Buscopan Ta Binj
Buscopan Ta Binj
Buscopan Ta Binj
DATA SHEET
*Only applicable for the product BUSCOPAN® FORTE 20 mg film coated tablet.
3 PHARMACEUTICAL FORM
Tablet 10 mg: white, unmarked, biconvex, sugar-coated.
Tablet 20 mg: white, round, biconvex, film coated tablets embossed with the letter ‘B’ on one side
and the number ‘20’ on the other side.
4 CLINICAL PARTICULARS
Oral:
Adults and children over 6 years: 2 BUSCOPAN 10 mg tablets (20 mg) four times a day
or
Parenteral:
Adults and adolescents over 12 years 1 or 2 ampoules (20 – 40 mg) may be administered by slow
intravenous, intramuscular or subcutaneous injection several
times a day. A maximum daily dose of 100mg should not be
exceeded.
Infants and young children: In severe cases, 0.3 - 0.6 mg/kg bodyweight, to be
administered by slow intravenous, intramuscular or
subcutaneous injection several times a day.The maximum
daily dose of 1.2 mg/kg should not be exceeded.
BUSCOPAN and BUSCOPAN FORTE should not be taken on a continuous daily basis or for
extended periods without investigating the cause of abdominal pain.
4.3 CONTRAINDICATIONS
In case of rare hereditary conditions that may be incompatible with an excipient of the product
(please refer to Section 4.4) the use of the product is contraindicated.
In case severe, unexplained abdominal pain persists or worsens, or occurs together with symptoms
like fever, nausea, vomiting, changes in bowel movements, abdominal tenderness, decreased blood
pressure, fainting or blood in stool, medical advice should immediately be sought where appropriate
diagnostic measures are needed to investigate the etiology of the symptoms.
Hyoscine may cause drowsiness: patients so affected should not drive or operate machinery. Patients
should abstain from alcohol. However, as a quaternary ammonium compound with low lipid
solubility, BUSCOPAN cannot cross the blood/brain barrier easily and only rarely causes the central
nervous system side effects associated with atropine and hyoscine.
Caution is needed in patients with cardiac conditions submitted to parenteral treatment with
BUSCOPAN. Monitoring of these patient is advised.
BUSCOPAN injection can cause tachycardia, hypotension and anaphylaxis, therefore use with
caution in patients with cardiac conditions such as cardiac failure, coronary heart disease, cardiac
arrhythmia or hypertension, and in cardiac surgery. Monitoring of these patients is advised.
Emergency equipment and personnel trained in its use must be readily available.
One sugar-coated tablet of 10 mg contains 41.2 mg sucrose, resulting in 329.6 mg sucrose per
maximum recommended daily dose. Patients with the rare hereditary condition of fructose
intolerance should not take this medicine.
One film-coated tablet of 20 mg contains 138.5 mg lactose, resulting in 554 mg lactose per
maximum recommended daily dose. Patients with the rare hereditary conditions of galactose
intolerance e.g. galactosaemia, the Lapp lactase deficiency or glucose-galactose malabsorption
should not take this medicine.
Paediatric use
The anticholinergic effect of drugs such as tri- and tetracyclic antidepressants, antihistamines,
antipsychotics, quinidine, amantadine, disopyramide and other anticholinergics (e.g. tiotropium,
ipratropium, atropine-like compounds) may be intensified by BUSCOPAN and BUSCOPAN
FORTE.
Concomitant treatment with dopamine antagonists such as metoclopramide may result in diminution
of the effects of both drugs on the gastrointestinal tract.
Animal studies do not indicate direct or indirect harmful effects with respect to reproductive toxicity
(please refer to Section 5.3).
No studies on the effects on human fertility have been conducted (please refer to Section 5.3).
No studies on the effects on the ability to drive and use machines have been performed. However,
patients should be advised that they may experience undesirable effects such as accommodation
disorder or dizziness during treatment with BUSCOPAN injection. Therefore, caution should be
recommended when driving a car or operating machinery. If patients experience accommodation
disorder or dizziness, they should avoid potentially hazardous tasks such as driving or operating
machinery.
Many of the listed undesirable effects can be assigned to the anticholinergic properties of
BUSCOPAN and BUSCOPAN FORTE. Anticholinergic side effects of BUSCOPAN and
BUSCOPAN FORTE are generally mild and self-limited.
Adverse events have been ranked under headings of frequency using the following convention: Very
common ≥ 1/10
Not known: anaphylactic shock including fatal outcome, anaphylactoidic reactions, dyspnoea, skin
reactions (e.g. urticaria, rash, erythema, pruritus) and other hypersensitivity.
Cardiac disorders
Common: tachycardia
Gastrointestinal disorders
Very rarely in the national post marketing surveillance data base, there have been isolated reports
following parenteral administration of coma, hallucinations, dystonia, confusion, agitation and
dizziness from which the patient recovered after drug withdrawal and appropriate treatment. In very
rare cases, dyspnoea has been reported.
Reporting suspected adverse reactions after authorisation of the medicine is important. It allows
continued monitoring of the benefit/risk balance of the medicine. Healthcare professionals are asked
to report any suspected adverse reactions https://nzphvc.otago.ac.nz/reporting/.
4.9 OVERDOSE
Symptoms
Serious signs of poisoning following acute overdosage have not been observed in man. In case of
overdose, anticholinergic symptoms such as urinary retention, dry mouth, reddening of skin,
tachycardia, inhibition of gastrointestinal motility, and transient visual disturbances may occur.
Therapy
In the case of oral poisoning, gastric lavage with activated charcoal should be followed by
magnesium sulphate (15%). Symptoms of BUSCOPAN and BUSCOPAN FORTE overdosage
respond to parasympathomimetics. For patients with glaucoma, urgent ophthalmological advice
should be sought and pilocarpine should be given locally. If necessary, parasympathomimetics
should be administered, e.g. neostigmine 0.5-2.5 mg i.m. or i.v. Cardiovascular complications as a
result of using this medicine should be treated according to usual therapeutic principles. In case of
respiratory paralysis: intubation, artificial respiration should be considered. Catheterisation may be
required for urinary retention. In addition, appropriate supportive measures should be used as
required.
In the case of overdose, immediately contact the Poisons Information Centre, in New Zealand,
called 0800 764 766.
5 PHARMACOLOGICAL PROPERTIES
Absorption
0.11 ng/mL and 2.04 ng/mL were found at approximately 2 hours. In the same dose range, the
observed mean AUC0-tz-values varied from 0.37 to 10.7 ng h/mL. The median absolute
bioavailabilities of different dosage forms, i.e. coated tablets, suppositoires and oral solution,
containing 100 mg of hyoscine butylbromide each were found to be less than 1%.
Distribution
After intravenous administration hyoscine butylbromide is rapidly distributed (t1/2α = 4 min, t1/2β =
29 min) into the tissues. The volume of distribution (Vss) is 128 L (corresponding to approx. 1.7
L/kg).
Because of its high affinity for muscarinic receptors and nicotinic receptors, hyoscine butylbromide
is mainly distributed on muscle cells of the abdominal and pelvic area as well as in the intramural
ganglia of the abdominal organs. Plasma protein binding (albumin) of hyoscine butylbromide is
approximately 4.4%. Animal studies demonstrate that hyoscine butylbromide does not pass the
blood-brain barrier, but no clinical data to this effect is available. Hyoscine butylbromide (1 mM)
has been observed to interact with the choline transport (1.4 nM) in epithelial cells of human
placenta in vitro.
Following oral administration of single doses in the range of 100 to 400 mg, the terminal elimination
half-lives ranged from 6.2 to 10.6 hours. The main metabolic pathway is the hydrolytic cleavage of
the ester bond. Orally administered hyoscine butylbromide is excreted in the faeces and in the urine.
Studies in man show that 2 to 5% of radioactive doses is eliminated renally after oral, and 0.7 to
1.6% after rectal administration. Approximately 90% of recovered radioactivity can be found in the
faeces after oral administration. The urinary excretion of hyoscine butylbromide is less than 0.1% of
the dose. The mean apparent oral clearances after oral doses of 100 to 400 mg range from 881 to
1420 L/min, whereas the corresponding volumes of distribution for the same range vary from 6.13
to 11.3 x 105 L, probably due to very low systemic availability. The metabolites excreted via the
renal route bind poorly to the muscarinic receptors and are therefore not considered to contribute to
the effect of the hyoscine butylbromide
The half-life of the terminal elimination phase (t1/2γ) is approximately 5 hours. The total clearance is
1.2 L/min. Clinical studies with radiolabeled hyoscine butylbromide show that after intravenous
injection 42 to 61% of the radioactive dose is excreted renally and 28.3 to 37% faecally. The portion
of unchanged active ingredient excreted in the urine is approximately 50%. The metabolites
excreted via the renal route bind poorly to the muscarinic receptors and are therefore not considered
to contribute to the effect of the hyoscine butylbromide.
Acutely, hyoscine butylbromide has a low index of toxicity: oral LD50 values were 1000-3000
mg/kg in mice, 1040-3300 mg/kg in rats, and 600 mg/kg in dogs. Toxic signs were ataxia and
decreased muscle tone, additionally, in mice tremor and convulsions, in dogs mydriasis, dry mucous
membranes and tachycardia. Deaths from respiratory arrest occurred within 24 h. The intravenous
LD50 values of hyoscine butylbromide were 10-23 mg/kg in mice and 18 mg/kg in rats.
In repeated oral dose toxicity studies over 4 weeks, rats tolerated 500 mg/kg = "no observed adverse
effect level (NOAEL)". At 2000 mg/kg, by the action on parasympathetic ganglia of visceral area,
hyoscine butylbromide paralysed the gastrointestinal function resulting in obstipation. Eleven out of
50 rats died. Haematology and clinical chemistry results did not show dose-related variations.
Over 26 weeks, rats tolerated 200 mg/kg, while at 250 and 1000 mg/kg, the gastro-intestinal
function was depressed and deaths occurred. The NOAEL of the 39-week oral (capsule) dog study
was 30 mg/kg. The majority of clinical findings were attributable to acute effects of hyoscine
butylbromide at high dosages (200 mg/kg). No adverse histopathological findings were observed.
A repeated intravenous dose of 1 mg/kg was well tolerated by rats in a 4-week study. At 3 mg/kg,
convulsions occurred immediately after injection. Rats dosed with 9 mg/kg died from respiratory
paralysis.
Dogs treated intravenously over 5 weeks at 2 x 1, 2 x 3 and 2 x 9 mg/kg, showed a dose- dependent
mydriasis in all treated animals, in addition at 2 x 9 mg/kg, ataxia, salivation and decreased body
weight and food intake were observed. The solutions were locally well tolerated.
After repeated i.m. injection, the dose of 10 mg/kg was systemically well tolerated, but lesions of
muscles at the site of injection were distinctly increased if compared to control rats. At 60 and 120
mg/kg, mortality was high and local damages were dose-dependently increased.
Hyoscine butylbromide was neither embryotoxic nor teratogenic at oral doses of up to 200 mg/kg in
the diet (rat) and 200 mg/kg by gavage or 50 mg/kg s.c. (rabbit). Fertility was not impaired at doses
of up to 200 mg/kg p.o.
Like other cationic drugs, hyoscine butylbromide interacts with the choline transport system of
human placental epithelial cells in vitro. Transfer of hyoscine butylbromide to the foetal
compartment has not been proved.
In special studies concerning local tolerability, a repeated i.m. injection of 15 mg/kg BUSCOPAN
over 28 days was studied in dogs and monkeys. Small focal necroses at the site of injection were
seen only in dogs. BUSCOPAN was well tolerated in arteries and veins of the rabbit´s ear. In vitro,
2 % BUSCOPAN injectable solution showed no haemolytic action when mixed with 0.1 ml human
blood.
Hyoscine butylbromide revealed no mutagenic or clastogenic potential in the Ames test, in the in
vitro gene mutation assay in mammalian V79 cells (HPRT test) and in an in vitro chromosome
aberration test in human peripheral lymphocytes. In vivo, hyoscine butylbromide was negative in the
rat bone marrow micronucleus assay.
There are no in vivo carcinogenicity studies. Nevertheless, hyoscine butylbromide did not show a
tumorigenic potential in two oral 26-week-studies in rats given up to 1000 mg/kg.
6 PHARMACEUTICAL PARTICULARS
10 mg Tablets: dibasic calcium phosphate, maize starch, starch soluble, aerosil 200, tartaric acid,
stearic acid, polyvidone saccharose, talc, acacia, titanium dioxide, polyethylene glycol 6000,
carnauba wax, beeswax white.
6.2 INCOMPATIBILITIES
None known.
Injections: For single use only. Any unused solution should be discarded
7 MEDICINE SCHEDULE
10 mg Tablets: Prescription Medicine.
8 SPONSOR
sanofi-aventis new zealand limited
Level 8
56 Cawley Street Ellerslie,
Auckland
New Zealand
Tel: 0800 283 684