primarily
supraventricular) usually respond to conventional therapy but may require discontinuation of PegIntron
therapy. There are no data in children or adolescents with a history of cardiac disease.
Liver function
: As with all interferons
,
discontinue treatment with PegIntron in patients who develop
prolongation of coagulation markers which might indicate liver decompensation.
Pyrexia
: While pyrexia may be associated with the flu-like syndrome reported commonly during
interferon therapy, other causes of persistent pyrexia must be ruled out.
Hydration
: Adequate hydration must be maintained in patients undergoing PegIntron therapy since
hypotension related to fluid depletion has been seen in some patients treated with alpha interferons.
Fluid replacement may be necessary.
Pulmonary changes
: Pulmonary infiltrates, pneumonitis, and pneumonia, occasionally resulting in fatality,
have been observed rarely in interferon alpha treated patients. Any patient developing pyrexia, cough,
dyspnea or other respiratory symptoms must have a chest X-ray taken. If the chest X-ray shows
pulmonary infiltrates or there is evidence of pulmonary function impairment, the patient is to be
monitored closely, and, if appropriate, discontinue interferon alpha. Prompt discontinuation of interferon
alpha administration and treatment with corticosteroids appear to be associated with resolution of
pulmonary adverse events.
Autoimmune disease
: The development of auto-antibodies and autoimmune disorders has been
reported during treatment with alpha interferons. Patients predisposed to the development of
autoimmune disorders may be at increased risk. Patients with signs or symptoms compatible with
autoimmune disorders should be evaluated carefully, and the benefit-risk of continued interferon
therapy should be reassessed (see also section 4.4 Thyroid changes and section 4.8).
Cases of Vogt-Koyanagi-Harada (VKH) syndrome have been reported in patients with chronic
hepatitis C treated with interferon. This syndrome is a granulomatous inflammatory disorder affecting
the eyes, auditory system, meninges, and skin. If VKH syndrome is suspected, antiviral treatment
should be withdrawn and corticosteroid therapy discussed (see section 4.8).
Ocular changes
: Ophthalmologic disorders, including retinal haemorrhages, retinal exudates, and retinal
artery or vein occlusion have been reported in rare instances after treatment with alpha interferons
(see section 4.8). All patients should have a baseline eye examination. Any patient complaining of ocular
symptoms, including loss of visual acuity or visual field must have a prompt and complete eye
examination. Periodic visual examinations are recommended during PegIntron therapy, particularly in
patients with disorders that may be associated with retinopathy, such as diabetes mellitus or hypertension.
Discontinuation of PegIntron should be considered in patients who develop new or worsening
ophthalmological disorders.
Thyroid changes
:
Infrequently, adult patients treated for chronic hepatitis C with interferon alpha have
developed thyroid abnormalities, either hypothyroidism or hyperthyroidism. Approximately 21 % of
children treated with PegIntron/ribavirin combination therapy developed increase in thyroid
stimulating hormone (TSH). Another approximately 2 % had a transient decrease below the lower
limit of normal. Prior to initiation of PegIntron therapy, TSH levels must be evaluated and any thyroid
abnormality detected at that time must be treated with conventional therapy. Determine TSH levels if,
during the course of therapy, a patient develops symptoms consistent with possible thyroid
dysfunction. In the presence of thyroid dysfunction, PegIntron treatment may be continued if TSH
levels can be maintained in the normal range by medicine. Children and adolescents should be
monitored every 3 months for evidence of thyroid dysfunction (e.g. TSH).
Metabolic disturbances
: Hypertriglyceridemia and aggravation of hypertriglyceridemia, sometimes
severe, have been observed. Monitoring of lipid levels is, therefore, recommended.
HCV/HIV Co-infection
Mitochondrial toxicity and lactic acidosis:
Patients co-infected with HIV and receiving Highly Active Anti-Retroviral Therapy (HAART) may be
at increased risk of developing lactic acidosis. Caution should be used when adding PegIntron and
ribavirin to HAART therapy (see ribavirin SPC).
Hepatic decompensation in HCV/HIV co-infected patients with advanced cirrhosis:
Co-infected patients with advanced cirrhosis receiving HAART may be at increased risk of hepatic
decompensation and death. Adding treatment with alfa interferons alone or in combination with
ribavirin may increase the risk in this patient subset. Other baseline factors in co-infected patients that
may be associated with a higher risk of hepatic decompensation include treatment with didanosine and
elevated bilirubin serum concentration.
Co-infected patients receiving both antiretroviral (ARV) and anti-hepatitis treatment should be closely
monitored, assessing their Child-Pugh score during treatment.
Patients progressing to hepatic
decompensation should have their anti-hepatitis treatment immediately discontinued and the ARV
treatment reassessed.
Haematological abnormalities in HCV/HIV co-infected patients:
HCV/HIV co-infected patients receiving peginterferon alfa-2b/ribavirin treatment and HAART may
be at increased risk to develop haematological abnormalities (as neutropenia, thrombocytopenia and
anaemia) compared to HCV mono-infected patients. Although, the majority of them could be managed
by dose reduction, close monitoring of haematological parameters should be undertaken in this
population of patients (see section 4.2 and below “Laboratory tests” and section 4.8).
Patients treated with PegIntron and ribavirin combination therapy and zidovudine are at increased risk
of developing anaemia and therefore the concomitant use of this combination with zidovudine is not
recommended (see section 4.5).
Patients with low CD4 counts:
In patients co-infected with HCV/HIV, limited efficacy and safety data (N = 25) are available in
subjects with CD4 counts less than 200 cells/µl. Caution is therefore warranted in the treatment of
patients with low CD4 counts.
Please refer to the respective Summary of Product Characteristics of the antiretroviral medicinal
products that are to be taken concurrently with HCV therapy for awareness and management of
toxicities specific for each product and the potential for overlapping toxicities with PegIntron and
ribavirin.
Dental and periodontal disorders
: Dental and periodontal disorders, which may lead to loss of teeth,
have been reported in patients receiving PegIntron and ribavirin
combination therapy. In addition, dry
mouth could have a damaging effect on teeth and mucous membranes of the mouth during long-term
treatment with the combination of PegIntron and ribavirin. Patients should brush their teeth thoroughly
twice daily and have regular dental examinations. In addition some patients may experience vomiting.
If this reaction occurs, they should be advised to rinse out their mouth thoroughly afterwards.
Organ transplant recipients
:
The safety and efficacy of PegIntron alone or in combination with
ribavirin for the treatment of hepatitis C in liver or other organ transplant recipients have not been
studied. Preliminary data indicate that interferon alpha therapy may be associated with an increased
rate of kidney graft rejection. Liver graft rejection has also been reported.
Other
: Due to reports of interferon alpha exacerbating pre-existing psoriatic disease and sarcoidosis, use
of PegIntron in patients with psoriasis or sarcoidosis is recommended only if the potential benefit justifies
the potential risk.
Laboratory tests
: Standard haematologic tests, blood chemistry and a test of thyroid function must be
conducted in all patients prior to initiating therapy. Acceptable baseline values that may be considered as a
guideline prior to initiation of PegIntron therapy are:
must be within normal limits
Laboratory evaluations are to be conducted at weeks 2 and 4 of therapy, and periodically thereafter as
clinically appropriate. HCV-RNA should be measured periodically during treatment (see section 4.2).
Important information about some of the ingredients of PegIntron:
Patients with rare hereditary problems of fructose intolerance, glucose galactose malabsorption or sucrase-
isomaltase insufficiency should not take this medicine.
This medicinal product contains less than 1 mmol sodium (23 mg) per 0.7 ml, i.e., essentially
"sodium-free".
4.5 Interaction with other medicinal products and other forms of interaction
Results from a multiple-dose probe study assessing P450 substrates in chronic hepatitis C patients
receiving once weekly PegIntron (1.5 µg/kg) for 4 weeks demonstrated an increase in activity of
CYP2D6 and CYP2C8/9. No change in activity of CYP1A2, CYP3A4, or N-acetyltransferase was
observed.
Caution should be used when administering peginterferon alfa-2b with medicines metabolised by
CYP2D6 and CYP2C8/9, especially those with narrow therapeutic window, such as warfarin and
phenytoin (CYP2C9) and flecainide (CYP2D6).
These findings may partly relate to improved metabolic capacity due to reduced hepatic inflammation
in patients undergoing treatment with PegIntron. Caution is therefore advised when PegIntron
treatment is initiated for chronic hepatitis in patients treated with medicine with a narrow therapeutic
window and sensitive to mild metabolic impairment of the liver.
No pharmacokinetic interactions were noted between PegIntron and ribavirin in a multiple-dose
pharmacokinetic study.
Methadone:
In patients with chronic hepatitis C that were on stable methadone maintenance therapy and naïve to
peginterferon alfa-2b, addition of 1.5 microgram/kg/week of PegIntron subcutaneously for 4 weeks
increased R-methadone AUC by approximately 15 % (95 % Cl for AUC ratio estimate 103 – 128 %).
The clinical significance of this finding is unknown; however, patients should be monitored for signs
and symptoms of increased sedative effect, as well as respiratory depression. Especially in patients on
a high dose of methadone, the risk for QTc prolongation should be considered.
HCV/HIV Co-infection:
Nucleoside analogs: Use of nucleoside analogs, alone or in combination with other nucleosides, has
resulted in lactic acidosis. Pharmacologically, ribavirin increases phosphorylated metabolites of purine
nucleosides
in vitro
. This activity could potentiate the risk of lactic acidosis induced by purine
nucleoside analogs (e.g. didanosine or abacavir). Co-administration of ribavirin and didanosine is not
recommended. Reports of mitochondrial toxicity, in particular lactic acidosis and pancreatitis, of
which some fatal, have been reported (see ribavirin SPC).
Exacerbation of anaemia due to ribavirin has been reported when zidovudine is part of the regimen
used to treat HIV, although the exact mechanism remains to be elucidated. The concomitant use of
ribavirin with zidovudine is not recommended due to an increased risk of anaemia (see section 4.4).
Consideration should be given to replacing zidovudine in a combination anti-retroviral treatment
(ART) regimen if this is already established. This would be particularly important in patients with a
known history of zidovudine-induced anaemia.
4.6 Fertility, pregnancy and lactation
Women of childbearing potential/contraception in males and females
PegIntron is recommended for use in fertile women only when they are using effective contraception
during the treatment.
Combination therapy with ribavirin:
Extreme care must be taken to avoid pregnancy in female patients or in partners of male patients taking
PegIntron in combination with ribavirin. Females of childbearing potential and their partners must each
use an effective contraceptive during treatment and for 4 months after treatment has been concluded. Male
patients and their female partners must each use an effective contraceptive during treatment and for 7
months after treatment has been concluded (see ribavirin SPC).
Pregnancy
There are no adequate data from the use of interferon alfa-2b in pregnant women. Studies in animals have
shown reproductive toxicity (see section 5.3). Interferon alfa-2b has been shown to be abortifacient in
primates. PegIntron is likely to also cause this effect.
The potential risk in humans is unknown. PegIntron is to be used during pregnancy only if the potential
benefit justifies the potential risk to the foetus.
Combination therapy with ribavirin:
Ribavirin causes serious birth defects when administered during pregnancy, therefore
ribavirin therapy is
contraindicated in women who are pregnant.
Breast-feeding
It is not known whether the components of this medicinal product are excreted in human milk.
Because of the potential for adverse reactions in breast-fed infants, breast-feeding should be
discontinued prior to initiation of treatment.
4.7 Effects on ability to drive and use machines
Patients who develop fatigue, somnolence or confusion during treatment with PegIntron are cautioned to
avoid driving or operating machines.
Adults
The most common treatment-related adverse reactions reported during clinical trials with PegIntron in
combination with ribavirin in adults, seen in more than half of the study subjects, were fatigue,
headache, and injection site reaction. Additional adverse reactions reported in more than 25 % of
subjects included nausea, chills, insomnia, anaemia, pyrexia, myalgia, asthenia, pain, alopecia,
anorexia, weight decreased, depression, rash and irritability. The most frequently reported adverse
reactions were mostly mild to moderate in severity and were manageable without the need for
modification of doses or discontinuation of therapy. Fatigue, alopecia, pruritus, nausea, anorexia,
weight decreased, irritability and insomnia occur at a notably lower rate in patients treated with
PegIntron monotherapy compared to those treated with combination therapy (see
Table 4
).
The following treatment-related adverse reactions were reported in clinical trials or through post-
marketing surveillance in patients treated with peginterferon alfa-2b, including PegIntron monotherapy
or PegIntron/ribavirin. These reactions are listed in
table 4
by system organ class and frequency (very
common (≥ 1/10), common (≥ 1/100 to < 1/10), uncommon (≥ 1/1,000 to < 1/100), rare (≥ 1/10,000 to
< 1/1,000), very rare (< 1/10,000) or not known (cannot be estimated from the available data).
Within each frequency grouping, undesirable effects are presented in order of decreasing seriousness.
Table 4 Adverse reactions reported in clinical trials or through post-marketing
surveillance in patients treated with peginterferon alfa-2b, including PegIntron
monotherapy or PegIntron + ribavirin
Infections and infestations
Very common:
Viral infection
*
,
pharyngitis
*
Bacterial infection (including sepsis), fungal infection, influenza, upper
respiratory tract infection, bronchitis, herpes simplex, sinusitis, otitis
media, rhinitis
Injection site infection, lower respiratory tract infection
Blood and lymphatic system disorders
Very common: Anaemia, neutropenia
Common: Haemolytic anaemia, leukopenia, thrombocytopenia, lymphadenopathy
Very rare: Aplastic anaemia
Not known: Aplasia pure red cell
Immune system disorders
Uncommon:
Acute hypersensitivity reactions including angioedema, anaphylaxis
and anaphylactic reactions including anaphylactic shock, idiopathic
thrombocytopenic purpura, thrombotic thrombocytopenic purpura,
systemic lupus erythematosus
Endocrine disorders
Common: Hypothyroidism, hyperthyroidism
Metabolism and nutrition disorders
Very common:
Hypocalcemia, hyperuricemia, dehydration, increased appetite
Diabetes mellitus, hypertriglyceridaemia
Psychiatric disorders
Very common: Depression, anxiety
*
, emotional lability
*
,
concentration impaired,
insomnia
Common: Aggression, agitation, anger, mood altered, abnormal behaviour,
nervousness, sleep disorder, libido decreased, apathy, abnormal dreams,
crying
Uncommon: Suicide, suicide attempt, suicidal ideation, psychosis, hallucination,
panic attack
Rare: Bipolar disorders
Not known: Homicidal ideation, mania
Nervous system disorders
Very common:
Amnesia, memory impairment, syncope, migraine, ataxia, confusion,
neuralgia, paraesthesia, hypoaesthesia, hyperaesthesia, hypertonia,
somnolence, disturbance in attention, tremor, dysgeusia
Neuropathy, neuropathy peripheral
Cerebrovascular haemorrhage, cerebrovascular ischaemia,
encephalopathy
Facial palsy, mononeuropathies
Common: Visual disturbance, vision blurred, photophobia, conjunctivitis, eye
irritation, lacrimal disorder, eye pain, dry eye
Uncommon: Retinal exudates
Rare: Loss of visual acuity or visual fields, retinal haemorrhage, retinopathy,
retinal artery occlusion, retinal vein occlusion, optic neuritis,
papilloedema, macular oedema
Ear and labyrinth disorders
Common:
Hearing impaired/loss, tinnitus, vertigo
Cardiac disorders
Common:
Palpitations, tachycardia
Congestive heart failure, cardiomyopathy, arrhythmia, pericarditis
Vascular disorders
Common: Hypotension, hypertension, flushing
Rare: Vasculitis
Respiratory, thoracic and mediastinal disorders
Very common: Dyspnoea
*
, cough
*
Common: Dysphonia, epistaxis, respiratory disorder, respiratory tract congestion,
sinus congestion, nasal congestion, rhinorrhea, increased upper airway
secretion, pharyngolaryngeal pain
Very rare: Interstitial lung disease
Gastrointestinal disorders
Very common:
Vomiting
*
, nausea, abdominal pain, diarrhoea, dry mouth*
Dyspepsia, gastroesophageal reflux disease, stomatitis, mouth
ulceration, glossodynia, gingival bleeding, constipation, flatulence,
haemorrhoids, cheilitis, abdominal distension, gingivitis, glossitis, tooth
disorder
Hepatobiliary disorders
Common: Hyperbilirubinemia, hepatomegaly
Skin and subcutaneous tissue disorders
Very common:
Alopecia, pruritus
*
, dry skin
*
, rash
*
Psoriasis, photosensitivity reaction, rash maculo-papular, dermatitis,
erythematous rash, eczema, night sweats, hyperhidrosis, acne, furuncle,
erythema, urticaria, abnormal hair texture, nail disorder
Rare: Cutaneous sarcoidosis
Very rare: Stevens-Johnson syndrome, toxic epidermal necrolysis, erythema
multiforme
Musculoskeletal and connective tissue disorders
Very common: Myalgia, arthralgia, musculoskeletal pain
Common: Arthritis, back pain, muscle spasms, pain in extremity
Uncommon: Bone pain, muscle weakness
Rare: Rhabdomyolysis, myositis, rheumatoid arthritis
Renal and urinary disorders
Common:
Micturition frequency, polyuria, urine abnormality
Renal failure, renal insufficiency
Reproductive system and breast disorders
Common: Amenorrhoea, breast pain, menorrhagia, menstrual disorder, ovarian
disorder, vaginal disorder, sexual dysfunction, prostatitis, erectile
dysfunction
General disorders and administration site conditions
Very common:
Injection site reaction
*
,
injection site inflammation, fatigue, asthenia,
irritability, chills, pyrexia, influenza like illness, pain
Chest pain, chest discomfort, injection site pain, malaise, face oedema,
oedema peripheral, feeling abnormal, thirst
Investigations
Very common:
Weight decreased
*
These adverse reactions were common (
≥
1/100 to < 1/10) in clinical trials in patients treated with PegIntron monotherapy.
Most cases of neutropenia and thrombocytopenia were mild (WHO grades 1 or 2). There were some cases
of more severe neutropenia in patients treated with the recommended doses of PegIntron in combination
with ribavirin (WHO grade 3: 39 of 186 [21 %]; and WHO grade 4: 13 of 186 [7 %]).
In a clinical trial, approximately 1.2 % of patients treated with PegIntron or interferon alfa-2b in
combination with ribavirin reported life-threatening psychiatric events during treatment. These events
included suicidal ideation and attempted suicide (see section 4.4).
Cardiovascular (CVS) adverse events, particularly arrhythmia, appeared to be correlated mostly with
pre-existing CVS disease and prior therapy with cardiotoxic agents (see section 4.4). Cardiomyopathy,
that may be reversible upon discontinuation of interferon alpha, has been reported rarely in patients
without prior evidence of cardiac disease.
Ophthalmological disorders that have been reported rarely with alpha interferons include retinopathies
(including macular oedema), retinal haemorrhages, retinal artery or vein occlusion, retinal exudates,
loss of visual acuity or visual field, optic neuritis, and papilloedema (see section 4.4).
A wide variety of autoimmune and immune-mediated disorders have been reported with alpha interferons
including thyroid disorders, systemic lupus erythematosus, rheumatoid arthritis (new or aggravated),
idiopathic and thrombotic thrombocytopenic purpura, vasculitis, neuropathies including
mononeuropathies and Vogt-Koyanagi-Harada syndrome (see also section 4.4, Autoimmune
disorders).
HCV/HIV co-infected patients
For HCV/HIV co-infected patients receiving PegIntron in combination with ribavirin, other
undesirable effects (that were not reported in mono-infected patients) which have been reported in the
larger studies with a frequency > 5 % were: oral candidiasis (14 %), lipodystrophy acquired (13 %),
CD4 lymphocytes decreased (8 %), appetite decreased (8 %), gamma-glutamyltransferase increased
(9 %), back pain (5 %), blood amylase increased (6 %), blood lactic acid increased (5 %), cytolytic
hepatitis (6 %), lipase increased (6 %) and pain in limb (6 %).
Mitochondrial toxicity:
Mitochondrial toxicity and lactic acidosis have been reported in HIV-positive patients receiving NRTI
regimen and associated ribavirin for co-HCV infection (see section 4.4).
Laboratory values for HCV/HIV co-infected patients:
Although haematological toxicities of neutropenia, thrombocytopenia and anaemia occurred more
frequently in HCV/HIV co-infected patients, the majority could be managed by dose modification and
rarely required premature discontinuation of treatment (see section 4.4). Haematological abnormalities
were more frequently reported in patients receiving PegIntron in combination with ribavirin when
compared to patients receiving interferon alfa-2b in combination with ribavirin
.
In Study 1 (see section
5.1), decrease in absolute neutrophil count levels below 500 cells/mm
3
was observed in 4 % (8/194) of
patients and decrease in platelets below 50,000/mm
3
was observed in 4 % (8/194) of patients receiving
PegIntron in combination with ribavirin. Anaemia (hemoglobin < 9.4g/dl) was reported in 12%
(23/194) of patients treated with PegIntron in combination with ribavirin.
CD4 lymphocytes decrease:
Treatment with PegIntron in combination with ribavirin was associated with decreases in absolute
CD4+ cell counts within the first 4 weeks without a reduction in CD4+ cell percentage. The decrease
in CD4+ cell counts was reversible upon dose reduction or cessation of therapy. The use of PegIntron
in combination with ribavirin had no observable negative impact on the control of HIV viraemia
during therapy or follow-up. Limited safety data (N= 25) are available in co-infected patients with
CD4+ cell counts < 200/µl (see section 4.4).
Please refer to the respective Summary of Product Characteristics of the antiretroviral medicinal products
that are to be taken concurrently with HCV therapy for awareness and management of toxicities specific
for each product and the potential for overlapping toxicities with PegIntron in combination with ribavirin.
Paediatric patients
In a clinical trial with 107 children and adolescent patients (3 to 17 years of age) treated with combination
therapy of PegIntron and ribavirin, dose modifications were required in 25 % of patients, most commonly
for anaemia, neutropenia and weight loss. In general, the adverse reactions profile in children and
adolescents was similar to that observed in adults, although there is a paediatric-specific concern
regarding growth inhibition. During combination therapy for up to 48 weeks with PegIntron and ribavirin,
growth inhibition is observed, the reversibility of which is uncertain (see section 4.4). Weight loss and
growth inhibition were very common during the treatment (at the end of treatment, mean decrease from
baseline in weight and height percentile were of 15 percentiles and 8 percentiles, respectively) and growth
velocity was inhibited (< 3
rd
percentile in 70 % of the patients).
At the end of 24 weeks post-treatment follow-up, mean decrease from baseline in weight and height
percentiles were still of 3 percentiles and 7 percentiles respectively, and 20 % of the children
continued to have inhibited growth (growth velocity < 3
rd
percentile). Based on interim data from the
long-term follow-up portion of this study, 22 % (16/74) of children had a >15 percentile decrease in
height percentile, of whom 3 (4 %) children had a > 30 percentile decrease despite being off treatment
for more than 1 year. In particular, decrease in mean height percentile at year 1 of long-term follow-up
was most prominent in prepubertal age children (see section 4.4).
In this study, the most prevalent adverse reactions in all subjects were pyrexia (80 %), headache (62 %),
neutropenia (33 %), fatigue (30 %), anorexia (29 %) and injection-site erythema (29 %). Only 1 subject
discontinued therapy as the result of an adverse reaction (thrombocytopenia). The majority of adverse
reactions reported in the study were mild or moderate in severity. Severe adverse reactions were reported
in 7 % (8/107) of all subjects and included injection site pain (1 %), pain in extremity (1 %), headache
(1 %), neutropenia (1 %), and pyrexia (4 %). Important treatment-emergent adverse reactions that
occurred in this patient population were nervousness (8 %), aggression (3 %), anger (2 %),
depression/depressed mood (4 %) and hypothyroidism (3 %) and 5 subjects received levothyroxine
treatment for hypothyroidism/elevated TSH.
The following treatment-related adverse reactions were reported in the study in children and
adolescent patients treated with PegIntron in combination with ribavirin. These reactions are listed in
Table 5
by system organ class and frequency (very common (≥ 1/10), common (≥ 1/100 to < 1/10),
uncommon (≥ 1/1,000 to < 1/100), rare (≥ 1/10,000 to < 1/1,000), very rare (< 1/10,000) or not known
(cannot be estimated from the available data).
Within each frequency grouping, adverse reactions are presented in order of decreasing seriousness.
Table 5 Adverse reactions very commonly, commonly and uncommonly reported in the
clinical trial in children and adolescent patients treated with PegIntron in
combination with ribavirin
Infections and infestations
Common:
Fungal infection, influenza, oral herpes, otitis media, pharyngitis
streptococcal, nasopharyngitis, sinusitis
Uncommon: Pneumonia, ascariasis, enterobiasis, herpes zoster, cellulitis, urinary
tract infection, gastroenteritis
Blood and lymphatic system disorders
Very common:
Anaemia, leucopenia, neutropenia
Thrombocytopenia, lymphadenopathy
Endocrine disorders
Common: Hypothyroidism
Metabolism and nutrition disorders
Very common:
Anorexia, decreased appetite
Psychiatric disorders
Common: Suicidal ideation
§
, suicide attempt
§
, depression, aggression, affect
lability, anger, agitation, anxiety, mood altered, restlessness,
nervousness, insomnia
Uncommon: Abnormal behaviour, depressed mood, emotional disorder, fear,
nightmare
Nervous system disorders
Very common:
Dysgeusia, syncope, disturbance in attention, somnolence, poor quality
sleep
Neuralgia, lethargy, paraesthesia, hypoaesthesia, psychomotor
hyperactivity, tremor
Eye disorders
Common: Eye pain
Uncommon: Conjunctival haemorrhage, eye pruritus, keratitis, vision blurred,
photophobia
Ear and labyrinth disorders
Common:
Cardiac disorders
Common:
Palpitations, tachycardia
Vascular disorders
Common: Flushing
Uncommon: Hypotension, pallor
Respiratory, thoracic and mediastinal disorders
Common: Cough, epistaxis, pharyngolaryngeal pain
Uncommon: Wheezing, nasal discomfort, rhinorrhoea
Gastrointestinal disorders
Very common:
Abdominal pain, abdominal pain upper, vomiting, nausea
Diarrhoea, aphthous stomatitis, cheilosis, mouth ulceration, stomach
discomfort, oral pain
Hepatobiliary disorders
Uncommon: Hepatomagaly
Skin and subcutaneous tissue disorders
Very common:
Pruritus, rash, rash erythematous, eczema, acne, erythema
Uncommon: Photosensitivity reaction, rash maculo-papular, skin exfoliation,
pigmentation disorder, dermatitis atopic, skin discolouration
Musculoskeletal and connective tissue disorders
Very common:
Common: Musculoskeletal pain, pain in extremity, back pain
Uncommon: Muscle contracture, muscle twitching
Renal and urinary disorders
Uncommon: Proteinuria
Reproductive system and breast disorders
Uncommon:
General disorders and administration site conditions
Very common:
Injection site erythema, fatigue, pyrexia, rigors, influenza-like illness,
asthenia, pain, malaise, irritability
Injection site reaction, injection site pruritus, injection site rash
injection site dryness, injection site pain, feeling cold
Chest pain, chest discomfort, facial pain
Investigations
Very common:
Growth rate decrease (height and/or weight decrease for age)
Blood thyroid stimulating hormone increased, thyroglobulin increased
Anti-thyroid antibody positive
Injury and poisoning
Uncommon:
Contusion
§
class effect of interferon-alfa containing products – reported with standard interferon therapy in adult and paediatric
patients; with PegIntron reported in adult patients.
Most of the changes in laboratory values in the PegIntron/ribavirin clinical trial were mild or
moderate. Decreases in haemoglobin, white blood cells, platelets, neutrophils and increase in bilirubin
may require dose reduction or permanent discontinuation from therapy (see section 4.2). While
changes in laboratory values were observed in some patients treated with PegIntron used in
combination with ribavirin in the clinical trial, values returned to baseline levels within a few weeks
after the end of therapy.
Doses up to 10.5 times the intended dose have been reported. The maximum daily dose reported is
1,200 µg for one day. In general, the adverse events seen in overdose cases involving PegIntron are
consistent with the known safety profile for PegIntron; however, the severity of the events may be
increased. Standard methods to increase elimination of the medicinal product, e.g., dialysis, have not
been shown to be useful. No specific antidote for PegIntron is available; therefore, symptomatic
treatment and close observation of the patient are recommended in cases of overdose. If available,
prescribers are advised to consult with a poison control centre (PCC).
PHARMACOLOGICAL PROPERTIES
5.1
Pharmacodynamic properties
Pharmacotherapeutic group: Interferons, ATC code: L03AB10.
Recombinant interferon alfa-2b is covalently conjugated with monomethoxy polyethylene glycol at an
average degree of substitution of 1 mole of polymer/mole of protein. The average molecular mass is
approximately 31,300 daltons of which the protein moiety constitutes approximately 19,300.
•
Interferon alfa-2b
In vitro
and
in vivo
studies suggest that the biological activity of PegIntron is derived from its interferon
alfa-2b moiety.
Interferons exert their cellular activities by binding to specific membrane receptors on the cell surface.
Studies with other interferons have demonstrated species specificity. However, certain monkey
species, e.g., Rhesus monkeys are susceptible to pharmacodynamic stimulation upon exposure to
human type 1 interferons.
Once bound to the cell membrane, interferon initiates a complex sequence of intracellular events that
include the induction of certain enzymes. It is thought that this process, at least in part, is responsible
for the various cellular responses to interferon, including inhibition of virus replication in virus-
infected cells, suppression of cell proliferation and such immunomodulating activities as enhancement
of the phagocytic activity of macrophages and augmentation of the specific cytotoxicity of
lymphocytes for target cells. Any or all of these activities may contribute to interferon’s therapeutic
effects.
Recombinant interferon alfa-2b also inhibits viral replication
in vitro
and
in vivo
. Although the exact
antiviral mode of action of recombinant interferon alfa-2b is unknown, it appears to alter the host cell
metabolism. This action inhibits viral replication or if replication occurs, the progeny virions are
unable to leave the cell.
•
PegIntron
PegIntron pharmacodynamics were assessed in a rising single-dose trial in healthy subjects by examining
changes in oral temperature, concentrations of effector proteins such as serum neopterin and 2’5’-
oligoadenylate synthetase (2’5’-OAS), as well as white cell and neutrophil counts. Subjects treated with
PegIntron showed mild dose-related elevations in body temperature. Following single doses of PegIntron
between 0.25 and 2.0 micrograms/kg/week, serum neopterin concentration was increased in a dose-related
manner. Neutrophil and white cell count reductions at the end of week 4 correlated with the dose of
PegIntron.
PegIntron clinical trials – adults
- Naïve patients
Two pivotal trials have been conducted, one (C/I97-010) with PegIntron monotherapy; the other
(C/I98-580) with PegIntron in combination with ribavirin. Eligible patients for these trials had chronic
hepatitis C confirmed by a positive HCV-RNA polymerase chain reaction (PCR) assay (> 30 IU/ml), a
liver biopsy consistent with a histological diagnosis of chronic hepatitis with no other cause for the
chronic hepatitis, and abnormal serum ALT.
In the PegIntron monotherapy trial, a total of 916 naïve chronic hepatitis C patients were treated with
PegIntron (0.5, 1.0 or 1.5 micrograms/kg/week) for one year with a follow-up period of six months. In
addition, 303 patients received interferon alfa-2b (3 million International Units [MIU] three times a
week) as a comparator. This study showed that PegIntron was superior to interferon alfa-2b (
Table 6
).
In the PegIntron combination trial, 1,530 naïve patients were treated for one year with one of the
following combination regimens:
- PegIntron (1.5 micrograms/kg/week) + ribavirin (800 mg/day), (n = 511).
- PegIntron (1.5 micrograms/kg/week for one month followed by 0.5 microgram/kg/week for
11 months) + ribavirin (1,000/1,200 mg/day), (n = 514).
- Interferon alfa-2b (3 MIU three times a week) + ribavirin (1,000/1,200 mg/day) (n = 505).
In this trial, the combination of PegIntron (1.5 micrograms/kg/week) and ribavirin was significantly
more effective than the combination of interferon alfa-2b and ribavirin (
Table 6
), particularly in
patients infected with Genotype 1 (
Table 7
). Sustained response was assessed by the response rate six
months after the cessation of treatment.
HCV genotype and baseline virus load are prognostic factors which are known to affect response rates.
However, response rates in this trial were shown to be dependent also on the dose of ribavirin
administered in combination with PegIntron or interferon alfa-2b. In those patients that received
> 10.6 mg/kg ribavirin (800 mg dose in typical 75 kg patient), regardless of genotype or viral load,
response rates were significantly higher than in those patients that received ≤ 10.6 mg/kg ribavirin
(
Table 7
), while response rates in patients that received > 13.2 mg/kg ribavirin were even higher.
Sustained virological response (% patients HCV negative)
Response at end of
treatment
PegIntron 1.5 micrograms/kg
PegIntron 1.0 microgram/kg
PegIntron 0.5 microgram/kg
PegIntron (1.5 micrograms/kg) + ribavirin (800 mg)
PegIntron (1.5 to 0.5 microgram/kg) + ribavirin (1,000/1,200 mg)
Interferon alfa-2b (3 MIU) + ribavirin (1,000/1,200 mg)
p = 0.0143 P 1.5/R vs. I/R
Table 7
Sustained response rates with PegIntron + ribavirin
(by ribavirin dose, genotype and viral load)
HCV Genotype
Genotype 1
≤ 600,000 IU/ml
Genotype 1
> 600,000 IU/ml
PegIntron (1.5 micrograms/kg) + ribavirin (800 mg)
PegIntron (1.5 to 0.5 microgram/kg) + ribavirin (1,000/1,200 mg)
Interferon alfa-2b (3 MIU) + ribavirin (1,000/1,200 mg)
In the PegIntron monotherapy study, the Quality of Life was generally less affected by
0.5 microgram/kg of PegIntron than by either 1.0 microgram/kg of PegIntron once weekly or 3 MIU
of interferon alfa-2b three times a week.
In a separate trial, 224 patients with genotype 2 or 3 received PegIntron, 1.5 micrograms/kg
subcutaneously, once weekly, in combination with ribavirin 800 mg –1,400 mg p.o. for 6 months
(based on body weight, only three patients weighing > 105 kg, received the 1,400 mg dose) (
Table 8
).
Twenty-four % had bridging fibrosis or cirrhosis (Knodell 3/4).
Table 8 Virologic response at end of treatment, Sustained Virologic Response and relapse
by HCV Genotype and viral load*
PegIntron 1.5 μg/kg once weekly plus Ribavirin 800-1,400 mg/day
End of treatment
response
Sustained Virologic Response
* Any subject with an undetectable HCV-RNA level at the follow-up week 12 visit and missing data at the follow-
up week 24 visit was considered a sustained responder. Any subject with missing data in and after the follow-up
week 12 window was considered to be a non-responder at week 24 of follow-up.
The 6 month treatment duration in this trial was better tolerated than one year of treatment in the
pivotal combination trial; for discontinuation 5 % vs
.
14 %, for dose modification 18 % vs
.
49 %.
In a non-comparative trial, 235 patients with genotype 1 and low viral load (< 600,000 IU/ml) received
PegIntron, 1.5 micrograms/kg subcutaneously, once weekly, in combination with weight adjusted
ribavirin. The overall sustained response rate after a 24-week treatment duration was 50 %. Forty-one
percent of subjects (97/235) had nondetectable plasma HCV-RNA levels at week 4 and week 24 of
therapy. In this subgroup, there was a 92 % (89/97) sustained virological response rate. The high
sustained response rate in this subgroup of patients was identified in an interim analysis (n=49) and
prospectively confirmed (n=48).
Limited historical data indicate that treatment for 48 weeks might be associated with a higher
sustained response rate (11/11) and with a lower risk of relapse (0/11 as compared to 7/96 following
24 weeks of treatment).
A large randomized trial compared the safety and efficacy of treatment for 48 weeks with two
PegIntron/ribavirin regimens [PegIntron 1.5 µg/kg and 1 µg/kg subcutaneously once weekly both in
combination with ribavirin 800 to 1,400 mg p.o. daily (in two divided doses)] and peginterferon alfa-
2a 180 µg subcutaneously once weekly with ribavirin 1,000 to 1,200 mg p.o. daily (in two divided
doses) in 3,070 treatment-naïve adults with chronic hepatitis C genotype 1. Response to the treatment
was measured by Sustained Virologic Response (SVR) which is defined as undetectable HCV-RNA at
24 weeks post-treatment (see
Table 9
).
Table 9 Virologic response at treatment week 12, end of treatment response,
relapse rate *and Sustained Virologic Response (SVR)
Treatment group
peginterferon
alfa-2a 180 µg +
ribavirin
PegIntron 1.5 µg/kg
+ ribavirin
PegIntron 1 µg/kg
+ ribavirin
Undetectable
HCV-RNA at
treatment week
12
End of treatment
response
SVR in patients
with
undetectable
HCV-RNA at
treatment week
12
* (HCV-RNA PCR assay, with a lower limit of quantitation of 27 IU/ml)
Lack of early virologic response by Treatment week 12 (detectable HCV-RNA
with a < 2 log
10
reduction from baseline) was a criterion for discontinuation of treatment.
In all three treatment groups, sustained virologic response rates were similar. In patients of African
American origin (which is known to be a poor prognostic factor for HCV eradication), treatment with
PegIntron (1.5 µg/kg)/ribavirin combination therapy resulted in a higher sustained virologic response
rate compared to PegIntron 1 µg/kg dose. At the PegIntron 1.5 µg/kg plus ribavirin dose, sustained
virologic response rates were lower in patients with cirrhosis, in patients with normal ALT levels, in
patients with a baseline viral load > 600,000 IU/ml, and in patients > 40 years old. Caucasian patients
had a higher sustained virologic response rate compared to the African Americans. Among patients
with undetectable HCV-RNA at the end of treatment, the relapse rate was 24 %.
Predictability of sustained virological response – Naïve patients
Virological response by week 12 is defined as at least 2-log viral load decrease or undetectable levels
of HCV-RNA.Virological response by week 4 is defined as at least 1-log viral load decrease or
undetectable levels of HCV-RNA. These time points (treatment week 4 and treatment week 12) have
been shown to be predictive for sustained response (
Table 10
).
Predictive value of in-treatment Virologic Response while on PegIntron
1.5 µg/kg/ribavirin 800-1,400 mg combination therapy
Negative
No
response
at
treatment
week
Negative
predictive
value
Response
at
treatment
week
Positive
predictive
value
Genotype 1*
By week 4
***
(n=950)
HCV-RNA negative
or
≥ 1 log
decrease in
viral load
HCV-RNA negative
or
≥ 2 log decrease in
viral load
Genotype 2, 3**
By week 12
(n= 215)
HCV-RNA negative
or
≥ 2 log decrease in
viral load
*Genotype 1 receive 48 weeks treatment
**Genotype 2, 3 receive 24 weeks treatment
***The presented results are from a single point of time. A patient may be missing or have had a different result for week 4
or week 12.
†
These criteria were used in the protocol:
If week 12 HCV-RNA is positive and < 2log
10
decrease from baseline, patients to
stop therapy. If week 12 HCV-RNA is positive and decreased ≥ 2log
10
from baseline, then retest HCV-RNA at week 24
and if positive, patients to stop therapy.
The negative predictive value for sustained response in patients treated with PegIntron in monotherapy
was 98 %.
HCV/HIV Co-infected patients
Two trials have been conducted in patients co-infected with HIV and HCV. The response to treatment
in both of these trials is presented in
Table11.
Study 1 (RIBAVIC; P01017) was a randomized,
multicentre study which enrolled 412 previously untreated adult patients with chronic hepatitis C who
were co-infected with HIV. Patients were randomized to receive either PegIntron (1.5 µg/kg/week)
plus ribavirin (800 mg/day) or interferon alfa-2b (3 MIU TIW) plus ribavirin (800 mg/day) for
48 weeks with a follow-up period of 6 months. Study 2 (P02080) was a randomized, single centre
study that enrolled 95 previously untreated adult patients with chronic hepatitis C who were co-
infected with HIV. Patients were randomized to receive either PegIntron (100 or 150 µg /week based
on weight) plus ribavirin (800-1,200 mg/day based on weight) or interferon alfa-2b (3 MIU TIW) plus
ribavirin (800-1,200 mg/day based on weight). The duration of therapy was 48 weeks with a follow-up
period of 6 months except for patients infected with genotypes 2 or 3 and viral load < 800,000 IU/ml
(Amplicor) who were treated for 24 weeks with a 6-month follow-up period.
Sustained virological response based on genotype after PegIntron in
combination with Ribavirin in HCV/HIV Co-infected patients
PegIntron
(1.5 µg/kg/
week) +
ribavirin
(800 mg)
Interferon
alfa-2b
(3 MIU TIW) +
ribavirin
(800 mg)
PegIntron
(100 or
150
c
µg/week)
+ ribavirin
(800-
1,200 mg)
d
Interferon
alfa-2b
(3 MIU TIW)
+ ribavirin
(800-
1,200 mg)
d
27 % (56/205) 20 % (41/205) 0.047 44 % (23/52)
MIU = million international units; TIW = three times a week.
a: p value based on Cochran-Mantel Haenszel Chi square test.
b: p value based on chi-square test.
c: subjects < 75 kg received 100 µg/week PegIntron and subjects ≥ 75 kg received 150 µg/week PegIntron.
d: ribavirin dosing was 800 mg for patients < 60 kg, 1,000 mg for patients 60-75 kg, and 1,200 mg for patients > 75 kg.
1
Carrat F, Bani-Sadr F, Pol S et al. JAMA 2004; 292(23): 2839-2848.
2
Laguno M, Murillas J, Blanco J.L et al. AIDS 2004; 18(13): F27-F36.
Histological response
Liver biopsies were obtained before and after treatment in Study 1 and were available for 210 of the
412 subjects (51 %). Both the Metavir score and Ishak grade decreased among subjects treated with
PegIntron in combination with ribavirin. This decline was significant among responders (-0.3 for
Metavir and -1.2 for Ishak) and stable (-0.1 for Metavir and -0.2 for Ishak) among non-responders. In
terms of activity, about one-third of sustained responders showed improvement and none showed
worsening. There was no improvement in terms of fibrosis observed in this study. Steatosis was
significantly improved in patients infected with HCV Genotype 3.
- PegIntron/ribavirin retreatment of prior treatment failures
In a non-comparative trial, 2,293 patients with moderate to severe fibrosis who failed previous
treatment with combination alpha interferon/ribavirin were retreated with PegIntron,
1.5 micrograms/kg subcutaneously, once weekly, in combination with weight adjusted ribavirin.
Failure to prior therapy was defined as relapse or non-response (HCV-RNA positive at the end of a
minimum of 12 weeks of treatment).
Patients who were HCV-RNA negative at treatment week 12 continued treatment for 48 weeks and
were followed for 24 weeks post-treatment. Response week 12 was defined as undetectable HCV-
RNA after 12 weeks of treatment. Sustained Virologic Response (SVR) is defined as undetectable
HCV-RNA at 24 weeks post-treatment (
Table12
)
.
Table 12 Rates of response to retreatment in prior treatment failures
Patients with undetectable HCV–RNA
at treatment week 12 and SVR upon retreatement
interferon alpha/ribavirin
peginterferon alpha/ribavirin
38.6 (549/1,423) 59.4 (326/549)
54.0,64.8
31.5 (272/863) 50.4 (137/272)
42.6, 58.2
21.7 (497/2,293)
19.5, 23.9
59.6 (121/203)
50.7, 68.5
58.1 (200/344) 52.5 (105/200)
43.4, 61.6
37.7 (243/645)
32.8, 42.6
Genotype 1/4 59.7 (129/216)
48.6 (122/251) 44.3 (54/122)
32.7, 55.8
28.6 (134/468)
23.3, 34.0
Genotype 2/3 88.9 (72/81)
73.6 (53/72)
(60.2, 87.0)
61.3 (106/173)
51.7, 70.8
57.0 (147/258)
49.0, 64.9
12.4 (59/476) 44.1 (26/59)
27.4, 60.7
13.6 (188/1,385)
11.2, 15.9
Genotype 1/4 23.0 (182/790)
9.9 (123/1,242)
7.7, 12.1
Genotype 2/3 67.9 (74/109)
30.2 (343/1,135) 51.3 (176/343)
44.4, 58.3
23.0 (162/704) 42.6 (69/162)
32.6, 52.6
14.6 (270/1,846)
12.5, 16.7
73.0 (135/185)
64.6, 81.4
75.6 (96/127) 63.5 (61/96)
50.9, 76.2
55.3 (203/367)
48.6, 62.0
66.8 (129/193)
58.1, 75.6
33.6 (78/232) 57.7 (45/78)
43.3, 72.1
29.2 (191/653)
24.7, 33.8
62.6 (102/163)
52.8, 72.3
32.4 (78/241) 51.3 (40/78)
36.7, 65.9
21.9 (147/672)
17.8, 26.0
29.7 (116/390) 44.8 (52/116)
32.9, 56.7
16.5 (159/966)
13.4, 19.5
56.1 (157/280)
48.4, 63.7
26.5 (152/573) 41.4 (63/152)
31.2, 51.7
16.6 (239/1,441)
14.1, 19.1
30.2 (256/848)
26.1, 34.2
NR: Non-responder defined as serum/plasma HCV-RNA positive at the end of a minimum of 12 weeks of treatment.
Plasma HCV-RNA is measured with a research-based quantitative polymerase chain reaction assay by a central
laboratory
*Intent to treat population includes 7 patients for whom at least 12 weeks of prior therapy could not be confirmed
.
62.8 (169/269)
55.2, 70.4
41.0 (118/288) 61.0 (72/118)
49.5, 72.6
Overall, approximately 36 % (821/2,286) of patients had undetectable plasma HCV-RNA levels at
week 12 of therapy measured using a research-based test (limit of detection 125 IU/ml). In this
subgroup, there was a 56 % (463/823) sustained virological response rate. For patients with prior
failure on therapy with nonpegylated interferon or pegylated interferon and negative at week 12, the
sustained response rates were 59 % and 50 %, respectively.
Among 480 patients with > 2 log viral
reduction but detectable virus at week 12, altogether 188 patients continued therapy. In those patients
the SVR was 12 %.
Non-responders to prior therapy with pegylated interferon alpha/ribavirin were less likely to achieve a
week 12 response to retreatment than non-responders to nonpegylated interferon alpha/ribavirin
(12.4 % vs. 28.6 %). However, if a week 12 response was achieved, there was little difference in SVR
regardless of prior treatment or prior response.
- Long-term efficacy data
A large long-term follow-up study enrolled 567 patients after treatment in a prior study with PegIntron
(with or without ribavirin). The purpose of the study was to evaluate the durability of sustained
virologic response (SVR) and assess the impact of continued viral negativity on clinical outcomes.
327 patients completed at least 5 years of long-term follow-up and only 3 out of 366 sustained
responders relapsed during the study.
The Kaplan-Meier estimate for continued sustained response over 5 years for all patients is 99 %
(95 % CI: 98-100 %). SVR after treatment of chronic HCV with PegIntron (with or without ribavirin)
results in long-term clearance of the virus providing resolution of the hepatic infection and clinical
“cure” from chronic HCV. However, this does not preclude the occurrence of hepatic events in
patients with cirrhosis (including hepatocarcinoma).
PegIntron clinical trials – paediatric patients
Children and adolescents 3 to 17 years of age with compensated chronic hepatitis C and detectable
HCV-RNA were enrolled in a multicentre trial and treated with ribavirin 15 mg/kg per day plus
PegIntron 60 μg/m
2
once weekly for 24 or 48 weeks, based on HCV genotype and baseline viral load.
All patients were to be followed for 24 weeks post-treatment.
A total of 107 patients received
treatment of whom 52 % were female, 89 % Caucasian, 67 % with HCV Genotype 1 and 63 %
< 12 years of age. The population enrolled mainly consisted of children with mild to moderate
hepatitis C. Due to the lack of data in children with severe progression of the disease, and the potential
for undesirable effects
,
the benefit/risk of the combination of PegIntron with ribavirin needs to be
carefully considered in this population (see sections 4.1, 4.4 and 4.8). The study results are
summarized in
Table 13
Table 13 Sustained virological response rates (n
a,b
(%)) in previously untreated
children and adolescents by genotype and treatment duration – All
subjects
12/12 (100 %) 2/3 (67 %)
Genotype 4 - 4/5 (80 %)
a: Response to treatment was defined as undetectable HCV-RNA at 24 weeks post-treatment lower limit of
detection=125IU/ml
b: n = number of responders/number of subjects with given genotype, and assigned treatment duration.
c: Patients with genotype 3 low viral load (< 600,000 IU/ml) were to receive 24 weeks of treatment while
those with genotype 3 and high viral load (≥ 600,000 IU/ml) were to receive 48 weeks of treatment
.
5.2
Pharmacokinetic properties
PegIntron is a well characterized polyethylene glycol-modified (“pegylated”) derivative of interferon
alfa-2b and is predominantly composed of monopegylated species. The plasma half-life of PegIntron
is prolonged compared with nonpegylated interferon alfa-2b. PegIntron has a potential to depegylate to
free interferon alfa-2b. The biologic activity of the pegylated isomers is qualitatively similar, but
weaker than free interferon alfa-2b.
Following subcutaneous administration, maximal serum concentrations occur between 15-44 hours
post-dose, and are sustained for up to 48-72 hours post-dose.
PegIntron C
max
and AUC measurements increase in a dose-related manner. Mean apparent volume of
distribution is 0.99 l/kg.
Upon multiple dosing, there is an accumulation of immunoreactive interferons. There is, however, only a
modest increase in biologic activity as measured by a bioassay.
Mean (SD) PegIntron elimination half-life is approximately 40 hours (13.3 hours), with apparent
clearance of 22.0 ml/hr/kg. The mechanisms involved in clearance of interferons in man have not yet been
fully elucidated. However, renal elimination may account for a minority (approximately 30 %) of
PegIntron apparent clearance.
Renal function
: Renal clearance appears to account for 30 % of total clearance of PegIntron. In a
single dose study (1.0 microgram/kg) in patients with impaired renal function, C
max
, AUC, and half-
life increased in relation to the degree of renal impairment.
Following multiple dosing of PegIntron (1.0 microgram/kg subcutaneously administered every week
for four weeks) the clearance of PegIntron is reduced by a mean of 17 % in patients with moderate
renal impairment (creatinine clearance 30-49 ml/minute) and by a mean of 44 % in patients with
severe renal impairment (creatinine clearance 15-29 ml/minute) compared to subjects with normal
renal function. Based on single dose data, clearance was similar in patients with severe renal
impairment not on dialysis and in patients who were receiving hemodialysis. The dose of PegIntron
for monotherapy should be reduced in patients with moderate or severe renal impairment (see sections
4.2 and 4.4). Patients with creatinine clearance < 50 ml/minute must not be treated with PegIntron in
combination with ribavirin (see section 4.3).
Because of marked inter-subject variability in interferon pharmacokinetics, it is recommended that
patients with severe renal impairment be closely monitored during treatment with PegIntron (see
section 4.2)
Hepatic function
: The pharmacokinetics of PegIntron have not been evaluated in patients with severe
hepatic dysfunction.
Elderly patients ≥ 65 years of age
: The pharmacokinetics of PegIntron following a single subcutaneous
dose of 1.0 microgram/kg were not affected by age. The data suggest that no alteration in PegIntron
dosage is necessary based on advancing age.
Paediatric patients
: Multiple-dose pharmacokinetic properties for PegIntron and ribavirin (capsules
and oral solution) in children and adolescent patients with chronic hepatitis C have been evaluated
during a clinical study.
In children and adolescent patients receiving body surface area-adjusted dosing
of PegIntron at 60 μg/m
2
/week, the log transformed ratio estimate of exposure during the dosing
interval is predicted to be 58 % (90 % CI: 141-177 %) higher than observed in adults receiving
1.5 μg/kg/week.
Interferon neutralising factors
:
Interferon neutralising factor assays were performed on serum samples of
patients who received PegIntron in the clinical trial. Interferon neutralising factors are antibodies which
neutralise the antiviral activity of interferon. The clinical incidence of neutralising factors in patients who
received PegIntron 0.5 micrograms/kg is 1.1 %.
5.3 Preclinical safety data
PegIntron
: Adverse events not observed in clinical trials were not seen in toxicity studies in monkeys.
These studies were limited to four weeks due to the appearance of anti-interferon antibodies in most
monkeys.
Reproduction studies of PegIntron have not been performed. Interferon alfa-2b has been shown to be an
abortifacient in primates. PegIntron is likely to also cause this effect. Effects on fertility have not been
determined. It is not known whether the components of this medicinal product are excreted into
experimental animal or human milk (see section 4.6 for relevant human data on pregnancy and lactation).
PegIntron showed no genotoxic potential.
The relative non-toxicity of monomethoxy-polyethylene glycol (mPEG), which is liberated from
PegIntron by metabolism
in vivo
has been demonstrated in preclinical acute and subchronic toxicity
studies in rodents and monkeys, standard embryo-foetal development studies and in
in vitro
mutagenicity assays.
PegIntron plus ribavirin
: When used in combination with ribavirin, PegIntron did not cause any effects
not previously seen with either active substance alone. The major treatment-related change was a
reversible, mild to moderate anaemia, the severity of which was greater than that produced by either
active substance alone.
No studies have been conducted in juvenile animals to examine the effects of treatment with PegIntron
on growth, development, sexual maturation, and behaviour. Preclinical juvenile toxicity results have
demonstrated a minor, dose-related decrease in overall growth in neonatal rats dosed with ribavirin
(see section 5.3 of Rebetol SPC if PegIntron is to be administered in combination with ribavirin).
PHARMACEUTICAL PARTICULARS
Powder for solution for injection:
-
Sodium dihydrogen phosphate dihydrate
This medicinal product should only be reconstituted with the solvent provided (see section 6.6). In the
absence of compatibility studies, this medicinal product must not be mixed with other medicinal
products.
Before reconstitution:
3 years.
From a microbiological point of view, the product is to be used immediately. If not used
Disodium phosphate, anhydrous
Chemical and physical in-use stability has been demonstrated for 24 hours at 2°C - 8ºC.
immediately, in-use storage times and conditions prior to use are the responsibility of the user and
would normally not be longer than 24 hours at 2°C - 8°C.
6.4 Special precautions for storage
Store in a refrigerator (2°C - 8°C).
For storage conditions of the reconstituted medicinal product, see section 6.3.
6.5
Nature and contents of container
The powder is contained in a 2 ml vial (Type I flint glass) with a butyl rubber stopper in an aluminium
flip-off seal with a polypropylene bonnet. The solvent is presented in a 2 ml ampoule (Type I flint glass).
PegIntron 50 micrograms is supplied as:
-
1 vial of powder for solution for injection and 1 ampoule of solvent for parenteral use;
1 vial of powder for solution for injection, 1 ampoule of solvent for parenteral use, 1 injection
syringe, 2 injection needles and 1 cleansing swab;
4 vials of powder for solution for injection and 4 ampoules of solvent for parenteral use;
4 vials of powder for solution for injection, 4 ampoules of solvent for parenteral use, 4 injection
syringes, 8 injection needles and 4 cleansing swabs;
12 vials of powder for solution for injection, 12 ampoules of solvent for parenteral use, 12 injection
syringes, 24 injection needles and 12 cleansing swabs.
Not all pack sizes may be marketed.
6.6
Special precautions for disposal and other handling
Each vial is to be reconstituted with 0.7 ml of water for injections for administration of up to 0.5 ml of
solution. A small volume is lost during preparation of PegIntron for injection when the dose is measured
and injected. Therefore, each vial contains an excess amount of solvent and PegIntron powder to ensure
delivery of the labelled dose in 0.5 ml of PegIntron, solution for injection. The reconstituted solution has a
concentration of 50 micrograms/0.5 ml.
Using a sterilised injection syringe and injection needle, 0.7 ml of water for injections is injected into the
vial of PegIntron. Dissolution of powder is completed by agitating it gently. The appropriate dose can then
be withdrawn with a sterilised injection syringe and injected. A complete set of instructions is provided in
the Annex to the Package Leaflet.
As for all parenteral medicinal products, the reconstituted solution is to be inspected visually prior to
administration. The reconstituted solution should be clear and colourless. If discolouration or particulate
matter is present, the reconstituted solution should not be used. Any unused material is to be discarded.
MARKETING AUTHORISATION HOLDER
SP Europe
73, rue de Stalle
B-1180 Bruxelles
Belgium
MARKETING AUTHORISATION NUMBERS
EU/1/00/131/001
EU/1/00/131/002
EU/1/00/131/003
6 vials of powder for solution for injection and 6 ampoules of solvent for parenteral use.
EU/1/00/131/004
EU/1/00/131/005
EU/1/00/131/026
DATE OF FIRST AUTHORISATION/RENEWAL OF THE AUTHORISATION
Date of first authorisation: 25 May 2000
Date of latest renewal: 25 May 2010
10. DATE OF REVISION OF THE TEXT
Detailed information on this product is available on the web-site of the European Medicines Agency
http://www.ema.europa.eu/
This medicinal product should only be reconstituted with the solvent provided (see section 6.6). In the
absence of compatibility studies, this medicinal product must not be mixed with other medicinal
products.
Before reconstitution:
3 years.
Chemical and physical in-use stability has been demonstrated for 24 hours at 2°C - 8ºC.
From a microbiological point of view, the product is to be used immediately. If not used
Disodium phosphate, anhydrous
immediately, in-use storage times and conditions prior to use are the responsibility of the user and
would normally not be longer than 24 hours at 2°C - 8°C.
6.4 Special precautions for storage
Store in a refrigerator (2°C - 8°C).
For storage conditions of the reconstituted medicinal product, see section 6.3.
6.5
Nature and contents of container
The powder is contained in a 2 ml vial (Type I flint glass) with a butyl rubber stopper in an aluminium
flip-off seal with a polypropylene bonnet. The solvent is presented in a 2 ml ampoule (Type I flint glass).
PegIntron 100 micrograms is supplied as:
-
1 vial of powder for solution for injection and 1 ampoule of solvent for parenteral use;
1 vial of powder for solution for injection, 1 ampoule of solvent for parenteral use, 1 injection
syringe, 2 injection needles and 1 cleansing swab;
4 vials of powder for solution for injection and 4 ampoules of solvent for parenteral use;
4 vials of powder for solution for injection, 4 ampoules of solvent for parenteral use, 4 injection
syringes, 8 injection needles and 4 cleansing swabs;
12 vials of powder for solution for injection, 12 ampoules of solvent for parenteral use, 12 injection
syringes, 24 injection needles and 12 cleansing swabs.
Not all pack sizes may be marketed.
6.6
Special precautions for disposal and other handling
Each vial is to be reconstituted with 0.7 ml of water for injections for administration of up to 0.5 ml of
solution. A small volume is lost during preparation of PegIntron for injection when the dose is measured
and injected. Therefore, each vial contains an excess amount of solvent and PegIntron powder to ensure
delivery of the labelled dose in 0.5 ml of PegIntron, solution for injection. The reconstituted solution has a
concentration of 100 micrograms/0.5 ml.
Using a sterilised injection syringe and injection needle, 0.7 ml of water for injections is injected into the
vial of PegIntron. Dissolution of powder is completed by agitating it gently. The appropriate dose can then
be withdrawn with a sterilised injection syringe and injected. A complete set of instructions is provided in
the Annex to the Package Leaflet.
As for all parenteral medicinal products, the reconstituted solution is to be inspected visually prior to
administration. The reconstituted solution should be clear and colourless. If discolouration or particulate
matter is present, the reconstituted solution should not be used. Any unused material is to be discarded.
MARKETING AUTHORISATION HOLDER
SP Europe
73, rue de Stalle
B-1180 Bruxelles
Belgium
MARKETING AUTHORISATION NUMBERS
EU/1/00/131/011
EU/1/00/131/012
EU/1/00/131/013
6 vials of powder for solution for injection and 6 ampoules of solvent for parenteral use.
EU/1/00/131/014
EU/1/00/131/015
EU/1/00/131/028
DATE OF FIRST AUTHORISATION/RENEWAL OF THE AUTHORISATION
Date of first authorisation: 25 May 2000
Date of latest renewal: 25 May 2010
10. DATE OF REVISION OF THE TEXT
Detailed information on this product is available on the web-site of the European Medicines Agency
http://www.ema.europa.eu/
The active substance is peginterferon alfa-2b. Each pre-filled pen contains 150 micrograms of
peginterferon alfa-2b in 0.5 ml of solution when reconstituted as recommended
.
The other ingredients are:
Powder
: disodium phosphate, anhydrous, sodium dihydrogen phosphate dihydrate, sucrose and
polysorbate 80;
Solvent:
water for injections.
What PegIntron looks like and contents of the pack
PegIntron is a powder and solvent (liquid) for solution for injection in a pre-filled pen.
The white powder and the clear and colourless solvent are both contained in a two-chamber glass
cartridge assembled into a single use pre-filled pen.
PegIntron 150 micrograms is available in different pack sizes:
-
1 pen containing powder and solvent for solution for injection, 1 injection needle and 2 cleansing
swabs;
4 pens containing powder and solvent for solution for injection, 4 injection needles and 8 cleansing
swabs;
6 pens containing powder and solvent for solution for injection, 6 injection needles
and 12 cleansing swabs;
- 12 pens containing powder and solvent for solution for injection, 12 injection needles
and 24 cleansing swabs.
Not all pack sizes may be marketed.
Marketing Authorisation Holder
SP Europe, 73, rue de Stalle, B-1180 Bruxelles, Belgium
Manufacturer
SP Labo N.V., Industriepark, 30, B-2220 Heist-op-den-Berg, Belgium
For any information about this medicine, please contact the local representative of the Marketing
Authorisation Holder:
België/Belgique/Belgien
Rue de Stalle/Stallestraat 73
B-1180 Bruxelles/Brussel/Brüssel
Tél/Tel: + 32-(0)2 370 92 11
Luxembourg/Luxemburg
Rue de Stalle 73
B-1180 Bruxelles/Brüssel
Belgique/Belgien
Tél/Tel: + 32-(0)2 370 92 11
България
Ийст Парк Трейд Център
Бул. „Н.Й.Вапцаров” 53А, ет. 2
BG-София 1407
Тел.: +359 2 806 3030
Magyarország
Alkotás u. 53.
H-1123 Budapest
Tel.: +36 1 457-8500
Česká republika
Ke Štvanici 3
CZ-186 00 Praha 8
Tel: +420 221771250
Malta
168 Christopher Street
MT-VLT02 Valletta
Tel: + 356-21 23 21 75
Danmark
Lautrupbjerg 2
DK-2750 Ballerup
Tlf: + 45-44 39 50 00
Nederland
Waarderweg 39
NL-2031 BN Haarlem
Tel: + 31-(0)800 9999000
Deutschland
Thomas-Dehler-Straße 27
D-81737 München
Tel: + 49-(0)89 627 31-0
Norge
Pb. 398
N-1326 Lysaker
Tlf: + 47 67 16 64 50
Eesti
Järvevana tee 9
EE-11314 Tallinn
Tel: + 372 654 96 86
Österreich
Am Euro Platz 2
A-1120 Wien
Tel: + 43-(0) 1 813 12 31
Ελλάδα
Αγίου Δημητρίου 63
GR-174 55 Άλιμος
Tηλ.: + 30-210 98 97 300
Polska
Ul. Taśmowa 7
PL-02-677 Warszawa
Tel.: + 48-(0)22 478 41 50
España
Josefa Valcárcel, 38
E-28027 Madrid
Tel: + 34-91 321 06 00
Portugal
Rua Agualva dos Açores 16
P-2735-557 Agualva-Cacém
Tel: +351-21 433 93 00
France
34 avenue Léonard de Vinci
România
Şos. Bucureşti-Ploieşti, nr. 17-21,
F-92400 Courbevoie
Tél: + 33-(0)1 80 46 40 40
Băneasa Center, et. 8, sector 1
RO-013682 Bucureşti
Tel: + 40 21 233 35 30
Ireland
Shire Park
Welwyn Garden City
Hertfordshire AL7 1TW
Tel: +44-(0)1 707 363 636
Slovenija
Dunajska 22
SI-1000 Ljubljana
Tel: + 386 01 3001070
Ísland
Hörgatún 2
IS-210 Garðabær
Sími: + 354 535 70 00
Slovenská republika
Strakova 5
SK-811 01 Bratislava
Tel: + 421 (2) 5920 2712
Italia
Via fratelli Cervi snc,
Centro Direzionale Milano Due
Palazzo Borromini
I-20090 Segrate (Milano)
Tel: + 39-02 21018.1
Suomi/Finland
PL 46/PB 46
FIN-02151 Espoo/Esbo
Puh/Tel: + 358 (0)9 804 650
Κύπρος
Οδός Αγίου Νικολάου, 8
CY-1055 Λευκωσία
Τηλ: +357-22 757188
Sverige
Box 7125
S-192 07 Sollentuna
Tel: + 46-(0)8 6261400
Latvija
Bauskas 58a -401
Rīga, LV-1004
Tel: + 371-7 21 38 25
United Kingdom
Shire Park
Welwyn Garden City
Hertfordshire AL7 1TW - UK
Tel: + 44-(0)1 707 363 636
Lietuva
Kęstučio g. 65/40
LT-08124 Vilnius
Tel: + 370 52 101868
This leaflet was last approved in
Detailed information on this medicine is available on the web-site of the European Medicines Agency
http://www.ema.europa.eu
ANNEX TO THE PACKAGE LEAFLET
How to use the PegIntron pre-filled pen
The following instructions explain how to inject yourself with the single use PegIntron pre-filled pen.
Please read all of the instructions carefully before attempting to use the pen and follow them
step by step.
Your doctor or his/her assistant will show you how to self-inject with the PegIntron pre-filled pen. Do
not attempt to inject yourself unless you are sure you understand everything fully.
The PegIntron pre-filled pen should be used by one person only and must not be shared. Use the injection
needle and cleansing swabs provided in the pack
only
for the PegIntron pre-filled pen. Make sure that the
pen is at room temperature before you use it. Your doctor will have told you what dose you need to take
for your treatment.
Note: The colour of the dosing button is different for each strength of the PegIntron pre-filled pen.
Find a clean, well-lit, non-slip flat working surface and get together all of the supplies you will
need for the injection. All of the supplies you will need are in the PegIntron pack. The pack
contains:
•
PegIntron pre-filled pen
•
one disposable injection needle
•
two cleansing swabs, and
•
dosing tray
The PegIntron pre-filled pen should be stored in the refrigerator, but take it out and allow it to
come to room temperature before you use it. Before taking the PegIntron pre-filled pen out of its
carton, check the expiration date printed on the carton. Do not use if the expiration date has
passed.
Take the PegIntron pre-filled pen out of the carton. Look in the window of the pen and make
sure there is a white, to off-white tablet that is whole, or in pieces, or powdered. This is the
PegIntron which will be mixed with liquid inside the pen before it is injected.
Wash your hands thoroughly with soap and water, rinse, and towel dry. It is important to keep
your work area, your hands, and the injection site clean to lessen the risk of infection.
Please follow the 4 major steps below to use the pen.
Step 1: Mix the medicine
Key points:
Before you mix the PegIntron, make sure it is at room temperature. It is important that you
keep the PegIntron pre-filled pen upright (Dosing button down) (as shown in figure 1).
•
Place the PegIntron pre-filled pen
upright in the holder of
the tray provided in the pack (the dosing button will be on
the
bottom
) on a hard, flat, non-slip surface. You may want
to hold the pen using the grip.
•
To mix the powder and the liquid, keep the PegIntron pre-
filled pen upright in the dosing tray and
press the top half
of
the pen
downward
toward the hard, flat, non-slip surface
until you hear the pen click.
Once you have heard the click, you will notice in the window that
both dark stoppers are now touching. The dosing button should be
flush with the pen body.
•
Wait for several seconds to let the powder dissolve.
•
Gently turn the pen upside down twice. DO NOT
SHAKE THE PEN.
•
Keep the PegIntron pre-filled pen upright, with the dosing
button down. Then, look through the pen window to see
that the mixed PegIntron solution is competely dissolved. If
there is still foam, wait until it settles.
•
The solution should be clear and colourless before use.
Do
not use
the solution if it is discoloured, not clear, or
contains particles
.
•
Before attaching the needle, it is normal to see some small
bubbles in the pre-filled pen window, near the top of the
solution.
•
Place the pen back into the holder in the tray with the
dosing button on the bottom.
Step 2: Attach the needle
•
Keeping the pen upright in the tray holder, wipe the rubber
membrane of the PegIntron pre-filled pen with one cleansing
swab.
•
Take the injection needle provided in the tray and remove its
protective
paper tab
, but
DO NOT
remove either the outer
cap or the yellow inner cap from the injection needle.
•
Keeping the pen upright in the tray holder, FIRMLY
push
the injection needle straight onto the pen rubber membrane
(figure 2) and
screw it securely in place, in a clockwise
direction
.
•
Keep the PegIntron pre-filled pen
UPRIGHT
(Dosing button down)
and keep both needle caps
on until you are ready to inject.
•
Screwing the needle into place, “primes” the needle and allows the extra liquid and air in the pen
to be removed.
NOTE
: You may see some liquid trickle out from under the cap, as the air has
been expelled out of the pen. This is normal.
•
Wait about 5 seconds for this process to finish.
•
The dark stoppers
move up
and you will no longer see the fluid in the window once the needle is
successfully primed (figure 3).
•
Check through the window to be sure that the two stoppers
are together.
If they are not together, do not use this pen
because you may not be able to dial your dose (figure 3).
•
Take the pen from the tray holder.
•
Holding the pen firmly, pull the dosing button out as far as it
will go, until you see a
dark ring
on the pen. The dosing
button should be easy to pull out without too much force
being needed (figure 4).
NOTE: Do not push the dosing button back in at this time.
You will push it in when you are ready to self-inject the
PegIntron.
•
Turn the dosing button until your prescribed dose is in line with
the dosing tab. The button should turn easily without too much
force being needed (figure 5). If you have trouble dialing your
dose, check to make sure the dosing button has been pulled out
as far
as it will go.
NOTE
:
If you cannot easily pull out the dosing button or dial
the dose, do not use excessive force and do not use this pen
because it may not deliver the correct dose.
Carefully lay the pen down on a hard, flat, non-slip surface.
DO NOT remove either of the needle caps and DO NOT push
the dosing button in until you are ready to self-inject the
PegIntron dose.
Step 4: Inject the PegIntron solution
•
Select the injection site. Your doctor will have told you which sites to use (e.g., thigh or abdomen).
The best sites for giving yourself an injection are those areas with a layer of fat between the skin and
muscle, like your thigh, the outer surface of your upper arm, and abdomen. Do not inject yourself in
the area near your navel or waistline. If you are very thin, you should only use the thigh or outer
surface of the arm for injection.
You should use a different site each time you inject PegIntron to
avoid soreness at any one site.
Do not inject PegIntron into an area where the skin is irritated, red,
bruised, infected, or has scars, stretch marks, or lumps.
•
Clean the injection site skin with the second cleansing swab provided, and wait for the area to dry.
•
Pull off the
outer needle cap (figure 6)
.
•
There may be some liquid around the inner needle cap.
Don’t worry, this is normal. This liquid is not part of your
dose, it is extra.
•
Once the injection site is dry, pull off the
yellow inner
needle cap
carefully exposing the injection needle. You are
now ready to inject.
•
Hold the PegIntron pre-filled pen with your fingers
wrapped around the pen body barrel and your thumb on
the dosing button
(figure 7)
.
•
With your other hand, pinch a fold of loose skin in the area you
have cleaned for injection.
•
Insert the needle into the pinched skin at an angle of 45° to 90°.
•
Press the dosing button down
slowly
and
firmly
until the
button can no longer move.
•
Keep your thumb pressed down on the dosing button for
an additional 5 seconds
to ensure that you get the complete
dose.
•
Remove the needle from your skin.
•
Gently press the injection site with a small bandage or sterile gauze if necessary for a few
seconds.
•
Do not massage the injection site. If there is bleeding, cover with an adhesive bandage.
•
Discard the PegIntron pre-filled pen with the needle safely in a closed rigid container.
After 2 hours, check the injection site for redness, swelling, or tenderness.
If you have a skin reaction and it doesn’t clear up in a few days, contact your health care
professional.
Source: European Medicines Agency
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