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Glycopyrronium Bromide 2mg Tablets

Document: spc-doc_PL 20117-0095 change

SUMMARY OF PRODUCT CHARACTERISTICS

1    NAME OF THE MEDICINAL PRODUCT

Glycopyrronium Bromide 2mg Tablets

2    QUALITATIVE AND QUANTITATIVE    COMPOSITION

Each 2mg tablet contains 2mg of Glycopyrronium Bromide For the full list of excipients, see section 6.1.

3    PHARMACEUTICAL FORM

Tablets

Glycopyrronium Bromide 2 mg Tablets are white to off white capsule shaped, flat, beveled edge, scored tablets engraved with “I 22” on the scored side and plain on other side.

4    CLINICAL PARTICULARS

4.1    Therapeutic indications

For use in adults as add-on therapy in the treatment of peptic ulcer.

4.2 Posology and method of administration

Posology

The dosage of Glycopyrronium Bromide Tablets 1 mg or 2 mg should be adjusted to the needs of the individual patient to assure symptomatic control with a minimum of adverse reactions. The presently recommended maximum daily dosage of Glycopyrronium Bromide is 8 mg.

Glycopyrronium Bromide Tablets 1 mg.

The recommended initial dosage of Glycopyrronium Bromide 1 mg Tablets for adults is one tablet three times daily (in the morning, early afternoon, and at bedtime). Some patients may require two tablets at bedtime to assure overnight control of symptoms. For maintenance, a dosage of one tablet twice a day is frequently adequate.

Glycopyrronium Bromide Tablets 2 mg.

The recommended dosage of Glycopyrronium Bromide 2 mg Tablets for adults is one tablet two or three times daily at equally spaced intervals.

Paediatric population

Glycopyrronium Bromide Tablets are not recommended for use in children. Method of administration

For oral administration

In exceptional instances it may not be possible to administer the tablets orally, please refer to recommendations in section 6.6 for administration as an extemporaneous dispersion orally. This method is also suitable for administration via nasogastric tube or percutaneous endoscopic gastrostomy (PEG) tube.

4.3


Contraindications

Hypersensitivity to the active substance(s) or to any of the excipients listed in section 6.1.

In common with other antimuscarinics: angle-closure glaucoma; myasthenia gravis (large doses of quaternary ammonium compounds have been shown to block end plate nicotinic receptors); paralytic ileus; pyloric stenosis; prostatic enlargement.

4.4 Special warnings and precautions for use

Glycopyrronium Bromide Tablets should be used with caution in the elderly.

They should also be used with caution in gastro-oesophageal reflux disease, ulcerative colitis, acute myocardial infarction, hypertension, conditions characterised by tachycardia (including hyperthyroidism, cardiac insufficiency, cardiac surgery) because of the increase in heart rate produced by their administration, coronary artery disease and cardiac arrhythmias.

Diarrhoea may be an early symptom of incomplete intestinal obstruction, especially in patients with ileostomy or colostomy. In this instance treatment with this drug would be inappropriate and possibly harmful.

As Glycopyrronium Bromide inhibits sweating, patients with increased temperature (especially children) should be observed closely. In the presence of a high environmental temperature, heat prostration (fever and heat stroke due to decreased sweating) can occur with use of Glycopyrronium Bromide tablets.

Because of prolongation of renal elimination, repeated or large doses of Glycopyrronium Bromide should be avoided in patients with uraemia.

Large doses of quaternary anticholinergic compounds have been shown to block end plate nicotinic receptors. This should be considered before using Glycopyrronium Bromide in patients with myasthenia gravis.

Patients with rare hereditary problems of galactose intolerance, the Lapp lactase deficiency or glucose-galactose malabsorption should not take this medicine.

Paediatric population

Not applicable

4.5 Interaction with other medicinal products and other forms of interaction

Many drugs have antimuscarinic effects; concomitant use of two or more of such drugs can increase side-effects such as dry mouth, urine retention and constipation. Concomitant use can also lead to confusion in the elderly.

Anticholinergic agents may delay absorption of other medication given concomitantly.

Concurrent administration of anticholinergics and corticosteroids may result in increased intraocular pressure.

Concurrent use of anticholinergic agents with slow-dissolving tablets of digoxin may cause increased serum digoxin levels.

Increased antimuscarinic side-effects: amantadine; tricyclic antidepressants; antihistamines; clozapine; disopyramide; MAOIs; nefopam; pethidine; phenothiazines (increased antimuscarinic side effects of phenothiazines but reduced plasma concentrations)

Possibly increased antimuscarinic side-effects: tricyclic (related) antidepressants

Domperidone/Metoclopramide: antagonism of effect on gastro-intestinal activity

Ketoconazole: reduced absorption of ketoconazole Levodopa: absorption of levodopa possibly reduced Memantine: effects possibly enhanced by memantine

Nitrates: possibly reduced effect of sublingual nitrates (failure to dissolve under the tongue owing to dry mouth)

Parasympathomimetics: antagonism of effect

Ritodrine: tachycardia

Paediatric population

Not applicable

4.6 Fertility, pregnancy and lactation

Pregnancy

There are no or limited amount of data from the use of Glycopyrronium Bromide in pregnant women.

Animal studies do not indicate direct or indirect harmful effects with respect to reproductive toxicity (see section 5.3).

As a precautionary measure, it is preferable to avoid the use of Glycopyrronium Bromide Tablets during pregnancy.

Breastfeeding

It is unknown whether Glycopyrronium Bromide or its metabolites are excreted in human milk.

A risk to the newborns/infants cannot be excluded.

Breast-feeding should be discontinued during treatment with Glycopyrronium Bromide Tablets.

Fertility

Reproduction studies in rats revealed no teratogenic effects from Glycopyrronium Bromide; however, the potent anticholinergic action of this agent resulted in diminished rates of conception and of survival at weaning, in a dose-related manner. Other studies in dogs suggest that this may be due to diminished seminal secretion which is evident at high doses of Glycopyrronium Bromide.

No data are available in humans.

4.7 Effects on ability to drive and use machines

Glycopyrronium Bromide tablets may produce drowsiness or blurred vision. In this event, the patient should be warned not to engage in activities requiring mental alertness such as operating a motor vehicle or other machinery, or performing hazardous work while taking this drug.

4.8 Undesirable effects

Glycopyrronium Bromide may produce the following effects which are extensions of its fundamental pharmacological actions:

Eyes Disorders

Very rare (</10,000): angle-closure glaucoma

Not known: dilatation of the pupils with loss of accommodation

Gastrointestinal disorders Nausea, vomiting, and giddiness*

Not known: dry mouth, difficulty in micturition, constipation * These side effects occur occasionally

Skin and subcutaneous tissue disorders

Not known: inhibition of sweating, dryness of the skin and flushing Cardiac disorders

Not known: transient bradycardia (followed by tachycardia, palpitation and arrhythmias)

Respiratory, thoracic and mediastinal disorders

Not known: reduced bronchial secretions

Renal and urinary disorders

Not known: urinary urgency and retention

Psychiatric disorders Not known: photophobia

Nervous system disorders Confusion (particularly in the elderly)1

* These side effects occur occasionally

Immune system disorders

Not known: hypersensitivity, angioedema

Paediatric population Not applicable

Reporting of suspected adverse reactions

Reporting suspected adverse reactions after authorisation of the medicinal product is important. It allows continued monitoring of the benefit/risk balance of the medicinal product. Healthcare professionals are asked to report any suspected adverse reactions via the Yellow Card Scheme at: www.mhra.gov.uk/yellowcard.

4.9 Overdose

Since Glycopyrronium Bromide is a quaternary ammonium agent, symptoms of overdosage are peripheral rather than central in nature. Theoretically, with overdosage, a curare-like action may occur, i.e., neuro-muscular blockade leading to muscular weakness and possible paralysis.

The symptoms of overdosage of Glycopyrronium Bromide are peripheral in nature rather than central. Treatment is symptomatic and supportive.

•    To guard against further absorption of the drug-use gastric lavage, cathartics and/or enemas.

•    To combat hypotension - use pressor amines (norepinephrine, metaraminol) i.v.; and supportive care.

•    To combat respiratory depression - administer oxygen; utilize a respiratory stimulant such as Doxapram hydrochloride i.v.; artificial respiration.

5 PHARMACOLOGICAL PROPERTIES

5.1 Pharmacodynamic properties

Pharmacotherapeutic group: Synthetic anticholinergics, quaternary ammonium compounds;

ATC code: A03AB02

Mechanism of action

Glycopyrronium Bromide is a quaternary ammonium antimuscarinic agent and like other anticholinergic agents, it inhibits the action of acetylcholine on structures innervated by postganglionic cholinergic nerves and on smooth muscles that respond to acetylcholine but lack cholinergic innervation. These peripheral cholinergic receptors are present in the autonomic effector cells of smooth muscle, cardiac muscle, the sinoatrial node, the atrioventricular node, exocrine glands and to a limited degree in the autonomic ganglia. Thus it diminishes the volume and free acidity of gastric secretions and controls excessive pharyngeal, tracheal and bronchial secretions. Glycopyrronium Bromide antagonizes muscarinic symptoms (e.g. bronchorrhea, bronchospasm, bradycardia and intestinal hypermotility) induced by cholinergic drugs such as the anticholinesterases.

The highly polar quaternary ammonium group of Glycopyrronium Bromide limits its passage across lipid membranes, such as the blood-brain barrier, in contrast to atropine sulphate and scopolamine hydrobromide, which are non-polar tertiary amines which penetrate lipid barriers easily.

Pharmacodynamic effects

In common with other cholinergics, Glycopyrronium Bromide has gastrointestinal, genitourinary, cardiovascular, respiratory, and ophthalmic effects. Some antimuscarinic agents such as atropine cross the blood brain barrier to cause CNS effects such as drowsiness. In contrast, Glycopyrronium Bromide does not, so drowsiness is not a common adverse event. Specific known effects of Glycopyrronium Bromide include xerostomia, diminished gastrointestinal motility, decreased perspiration, increased body temperature, urinary retention, pupil dilation, loss of focusing accommodation, and increased heart rate. These expected effects of antimuscarinic drugs make them useful in treating certain conditions such as gastric ulcers, excess perspiration, overactive bladder, and pupil dilation during ophthalmologic examination. Treatment of drooling, is also a potential therapeutic use for the xerostomic effect of Glycopyrronium Bromide.

Clinical efficacy and safety

Glycopyrronium Bromide, like other anticholinergic (antimuscarinic) agents, inhibits the action of acetylcholine on structures innervated by postganglionic cholinergic nerves and on smooth muscles that respond to acetylcholine but lack cholinergic innervation. These peripheral cholinergic receptors are present in the autonomic effector cells of smooth muscle, cardiac muscle, the sino-atrial node, the atrioventricular node, exocrine glands, and, to a limited degree, in the autonomic ganglia. Thus, it diminishes the volume and free acidity of gastric secretions and controls excessive pharyngeal, tracheal, and bronchial secretions. Glycopyrronium Bromide antagonizes muscarinic symptoms (e.g., bronchorrhoea, bronchospasm, bradycardia, and intestinal hypermotility) induced by cholinergic drugs such as the anticholinesterases. The highly polar quaternary ammonium group of Glycopyrronium Bromide limits its passage across lipid membranes, such as the blood-brain barrier, in contrast to atropine sulphate and scopolamine hydrobromide, which are non-polar tertiary amines which penetrate lipid barriers easily.

The incidence of expected adverse events is dose-related. Therefore, dose is to be titrated to achieve an optimal balance of effectiveness with minimal anticholinergic associated adverse events.

5.2 Pharmacokinetic properties

Absorption

Glycopyrronium Bromide is poorly absorbed from the gastrointestinal tract; about 10 to 25% is absorbed after an oral dose. Oral Glycopyrronium Bromide has low oral bioavailability, a median of 3.3% is found in plasma.

Oral Glycopyrronium Bromide (2 mg) produces low plasma concentrations (Cmax 190 - 440 pg/mL) lasting up to 12 hours.

Food effect data indicate that the mean Cmax under fed high fat meal conditions is about 74% lower than the Cmax observed under fasting conditions.

Distribution

Glycopyrronium Bromide penetrates the blood-brain barrier poorly. Glycopyrronium Bromide crosses the placenta to a limited extent; and is not known whether it is distributed into milk.

Biotransformation

In adult patients who underwent surgery for cholelithiasis and were given a single IV dose of tritiated Glycopyrronium Bromide, approximately 85% of total radioactivity was excreted in urine and < 5% was present in T-tube drainage of bile. In both urine and bile, > 80% of the radioactivity corresponded to unchanged drug. These data suggest a small proportion of IV Glycopyrronium Bromide is excreted as one or more metabolites.

Elimination

Glycopyrronium Bromide is excreted largely unchanged in the urine. Approximately 65-80% of an IV Glycopyrronium Bromide dose was eliminated unchanged in urine in adults. In two studies, after IV administration to paediatric patients ages 1-14 years, mean clearance values ranged from 1.01- 1.41 L/kg/hr (range 0.32 - 2.22 L/kg/hr). In adults, IV clearance values were 0.54 ± 0.14 L/kg/hr.

5.3 Preclinical safety data

Acute toxicity of Glycopyrronium Bromide was studied in mice and rats. Following intraperitoneal administration, the LD50 was estimated to be 107 mg/kg in mice and 196 mg/kg in rats. Following oral dosing, the LD50 was estimated to be 1150 mg/kg in rats. Chronic oral administration doses of 4, 16, and 64 mg/kg for up to 27 weeks in dogs produced mydriasis, cycloplegia, xerostomia, emesis, occasional lacrimation, injection of sclera and rhinorrhoea. There were no changes in organ weight and histopathology showed no drug-related changes.

Although reproduction studies in rats and rabbits revealed no teratogenic effects from Glycopyrronium Bromide, safety in human pregnancy and lactation has not been established. Diminished rates of conception and of survival at weaning were observed in rats, in a dose-related manner. Studies in dogs suggest that this may be due to diminished seminal secretion which is evident at high doses of Glycopyrronium Bromide. The significance of this for man is not clear.

6 PHARMACEUTICAL PARTICULARS

6.1 List of excipients

Lactose Monohydrate Dibasic calcium phosphate Povidone

Sodium starch glycolate Magnesium stearate

Incompatibilities

6.2


Not applicable.

6.3    Shelf life

3 years

6.4    Special precautions for storage

None

6.5    Nature and contents of container

Aluminium blisters of 10, 14, 28, 30, 56, 60, 90 and 112 tablets.

Not all pack sizes may be marketed.

6.6 Special precautions for disposal and other handling of the product

No Special requirements for disposal.

For patients where oral administration of tablet is not possible, or not desired, administration by tablet solubilisation, and subsequent administration as an extemporaneous oral dispersion, or by administration via a nasogastric tube or a percutaneous endoscopic gastrostomy (PEG) tube. Such dispersions should be administered as suggested following. For dosage recommendations see section 4.2 previously.

Dispersions of a tablet, either 1 mg or 2 mg, is done as follows, use water as a dispersant medium and a 60 ml oral syringe as the vessel for dispersion.

-    Remove the plunger from the syringe and introduce a single tablet into the syringe barrel, replace the plunger and depress to just above tablet

-    Draw up the required volume of water, either potable or purified is suitable, a volume of 10 ml to 30 ml is recommended, dependent upon any patient fluid intake restrictions, and manually shake the syringe assembly for 30 seconds

-    Allow to stand for 5 minutes and manually shake for another 30 seconds

-    Allow to stand for a further 5 minutes and manually shake for another 30 seconds

-    Allow to stand for a further 5 minutes and manually shake for another 30 seconds

The tablet dispersion should be administered immediately after preparation. The dispersion is opaque, with some visible heavy particulates that are an inactive ingredient. The whole of the dispersion, including residue, is to be administered.

The studies conducted with the Nasogastric and PEG tubes evaluated three types of tubing, polyvinylchloride, polyurethane and silicone, which concluded that there were no significant differences evident between the three types of tubing and showed more than 90% overall recovery. Similarly, filtration studies prior to analysis were performed to evaluate if undissolved residues contained significant amounts of glycopyrronium bromide, concluded that there was no significant decrease in amount recovered. Filtered and unfiltered samples both showed overall recovery more than 90%.

Administration may be by the following routes:

-    Administration orally, as an aqueous dispersion. Following

administration of the dispersion, the oral syringe is rinsed with a further quantity of water, a minimum of 10 ml, that should also be taken to ensure complete dosing

-    Administration via either a nasogastric tube, or by a PEG tube. Tubes

made of polyvinylchloride, polyurethane, or silicon are suitable. There is no data available on tubes made of latex; such tubes should not be used. Immediately following administration of the initial dispersion, by connection of the oral syringe to the tube, the oral syringe is disconnected and rinsed with a further 10 ml of water, which should also be administered, in order to ensure complete dosing.

Such dispersions should not be used to provide doses below that of the tablet used to prepare the dispersion, since there is no data available to support such dose subdivision. Dispersion should be administered immediately following preparation. There is no data available to show that the medicine could be co-administered with food when administered through enteral tubes.

7 MARKETING AUTHORISATION HOLDER

Morningside Healthcare Ltd

115 Narborough Road

Leicester

LE30PA

UK

8    MARKETING AUTHORISATION NUMBER(S)

PL 20117/0095

9    DATE OF FIRST AUTHORISATION/RENEWAL OF THE

AUTHORISATION

06/02/2014

10 DATE OF REVISION OF THE TEXT

27/09/2016

1

   To combat peripheral anticholinergic effects (residual mydriasis, dry mouth, etc.) - utilize a quaternary ammonium anticholinesterase, such as neostigmine methylsulfate in increments of 0.25mg in adults. The dose may be repeated every 5 - 10 minutes until anticholinergic over-activity is reversed or up to a maximum of 2.5mg. Proportionately smaller doses should be used in children.