Loristiven 1.5 Mg Capsule Hard
Out of date information, search anotherSUMMARY OF PRODUCT CHARACTERISTICS
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4.1
4.2
NAME OF THE MEDICINAL PRODUCT
Loristiven 1.5 mg capsule, hard
QUALITATIVE AND QUANTITATIVE COMPOSITION
Each capsule contains rivastigmine hydrogen tartrate corresponding to rivastigmine 1.5 mg.
For a full list of excipients, see section 6.1.
PHARMACEUTICAL FORM
Capsule, hard
Hard gelatine capsules with opaque yellow cap and opaque yellow body with off-white powder
CLINICAL PARTICULARS
Therapeutic indications
Symptomatic treatment of mild to moderately severe Alzheimer’s dementia.
Symptomatic treatment of mild to moderately severe dementia in patients with idiopathic Parkinson’s disease.
Posology and method of administration
Treatment should be initiated and supervised by a physician experienced in the diagnosis and treatment of Alzheimer’s dementia or dementia associated with Parkinson’s disease. Diagnosis should be made according to current guidelines. Therapy with rivastigmine should only be started if a caregiver is available who will regularly monitor intake of the medicinal product by the patient.
Rivastigmine should be administered twice a day, with morning and evening meals. The capsules should be swallowed whole.
Initial dose
1.5 mg twice a day.
The starting dose is 1.5 mg twice a day. If this dose is well tolerated after a minimum of two weeks of treatment, the dose may be increased to 3 mg twice a day. Subsequent increases to 4.5 mg and then 6 mg twice a day should also be based on good tolerability of the current dose and may be considered after a minimum of two weeks of treatment at that dose level.
If adverse reactions (e.g. nausea, vomiting, abdominal pain or loss of appetite), weight decrease or worsening of extrapyramidal symptoms (e.g. tremor) in patients with dementia associated with Parkinson’s disease are observed during treatment, these may respond to omitting one or more doses. If adverse reactions persist, the daily dose should be temporarily reduced to the previous well-tolerated dose or the treatment may be discontinued.
Maintenance dose
The effective dose is 3 to 6 mg twice a day; to achieve maximum therapeutic benefit patients should be maintained on their highest well tolerated dose. The recommended maximum daily dose is 6 mg twice a day.
Maintenance treatment can be continued for as long as a therapeutic benefit for the patient exists.
Therefore, the clinical benefit of rivastigmine should be reassessed on a regular basis, especially for patients treated at doses less than 3 mg twice a day. If after 3 months of maintenance dose treatment the patient’s rate of decline in dementia symptoms is not altered favourably, the treatment should be discontinued. Discontinuation should also be considered when evidence of a therapeutic effect is no longer present.
Individual response to rivastigmine cannot be predicted. However, a greater treatment effect was seen in Parkinson’s disease patients with moderate dementia. Similarly a larger effect was observed in Parkinson’s disease patients with visual hallucinations (see section 5.1).
Treatment effect has not been studied in placebo-controlled trials beyond 6 months. Re-initiation of therapy
If treatment is interrupted for more than several days, it should be re-initiated at 1.5 mg twice daily.
Dose titration should then be carried out as described above.
Renal and hepatic impairment
Due to increased exposure in moderate renal and mild to moderate hepatic impairment, dosing recommendations to titrate according to individual tolerability should be closely followed (see section 5.2).
Patients with severe liver impairment have not been studied (see section 4.3).
Paediatric population
The safety and efficacy of Loristivenin children aged 0 to below 18 years have not been established. No data are available.
There is no relevant use of Loristivenin the paediatric population in children aged 0 to below 18 years in the treatment of Alzheimer’s dementia and dementia in patients with idiopathic Parkinson’s disease.
4.3 Contraindications
The use of this medicinal product is contraindicated in patients with known
hypersensitivity to the active substance rivastigmine, to other carbamate derivatives or to any of
the excipients listed in section 6.1 used in the formulation,
- Previous history of application site reactions suggestive of allergic contact dermatitis with
rivastigmine patch (see section 4.4).
4.4 Special warnings and precautions for use
The incidence and severity of adverse reactions generally increase with higher doses. If treatment is interrupted for more than several days, it should be re-initiated at 1.5 mg twice daily to reduce the possibility of adverse reactions (e.g. vomiting).
There have been rare post-marketing reports of patients experiencing disseminated skin hypersensitivity reactions when administered rivastigmine irrespective of the route of administration (oral, transdermal). In these cases, treatment should be discontinued (see section 4.3).
Patients and caregivers should be instructed accordingly.
Dose titration: Adverse reactions (e.g. hypertension and hallucinations in patients with Alzheimer’s dementia and worsening of extrapyramidal symptoms, in particular tremor, in patients with dementia associated with Parkinson’s disease) have been observed shortly after dose increase. They may respond to a dose reduction. In other cases, rivastigmine has been discontinued (see section 4.8).
Gastrointestinal disorders such as nausea and vomiting may occur particularly when initiating treatment and/or increasing the dose. These adverse reactions occur more commonly in women.
Patients with Alzheimer’s disease may lose weight. Cholinesterase inhibitors, including rivastigmine, have been associated with weight loss in these patients. During therapy patient’s weight should be monitored.
In case of severe vomiting associated with rivastigmine treatment, appropriate dose adjustments as recommended in section 4.2 must be made. Some cases of severe vomiting were associated with oesophageal rupture (see section 4.8). Such events appeared to occur particularly after dose increments or high doses of rivastigmine.
Care must be taken when using rivastigmine in patients with sick sinus syndrome or conduction defects (sino-atrial block, atrio-ventricular block) (see section 4.8).
Rivastigmine may cause increased gastric acid secretions. Care should be exercised in treating patients with active gastric or duodenal ulcers or patients predisposed to these conditions.
Cholinesterase inhibitors should be prescribed with care to patients with a history of asthma or obstructive pulmonary disease.
Cholinomimetics may induce or exacerbate urinary obstruction and seizures. Caution is recommended in treating patients predisposed to such diseases.
The use of rivastigmine in patients with severe dementia of Alzheimer’s disease or associated with Parkinson’s disease, other types of dementia or other types of memory impairment (e.g. age-related cognitive decline) has not been investigated and therefore use in these patient populations is not recommended.
Like other cholinomimetics, rivastigmine may exacerbate or induce extrapyramidal symptoms.
Worsening (including bradykinesia, dyskinesia, gait abnormality) and an increased incidence or severity of tremor have been observed in patients with dementia associated with Parkinson’s disease (see section 4.8). These events led to the discontinuation of rivastigmine in some cases (e.g. discontinuations due to tremor 1.7% on rivastigmine vs 0% on placebo). Clinical monitoring is recommended for these adverse reactions.
4.5 Interaction with other medicinal products and other forms of interaction
As a cholinesterase inhibitor, rivastigmine may exaggerate the effects of succinylcholine-type muscle relaxants during anaesthesia. Caution is recommended when selecting anaesthetic agents. Possible dose adjustments or temporarily stopping treatment can be considered if needed.
In view of its pharmacodynamic effects, rivastigmine should not be given concomitantly with other cholinomimetic substances and might interfere with the activity of anticholinergic medicinal products.
No pharmacokinetic interaction was observed between rivastigmine and digoxin, warfarin, diazepam or fluoxetine in studies in healthy volunteers. The increase in prothrombin time induced by warfarin is not affected by administration of rivastigmine. No untoward effects on cardiac conduction were observed following concomitant administration of digoxin and rivastigmine.
According to its metabolism, metabolic interactions with other medicinal products appear unlikely, although rivastigmine may inhibit the butyrylcholinesterase mediated metabolism of other substances.
4.6 Pregnancy and lactation
For rivastigmine no clinical data on exposed pregnancies are available. No effects on fertility or embryofoetal development were observed in rats and rabbits, except at doses related to maternal toxicity.
In peri/postnatal studies in rats, an increased gestation time was observed. Rivastigmine should not be used during pregnancy unless clearly necessary.
In animals, rivastigmine is excreted into milk. It is not known if rivastigmine is excreted into human milk. Therefore, women on rivastigmine should not breastfeed.
4.7 Effects on ability to drive and use machines
Alzheimer’s disease may cause gradual impairment of driving performance or compromise the ability to use machinery. Furthermore, rivastigmine can induce dizziness and somnolence, mainly when initiating treatment or increasing the dose. As a consequence, rivastigmine has minor or moderate influence on the ability to drive and use machines. Therefore, the ability of patients with dementia on rivastigmine to continue driving or operating complex machines should be routinely evaluated by the treating physician.
4.8 Undesirable effects
The most commonly reported adverse reactions are gastrointestinal, including nausea (38%) and vomiting (23%), especially during titration. Female patients in clinical studies were found to be more susceptible than male patients to gastrointestinal adverse reactions and weight loss.
Adverse reactions are ranked Table 1 and Table 2 under headings of frequency, the most frequent first, using the following convention: Very common (>1/10); common (>1/100, <1/10); uncommon (>1/1,000, <1/100); rare (>1/10,000, <1/1,000); very rare (<1/10,000) and not known (cannot be estimated from the available data).
The following adverse reactions, listed below in Table 1, have been accumulated in patients with Alzheimer’s dementia treated with Loristiven.
Table 1
|
Infections and infestations Very rare |
Urinary infection |
|
Psychiatric disorders Common Common Uncommon Uncommon Very rare |
Agitation Confusion Insomnia Depression Hallucinations |
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Nervous system disorders Very common Common Common Common Uncommon Rare Very rare |
Dizziness Headache Somnolence Tremor Syncope Seizures Extrapyramidal symptoms (including worsening of Parkinson’s disease) |
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Cardiac disorders Rare Very rare |
Angina pectoris Cardiac arrhythmia (e.g. bradycardia, atrio-ventricular block, atrial fibrillation and tachycardia) |
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Vascular disorders Very rare |
Hypertension |
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Gastrointestinal disorders Very common Very common Very common Common Rare Very rare Very rare Not known Metabolism and nutritional disorders |
Nausea Vomiting Diarrhoea Abdominal pain and dyspepsia Gastric and duodenal ulcers Gastrointestinal haemorrhage Pancreatitis Some cases of severe vomiting were associated with oesophageal rupture (see section 4.4). |
|
Very common |
Anorexia |
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Hepatobiliary disorders Uncommon |
Elevated liver function tests |
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Skin and subcutaneous tissue disorders Common Rare |
Sweating increased Rashes |
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General disorders and administration site conditions Common Common Uncommon |
Fatigue and asthenia Malaise Accidental fall |
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Investigations | |
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Common |
Weight loss |
Table 2 shows the adverse reactions reported during clinical studies conducted in patients with dementia associated with Parkinson’s disease treated with rivastigmine capsules.
Table 2
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Psychiatric disorders Common Common Common Common Common |
Insomnia Anxiety Restlessness Hallucination, visual Depression |
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Nervous system disorders Very common Common Common Common Common Common Common Common Common Uncommon |
Tremor Dizziness Somnolence Headache Worsening of Parkinson’s disease Bradykinesia Dyskinesia Hypokinesia Cogwheel rigidity Dystonia |
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Cardiac disorders Common Uncommon Uncommon |
Bradycardia Atrial Fibrillation Atrioventricular block |
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Vascular disorders Common Uncommon |
Hypertension Hypertension |
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Gastrointestinal disorders Very common Very common Common Common Common |
Nausea Vomiting Diarrhoea Abdominal pain and dyspepsia Salivary hypersecretion |
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Skin and subcutaneous tissue disorders Common |
Sweating increased |
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Metabolism and nutritional disorders Common Common |
Decreased appetiteDehydration |
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General disorders and administration site conditions Very common Common Common Common |
Fall Fatigue and asthenia Gait disturbance Parkinson gait |
Table 3 lists the number and percentage of patients from the specific 24-week clinical study conducted with rivastigmine in patients with dementia associated with Parkinson’s disease with pre-defined adverse events that may reflect worsening of parkinsonian symptoms.
Table 3
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Pre-defined adverse events that may reflect worsening of parkinsonian symptoms in patients with dementia associated with Parkinson’s disease |
Rivastigmine n (%) |
Placebo n (%) |
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Total patients studied Total patients with pre-defined AE(s) |
362 (100) 99 (27.3) |
179 (100) 28 (15.6) |
|
Tremor |
37 (10.2) |
7 (3.9) |
|
Fall |
21 (5.8) |
11 (6.1) |
|
Parkinson’s disease (worsening) |
12 (3.3) |
2 (1.1) |
|
Salivary hypersecretion |
5 (1.4) |
0 |
|
Dyskinesia |
5 (1.4) |
1 (0.6) |
|
Parkinsonism |
8 (2.2) |
1 (0.6) |
|
Hypokinesia |
1 (0.3) |
0 |
|
Movement disorder |
1 (0.3) |
0 |
|
Bradykinesia |
9 (2.5) |
3 (1.7) |
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Dystonia |
3 (0.8) |
1 (0.6) |
|
Gait abnormality |
5 (1.4) |
0 |
|
Muscle rigidity |
1 (0.3) |
0 |
|
Balance disorder |
3 (0.8) |
2 (1.1) |
|
Musculoskeletal stiffness |
3 (0.8) |
0 |
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Rigors |
1 (0.3) |
0 |
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Motor dysfunction |
1 (0.3) |
0 |
4.9 Overdose
Symptoms
Most cases of accidental overdose have not been associated with any clinical signs or symptoms and almost all of the patients concerned continued rivastigmine treatment. Where symptoms have occurred, they have included nausea, vomiting and diarrhoea, hypertension or hallucinations. Due to the known vagotonic effect of cholinesterase inhibitors on heart rate, bradycardia and/or syncope may also occur.
Ingestion of 46 mg occurred in one case; following conservative management the patient fully recovered within 24 hours.
Treatment
As rivastigmine has a plasma half-life of about 1 hour and a duration of acetylcholinesterase inhibition of about 9 hours, it is recommended that in cases of asymptomatic overdose no further dose of rivastigmine should be administered for the next 24 hours. In overdose accompanied by severe nausea and vomiting,
the use of antiemetics should be considered. Symptomatic treatment for other adverse reactions should be given as necessary.
In massive overdose, atropine can be used. An initial dose of 0.03 mg/kg intravenous atropine sulphate is recommended, with subsequent doses based on clinical response. Use of scopolamine as an antidote is not recommended.
5 PHARMACOLOGICAL PROPERTIES
5.1 Pharmacodynamic properties
Pharmacotherapeutic group: anticholinesterases, ATC code: N06DA03
Rivastigmine is an acetyl- and butyrylcholinesterase inhibitor of the carbamate type, thought to facilitate cholinergic neurotransmission by slowing the degradation of acetylcholine released by functionally intact cholinergic neurones. Thus, rivastigmine may have an ameliorative effect on cholinergic-mediated cognitive deficits in dementia associated with Alzheimer’s disease and Parkinson’s disease.
Rivastigmine interacts with its target enzymes by forming a covalently bound complex that temporarily inactivates the enzymes. In healthy young men, an oral 3 mg dose decreases acetylcholinesterase (AChE) activity in CSF by approximately 40% within the first 1.5 hours after administration. Activity of the enzyme returns to baseline levels about 9 hours after the maximum inhibitory effect has been achieved. In patients with Alzheimer’s disease, inhibition of AChE in CSF by rivastigmine was dose-dependent up to 6 mg given twice daily, the highest dose tested. Inhibition of butyrylcholinesterase activity in CSF of 14 Alzheimer patients treated by rivastigmine was similar to that of AChE.
Clinical studies in Alzheimer’s dementia
The efficacy of rivastigmine has been established through the use of three independent, domain specific, assessment tools which were assessed at periodic intervals during 6 month treatment periods. These include the ADAS-Cog (Alzheimer’s Disease Assessment Scale - Cognitive subscale, a performance based measure of cognition), the CIBIC-Plus (Clinician’s Interview Based Impression of Change-Plus, a comprehensive global assessment of the patient by the physician incorporating caregiver input), and the PDS (Progressive Deterioration Scale, a caregiver-rated assessment of the activities of daily living including personal hygiene, feeding, dressing, household chores such as shopping, retention of ability to orient oneself to surroundings as well as involvement in activities relating to finances, etc.).
The patients studied had an MMSE (Mini-Mental State Examination) score of 10-24.
The results for clinically relevant responders pooled from two flexible dose studies out of the three pivotal 26-week multicentre studies in patients with mild-to-moderately severe Alzheimer’s Dementia, are provided in Table 4 below. Clinically relevant improvement in these studies was defined a priori as at least 4-point improvement on the ADAS-Cog, improvement on the CIBIC-Plus, or at least a 10% improvement on the PDS.
In addition, a post-hoc definition of response is provided in the same table. The secondary definition of response required a 4-point or greater improvement on the ADAS-Cog, no worsening on the CIBIC-Plus, and no worsening on the PDS. The mean actual daily dose for responders in the 6-12 mg group, corresponding to this definition, was 9.3 mg. It is important to note that the scales used in this indication vary and direct comparisons of results for different therapeutic agents are not valid.
Table 4
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Patients with Clinically Significant Response (%) | ||||
|
Intent to Treat |
Last Observation Carried Forward | |||
|
Response Measure |
Rivastigmine 6-12 mg |
Placebo |
Rivastigmine 6-12 mg |
Placebo |
|
N=473 |
N=472 |
N=379 |
N=444 | |
|
ADAS-Cog: improvement of at least 4 points |
21*** |
12 |
25*** |
12 |
|
CIBIC-Plus: improvement |
29*** |
18 |
32*** |
19 |
|
PDS: improvement of at least 10% |
26*** |
17 |
30*** |
18 |
|
At least 4 points improvement on ADAS-Cog with no worsening on CIBIC-Plus and PDS |
10* |
6 |
12** |
6 |
*p<0.05, **p<0.01, ***p<0.001
Clinical studies in dementia associated with Parkinson’s disease The efficacy of rivastigmine in dementia associated with Parkinson’s disease has been demonstrated in a 24-week multicentre, double-blind, placebo-controlled core study and its 24-week open-label extension phase. Patients involved in this study had an MMSE (Mini-Mental State Examination) score of 10-24. Efficacy has been established by the use of two independent scales which were assessed at regular intervals during a 6-month treatment period as shown in Table 5 below: the ADAS-Cog, a measure of cognition, and the global measure ADCS-CGIC (Alzheimer’s Disease Cooperative Study- Clinician’s Global Impression of Change).
Table 5
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Dementia associated with Parkinson’s Disease |
ADAS-Cog Rivastigmine |
ADAS-Cog Placebo |
ADCS-CGIC Rivastigmine |
ADCS-CGIC Placebo |
|
ITT + RDO population |
(n=329) |
(n=161) |
(n=329) |
(n=165) |
|
Mean baseline ± SD |
23.8 ± 10.2 |
24.3 ± 10.5 |
n/a |
n/a |
|
Mean change at 24 weeks ± SD |
2.1 ± 8.2 |
-0.7 ± 7.5 |
3.8 ± 1.4 |
4.3 ± 1.5 |
'Based on ANCOVA with treatment and country as factors and baseline ADAS-Cog as a covariate. A positive change indicates improvement.
|
Adjusted treatment | ||||
|
difference |
2.881 |
n/a | ||
|
p-value versus placebo |
<0.001' |
0.0072 | ||
|
ITT - LOCF population |
(n=287) |
(n=154) |
(n=289) |
(n=158) |
|
Mean baseline ± SD |
24.0 ± 10.3 |
24.5 ± 10.6 |
n/a |
n/a |
|
Mean change at 24 weeks |
2.5 ± 8.4 |
-0.8 ± 7.5 |
3.7 ± 1.4 |
4.3 ± 1.5 |
|
± SD | ||||
|
Adjusted treatment | ||||
|
difference |
3.541 |
n/a | ||
|
p-value versus placebo |
<0.001' |
<0.0012 | ||
2Mean data shown for convenience, categorical analysis performed using van Elteren test ITT: Intent-To-Treat; RDO: Retrieved Drop Outs; LOCF: Last Observation Carried Forward
Although a treatment effect was demonstrated in the overall study population, the data suggested that a larger treatment effect relative to placebo was seen in the subgroup of patients with moderate dementia associated with Parkinson’s disease. Similarly a larger treatment effect was observed in those patients with visual hallucinations (see Table 6).
Table 6
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Dementia associated with |
ADAS-Cog |
ADAS-Cog |
ADAS-Cog |
ADAS-Cog |
|
Parkinson’s Disease |
Rivastigmine |
Placebo |
Rivastigmine |
Placebo |
|
Patients with visual |
Patients without visual | |||
|
hallucinations |
hallucinations | |||
|
ITT + RDO population |
(n=107) |
(n=60) |
(n=220) |
(n=101) |
|
Mean baseline ± SD |
25.4 ± 9.9 |
27.4 ± 10.4 |
23.1 ± 10.4 |
22.5 ± 10.1 |
|
Mean change at 24 weeks |
1.0 ± 9.2 |
-2.1 ± 8.3 |
2.6 ± 7.6 |
0.1 ± 6.9 |
|
± SD | ||||
|
Adjusted treatment | ||||
|
difference |
4.271 |
2.091 | ||
|
p-value versus placebo |
0.0021 |
0.0151 | ||
|
Patients with moderate |
Patients with mild dementia | |||
|
dementia (MMSE 10-17) |
(MMSE 18-24) | |||
|
ITT + RDO population |
(n=87) |
(n=44) |
(n=237) |
(n=115) |
|
Mean baseline ± SD |
32.6 ± 10.4 |
33.7 ± 10.3 |
20.6 ± 7.9 |
20.7 ± 7.9 |
|
Mean change at 24 weeks |
2.6 ± 9.4 |
-1.8 ± 7.2 |
1.9 ± 7.7 |
-0.2 ± 7.5 |
|
± SD | ||||
|
Adjusted treatment | ||||
|
difference |
4.731 |
2.141 | ||
|
p-value versus placebo |
0.0021 |
0.0101 | ||
'Based on ANCOVA with treatment and country as factors and baseline ADAS-Cog as a covariate. A positive change indicates improvement.
ITT: Intent-To-Treat; RDO: Retrieved Drop Outs
The European Medicines Agency has waived the obligation to submit the results of studies with Loristiven in all subsets of the paediatric population in the treatment of Alzheimer’s dementia and in the treatment of dementia in patients with idiopathic Parkinson’s disease (see section 4.2 for information on paediatric use).
5.2 Pharmacokinetic properties
Absorption
Rivastigmine is rapidly and completely absorbed. Peak plasma concentrations are reached in approximately 1 hour. As a consequence of rivastigmine’s interaction with its target enzyme, the increase in bioavailability is about 1.5-fold greater than that expected from the increase in dose. Absolute bioavailability after a 3 mg dose is about 36%±13%. Administration of rivastigmine with food delays absorption (tmax) by 90 min and lowers Cmax and increases AUC by approximately 30%.
Distribution
Protein binding of rivastigmine is approximately 40%. It readily crosses the blood brain barrier and has an apparent volume of distribution in the range of 1.8-2.7 l/kg.
Metabolism
Rivastigmine is rapidly and extensively metabolised (half-life in plasma approximately 1 hour), primarily via cholinesterase-mediated hydrolysis to the decarbamylated metabolite. In vitro, this metabolite shows minimal inhibition of acetylcholinesterase (<10%). Based on evidence from in vitro and animal studies the major cytochrome P450 isoenzymes are minimally involved in rivastigmine metabolism. Total plasma clearance of rivastigmine was approximately 130 l/h after a 0.2 mg intravenous dose and decreased to 70 l/h after a 2.7 mg intravenous dose.
Excretion
Unchanged rivastigmine is not found in the urine; renal excretion of the metabolites is the major route of elimination. Following administration of 14C-rivastigmine, renal elimination was rapid and essentially complete (>90%) within 24 hours. Less than 1% of the administered dose is excreted in the faeces. There is no accumulation of rivastigmine or the decarbamylated metabolite in patients with Alzheimer’s disease.
Elderly subjects
While bioavailability of rivastigmine is greater in elderly than in young healthy volunteers, studies in Alzheimer patients aged between 50 and 92 years showed no change in bioavailability with age.
Subjects with hepatic impairment
The Cmax of rivastigmine was approximately 60% higher and the AUC of rivastigmine was more than twice as high in subjects with mild to moderate hepatic impairment than in healthy subjects.
Subjects with renal impairment
Cmax and AUC of rivastigmine were more than twice as high in subjects with moderate renal impairment compared with healthy subjects; however there were no changes in Cmax and AUC of rivastigmine in subjects with severe renal impairment.
5.3 Preclinical safety data
Repeated-dose toxicity studies in rats, mice and dogs revealed only effects associated with an exaggerated pharmacological action. No target organ toxicity was observed. No safety margins to human exposure were achieved in the animal studies due to the sensitivity of the animal models used.
Rivastigmine was not mutagenic in a standard battery of in vitro and in vivo tests, except in a chromosomal aberration test in human peripheral lymphocytes at a dose 104 times the maximum clinical exposure. The in vivo micronucleus test was negative.
No evidence of carcinogenicity was found in studies in mice and rats at the maximum tolerated dose, although the exposure to rivastigmine and its metabolites was lower than the human exposure. When normalised to body surface area, the exposure to rivastigmine and its metabolites was approximately equivalent to the maximum recommended human dose of 12 mg/day(on mg/m2 basis); however, when compared to the maximum human dose of 12mg/Kg , a multiple of approximately 6-fold was achieved in animals.
In animals, rivastigmine crosses the placenta and is excreted into milk. Oral studies in pregnant rats and rabbits gave no indication of teratogenic potential on the part of rivastigmine.
6 PHARMACEUTICAL PARTICULARS
6.1 List of excipients
Granules:
Microcrystalline cellulose
Hypromellose
Silica, colloidal anhydrous
Magnesium stearate
Body cap:
Gelatin
Titanium dioxide (E171) Yellow iron oxide (E172)
6.2 Incompatibilities
Not applicable.
6.3 Shelf life
3 years
6.4 Special precautions for storage
Do not store above 30°C.
6.5 Nature and contents of container
- Blister of transparent PVC/PE/PVDC - Aluminium foil. Each box contains 28, 56 or 112 capsules.
Not all pack sizes may be marketed.
6.6 Special precautions for disposal and other handling
No special requirements.
7 MARKETING AUTHORISATION HOLDER
Pharmathen Pharmaceuticals S.A.
6 Dervenakion Street Pallini Attikis 15351 Greece
8 MARKETING AUTHORISATION NUMBER(S)
PL 17277/0120
9 DATE OF FIRST AUTHORISATION/RENEWAL OF THE AUTHORISATION
18/05/2010
10 DATE OF REVISION OF THE TEXT
06/03/2013