Fluticasone 50 inhaler
(i) ROUTE OF ADMINISTRATION
Inhalation
DOSAGE AND ADMINISTRATION
Adults and children over
16 years of age :
100 to 1,000 µg twice daily. Patients should be given a starting dose
of inhaled fluticasone propionate which is appropriate for the severity of
their disease
Mild asthma: 100 to 250 µg twice daily.
Moderate asthma: 250 to 500 µg twice daily.
Severe asthma: 500 to 1,000 µg twice daily.
Children over 4 years
:
50 to 100 µg twice daily.
Children under 4 years
Not recommended.
(ii) THERAPEUTIC / DIAGNOSTIC CLAIMS
Health 2000 Fluticasone 50 mcg inhaler is indicated for the maintenance treatment of asthma in adults and children above 4 years as prophylactic therapy. It is also indicated for patients requiring oral corticosteroid therapy for asthma. Many of these patients may be able to reduce or eliminate their requirement for oral corticosteroid over time.
Health 2000 Fluticasone
50 mcg inhaler is not indicated for the relief of acute bronchospasm.
Health 2000 Fluticasone 50 mcg inhaler may be used with a Health 2000 Spacer
device in patients who find it difficult to synchronise aerosol actuation
with inspiration of breath.
(ii) DESCRIPTION OF DOSAGE FORM
Fluticasone propionate is a synthetic, trifluorinated glucocorticoid with
potent anti- inflammatory activity. In vitro assays have established fluticasone
propionate as a human glucocorticoid receptor agonist with an affinity 18
times greater than dexamethasone, almost twice that of beclomethasone-17-mono-propionate,
the active metabolite of beclomethasone dipropionate, and over three times
that of budesonide. Data from the McKenzie vasoconstrictor assay in man are
consistent with these results.
Inflammation is recognized as an important component in the pathogenesis of
asthma. Glucocorticoids have been shown to inhibit multiple cell types (eg
mast cells, eosinophils, basophils, lymphocytes, macrophages, and neutrophils)
and mediator production or secretion (e.g. histamine, eicosanoids, leukotrienes,
and cytokines) involved in the asthmatic response. These anti-inflammatory
actions of glucocorticoids may contribute to their efficacy in asthma.
Though highly effective for the treatment of asthma, glucocorticoids do not affect asthma symptoms immediately. However, improvement following inhaled administration of fluticasone propionate can occur within 24 hours of beginning treatment, although maximum benefit may not be achieved for 1 to 2 weeks or longer after starting treatment. When glucocorticoids are discontinued, asthma stability may persist for several days or longer.
(iv) CONTRAINDICATIONS
Health 2000 Fluticasone 50 mcg inhaler is contraindicated in the following situations: in patients with a history of hypersensitivity to any of its components, in children under 4 years of age, and in the primary treatment of status asthmaticus or other acute episodes of asthma where intensive measures are required.
WARNINGS AND PRECAUTIONS
Patient's inhaler technique should be checked regularly to make sure that
inhaler actuation is synchronised with inspiration to ensure optimum delivery
of the drug to the lungs.
Health 2000 Fluticasone 50 mcg inhaler is not designed to relieve acute symptoms,
for which an inhaled short-acting bronchodilator is required. Patients should
be advised to have such rescue medication available.
Severe asthma requires regular medical assessment, including lung-function
testing, as patients are at risk of severe attacks and even death.
Increasing use of short-acting inhaled beta2-agonists to relieve symptoms
indicates deterioration of asthma control. If patients find that short-acting
relief bronchodilator treatment becomes less effective, or they need more
inhalations than usual, medical attention must be sought.
In this situation patients should be reassessed and consideration given to the need for increased anti-inflammatory therapy (e.g. higher doses of inhaled corticosteroids or a course of oral corticosteroids). Severe exacerbations of asthma must be treated in the normal way.
Adrenal function and adrenal
reserve usually remain within the normal range on inhaled fluticasone propionate.
However, some systemic effects may occur in a small proportion of adult patients
after prolonged treatment at high doses. Patients transferred from other inhaled
steroids or oral steroids remain at risk of impaired adrenal reserve for a
considerable time after transferring to inhaled fluticasone propionate.
Patients in a medical or surgical emergency, who in the past have required
high doses of other inhaled steroids and/or intermittent treatment with oral
steroids, remain at risk of impaired adrenal reserve for a considerable time
after transferring to inhaled fluticasone propionate. The extent of the adrenal
impairment may require specialist advice before elective procedures. The possibility
of residual impaired adrenal response should always be borne in mind in emergency
and elective situations likely to produce stress, and appropriate corticosteroid
treatment must be considered.
In children taking recommended doses of inhaled fluticasone propionate, adrenal function and adrenal reserve usually remain within the normal range. Very rarely biochemical changes suggestive of systemic effects have been reported. The clinical relevance of these changes has not been substantiated, and, in particular, no stunting of growth in children has been observed. The possible effects of previous or intermittent treatment with oral steroids should not be discounted. The benefits of Health 2000 Fluticasone 50 mcg inhaler should minimise the need for oral steroids.
Lack of response or severe exacerbations of asthma should be treated by increasing the dose of inhaled fluticasone propionate and, if necessary, by giving a systemic steroid and/or an antibiotic if there is an infection.
For the transfer of patients
being treated with oral corticosteroids:
The transfer of oral steroid-dependent patients to Health 2000 Fluticasone
50 mcg inhaler and their subsequent management, needs special care as recovery
from impaired adrenocortical function, caused by prolonged systemic steroid
therapy, may take a considerable time.
Patients who have been treated with systemic steroids for long periods of time, or at a high dose, may have adrenocortical suppression. With these patients, adrenocortical function should be monitored regularly and their dose of systemic steroid reduced cautiously.
After approximately a week, gradual withdrawal of the systemic steroid is started by reducing the daily dose by 1 mg prednisolone, or its equivalent, at not less than weekly intervals. For maintenance doses of prednisolone in excess of 10 mg daily, it may be appropriate to cautiously use larger reductions in dose at weekly intervals.
Some patients feel unwell in a non-specific way during the withdrawal phase despite maintenance or even improvement of respiratory function. They should be encouraged to persevere with Health 2000 Fluticasone 50 mcg inhaler and to continue withdrawal of systemic steroid, unless there are objective signs of adrenal insufficiency.
Patients transferred from
oral steroids whose adrenocortical function is still impaired should carry
a steroid warning card indicating that they need supplementary systemic steroid
during periods of stress, e.g. worsening asthma attacks, chest infections,
major intercurrent illness, surgery, trauma, etc.
Replacement of systemic steroid treatment with inhaled therapy sometimes unmasks
allergies such as allergic rhinitis or eczema previously controlled by the
systemic drug. These allergies should be symptomatically treated with antihistamine
and/or topical preparations, including topical steroids.
Treatment with Health 2000 Fluticasone 50 mcg inhaler should not be stopped abruptly. Special care is necessary in patients with active or quiescent pulmonary tuberculosis.
PREGNANCY AND
LACTATION
There is inadequate evidence of safety of fluticasone propionate in human
pregnancy. Administration of corticosteroids to pregnant animals can cause
abnormalities of fetal development, including cleft palate and intrauterine
growth retardation. There may therefore be a very small risk of such effects
in the human foetus. It should be noted, however, that the foetal changes
in animals occur after relatively high systemic exposure. Because fluticasone
propionate is delivered directly to the lungs by the inhaled route it avoids
the high level of exposure that occurs when corticosteroids are given by systemic
routes. Administration of fluticasone propionate during pregnancy should only
be considered if the expected benefit to the mother is greater than any possible
risk to the foetus.
The secretion of fluticasone propionate in human breast milk has not been investigated. Subcutaneous administration of fluticasone propionate to lactating laboratory rats produced measurable plasma levels and evidence of fluticasone propionate in the milk. However plasma levels in humans after inhalation at recommended doses are likely to be low. When fluticasone propionate is used in breast-feeding mothers the therapeutic benefits must be weighed against the potential hazards to mother and baby.
(v) SIDE EFFECTS
Candidiasis of the mouth
and throat (thrush) occurs in some patients. Such patients may find it helpful
to rinse out their mouth with water after use. Symptomatic candidiasis can
be treated with topical anti-fungal therapy whilst still continuing with inhaled
fluticasone propionate.
In some patients inhaled fluticasone propionate may cause hoarseness. It may
be helpful to rinse out the mouth with water immediately after inhalation.
There have been rare reports of cutaneous hypersensitivity to fluticasone
propionate inhaled preparations.
As with other inhalation therapy paradoxical bronchospasm may occur with an
immediate increase in wheezing after dosing. This responds to a fast-acting
inhaled bronchodilator. The preparation should be discontinued immediately,
the patient assessed, and, if necessary, alternative therapy instituted.
(vi) TOXIC EFFECTS:
MUTAGENICITY
No evidence of mutagenicity has been found in microbial tests.Mice have been dosed daily for 18 months with 1 mg.kg-1 orally and rats have had snout applications daily for 2 years without evidence of carcinogenicity.
No evidence of a tumorigenic
effect was observed in either a 2 year study in rats receiving doses of fluticasone
propionate up to 57 µg/kg/day by inhalation or in an 18 month study
in mice receiving oral doses of fluticasone propionate up to 1 mg/kg/day.
There was no evidence of a mutagenic potential in a standard battery of mutagenicity
assays.
A fertility study in rats showed decreased mean fetal weight, retardation
of ossification, and decreased postnatal viability at the dose of 50 µg/kg/day
SC of fluticasone propionate.
CARCINOGENICITY
Two 18-month studies were performed in mice to evaluate the carcinogenic potential
of fluticasone propionate when given topically (as an 0.05% ointment) and
orally. No evidence of carcinogenicity was found in either study.
TERATOGENECITY
Teratogenicity studies in mice, rats and rabbits have shown effects which are similar to those of other corticosteroids with growth retardation, cleft palate, and decreased cranial ossification. In pregnant rats, subcutaneous doses of 10, 30 or 100 mg.kg-1 daily were administered on days 6 to 15 of pregnancy.No important effects were seen. In pregnant mice treated with 15 to 150 mg.kg-1 from day 6 to day 15 of pregnancy a single cleft palate occurred at 45 mg.kg-1 and 150 mg.kg-1 daily cleft palate was observed in more than half of litters with an increased in impaired cranial ossification.