1. Name Of The Medicinal Product
Madopar 50 mg/12.5 mg Hard Capsules
Madopar 100 mg/25 mg Hard Capsules
Madopar 200 mg/50 mg Hard Capsules
2. Qualitative And Quantitative Composition
Madopar 50 mg/12.5 mg: Each capsule contains 50.0 mg Levodopa and 12.5 mg Benserazide (as benserazide hydrochloride).
Madopar 100 mg/25 mg: Each capsule contains 100.0 mg Levodopa and 25 mg Benserazide (as benserazide hydrochloride).
Madopar 200 mg/50 mg: Each capsule contains 200.0 mg Levodopa and 50 mg Benserazide (as benserazide hydrochloride).
For excipients, see section 6.1
3. Pharmaceutical Form
Capsules, hard.
Madopar 50 mg/12.5 mg: Light grey opaque body and a powder blue opaque cap, imprinted with the name 'Roche' in black ink on both sides.
Madopar 100 mg/25 mg: Pale pink opaque body and a powder blue opaque cap, imprinted with the name 'Roche' in black ink on both sides.
Madopar 200 mg/50 mg: Light brown opaque body and a powder blue opaque cap, imprinted with the name 'Roche' in black ink on both sides.
4. Clinical Particulars
4.1 Therapeutic Indications
Parkinsonism - idiopathic post-encephalitic.
Previous neurosurgery is not a contra-indication to Madopar.
4.2 Posology And Method Of Administration
Dosage and administration are variable and no more than a guide can be given.
Adults
Patients not previously treated with levodopa
The recommended initial dose is one capsule or dispersible tablet of Madopar 50 mg/12.5 mg three or four times daily. If the disease is at an advanced stage, the starting dose should be one capsule or dispersible tablet of Madopar 100 mg/25 mg three times daily.
The daily dosage should then be increased by one capsule or dispersible tablet of Madopar 100 mg/25 mg, or their equivalent, once or twice weekly until a full therapeutic effect is obtained, or side-effects supervene.
In some elderly patients, it may suffice to initiate treatment with one capsule or dispersible tablet of Madopar 50 mg/12.5 mg once or twice daily, increasing by one capsule or dispersible tablet every third or fourth day.
The effective dose usually lies within the range of four to eight capsules or dispersible tablets of Madopar 100 mg/25 mg (two to four capsules of Madopar 200 mg/50 mg) daily in divided doses, most patients requiring no more than six capsules or dispersible tablets of Madopar 100 mg/25 mg daily.
Optimal improvement is usually seen in one to three weeks but the full therapeutic effect of Madopar may not be apparent for some time. It is advisable, therefore, to allow several weeks to elapse before contemplating dosage increments above the average dose range. If satisfactory improvement is still not achieved, the dose of Madopar may be increased but with caution. It is rarely necessary to give more than ten capsules or dispersible tablets of Madopar 100 mg /25 mg (five capsules of Madopar 200 mg/50 mg) per day.
Treatment should be continued for at least six months before failure is concluded from the absence of a clinical response.
Madopar 50 mg/12.5 mg capsules or dispersible tablets may be used to facilitate adjustment of dosage to the needs of the individual patient. Patients who experience fluctuations in response may be helped by dividing the dosage into smaller, more frequent doses with the aid of Madopar 50 mg/12.5 mg capsules or dispersible tablets without, however, altering the total daily dose.
Madopar 200 mg/50 mg capsules are only for maintenance therapy once the optimal dosage has been determined using Madopar 100 mg/25 mg capsules or dispersible tablets.
Patients previously treated with levodopa
The following procedure is recommended: Levodopa alone should be discontinued and Madopar started on the following day. The patient should be initiated on a total of one less Madopar 100 mg/25 mg capsule or dispersible tablet daily than the total number of 500 mg levodopa tablets or capsules previously taken (for example, if the patient had previously taken 2g levodopa daily, then he should start on three capsules or dispersible tablets Madopar 100 mg/25 mg daily on the following day). Observe the patient for one week and then, if necessary, increase the dosage in the manner described for new patients.
Patients previously treated with other levodopa/decarboxylase inhibitor combinations
Previous therapy should be withdrawn for 12 hours. In order to minimise the potential for any effects of levodopa withdrawal, it may be beneficial to discontinue previous therapy at night and institute Madopar therapy the following morning. The initial Madopar dose should be one capsule or dispersible tablet of Madopar 50 mg/12.5 mg three or four times daily. This dose may then be increased in the manner described for patients not previously treated with levodopa.
Other anti-Parkinsonian drugs may be given with Madopar. Existing treatment with other anti-Parkinsonian drugs, e.g. anticholinergics or amantadine, should be continued during initiation of Madopar therapy. However, as treatment with Madopar proceeds and the therapeutic effect becomes apparent, the dosage of the other drugs may need to be reduced or the drugs gradually withdrawn.
Elderly
Although there may be an age-related decrease in tolerance to levodopa in the elderly, Madopar appears to be well-tolerated and side-effects are generally not troublesome.
Children
Not to be given to patients under 25 years of age: therefore, no dosage recommendations are made for the administration of Madopar to children.
Madopar capsules are for oral administration. They should be taken with, or immediately after, meals.
4.3 Contraindications
Madopar must not be given to patients with known hypersensitivity to levodopa or benserazide.
Madopar is contra-indicated in narrow-angle glaucoma (it may be used in wide-angle glaucoma provided that the intra-ocular pressure remains under control); severe psychoneuroses or psychoses; severe endocrine, renal, hepatic or cardiac disorders.
It should not be given in conjunction with, or within 2 weeks of withdrawal of, monoamine oxidase (MAO) inhibitors, except selective MAO-B inhibitors (e.g. selegiline) or selective MAO-A inhibitors (e.g. moclobemide).
It should not be given to patients under 25 years of age.
It should not be given to pregnant women or to women of childbearing potential in the absence of adequate contraception. If pregnancy occurs in a woman taking Madopar, the drug must be discontinued.
Suspicion has arisen that levodopa may activate a malignant melanoma. Therefore, Madopar should not be used in persons who have a history of, or who may be suffering from, a malignant melanoma.
4.4 Special Warnings And Precautions For Use
When other drugs must be given in conjunction with Madopar, the patient should be carefully observed for unusual side-effects or potentiating effects.
In the event of general anaesthesia being required, Madopar therapy may be continued as long as the patient is able to take fluids and medication by mouth. If therapy is temporarily interrupted, the usual daily dosage may be administered as soon as the patient is able to take oral medication. Whenever therapy has been interrupted for longer periods, dosage should again be adjusted gradually; however, in many cases the patient can rapidly be returned to his previous therapeutic dosage.
If a patient has to undergo emergency surgery, when Madopar has not been withdrawn, anaesthesia with halothane should be avoided.
There have been occasional reports of a neuroleptic malignant-like syndrome, involving hyperthermia, on abrupt withdrawal of levodopa preparations. Sudden discontinuation of Madopar, without close supervision, or "drug holidays" should therefore be avoided.
Pyridoxine (vitamin B6) may be given with Madopar since the presence of a decarboxylase inhibitor protects against the peripheral levodopa transformation facilitated by pyridoxine.
Levodopa has been associated with somnolence and episodes of sudden sleep onset. Sudden onset of sleep during daily activities, in some cases without awareness or warning signs, has been reported very rarely. Patients must be informed of this and advised to exercise caution while driving or operating machines during treatment with levodopa. Patients who have experienced somnolence and/or an episode of sudden sleep onset must refrain from driving or operating machines. Furthermore a reduction of dosage or termination of therapy may be considered.
Pathological gambling, increased libido and hypersexuality have been reported in patients treated with dopamine agonists and/or levodopa for Parkinson's disease.
Care should be taken when using Madopar in the following circumstances: in endocrine, renal, pulmonary or cardiovascular disease, particularly where there is a history of myocardial infarction or arrhythmia; psychiatric disturbances (e.g. depression); hepatic disorder; peptic ulcer; osteomalacia; where sympathomimetic drugs may be required (e.g. bronchial asthma), due to possible potentiation of the cardiovascular effects of levodopa; where antihypertensive drugs are being used, due to possible increased hypotensive action.
Periodic evaluation of hepatic, haemopoietic, renal and cardiovascular functions is advised.
Patients with diabetes should undergo frequent blood sugar tests and the dosage of anti-diabetic agents should be adjusted to blood sugar levels.
Patients who improve on Madopar therapy should be advised to resume normal activities gradually as rapid mobilisation may increase the risk of injury.
4.5 Interaction With Other Medicinal Products And Other Forms Of Interaction
Ferrous sulphate decreases the maximum plasma concentration and the AUC of levodopa by 30
Opioids and drugs which interfere with central amine mechanisms, such as rauwolfia alkaloids (reserpine), tetrabenazine (Nitoman), metoclopramide, phenothiazines, thioxanthenes, butyrophenones, amphetamines and papaverine, should be avoided where possible. If, however, their administration is considered essential, extreme care should be exercised and a close watch kept for any signs of potentiation, antagonism or other interactions and for unusual side-effects. Metoclopramide has been shown to increase the rate of levodopa absorption.
Co-administration of the anticholinergic drug trihexyphenidyl with Madopar reduces the rate, but not the extent, of levodopa absorption.
Combination with other anti-Parkinsonian agents (anticholinergics, amantadine, dopamine agonists) is permissible, though both the desired and undesired effects of treatment may be intensified. It may be necessary to reduce the dosage of Madopar or the other substance. When initiating an adjuvant treatment with a COMT inhibitor, a reduction of the dosage of Madopar may be necessary. Anticholinergics should not be withdrawn abruptly when Madopar therapy is instituted, as levodopa does not begin to take effect for some time.
There have been rare reports of possible antagonism of levodopa by diazepam. Isolated cases of hypertensive crisis have been reported with concomitant use of tricyclic antidepressants. Madopar must not be given in conjunction with MAO inhibitors (see section 4.3 Contra-indications)
Use with antihypertensive agents may increase the hypotensive response, while sympathomimetics may increase the cardiovascular side-effects of levodopa.
Levodopa may interfere chemically with several diagnostic laboratory tests including those for glucose, ketone bodies or catecholamines in urine and for glucose or uric acid in blood. Levodopa therapy has been reported to inhibit the response to protirelin in tests of thyroid function. Coombs' tests may give a false-positive result in patients taking Madopar.
4.6 Pregnancy And Lactation
Madopar is contra-indicated in pregnancy and in women of childbearing potential in the absence of adequate contraception, since there is evidence of harmful effects in studies in pregnant rabbits and the benserazide component has been found to be associated with skeletal malformations in the rat. If pregnancy occurs in a woman taking Madopar, the drug must be discontinued. Patients taking Madopar should not breast-feed their infants.
4.7 Effects On Ability To Drive And Use Machines
Patients being treated with levodopa and presenting with somnolence and/or sudden sleep episodes must be informed to refrain from driving or engaging in activities where impaired alertness may put themselves or others at risk of serious injury or death (e.g. operating machines) until such recurrent episodes and somnolence have resolved (see Section 4.4).
4.8 Undesirable Effects
Gastrointestinal:
- Anorexia, nausea, vomiting, diarrhoea (less commonly than with levodopa) mainly occurring in the early stages of treatment. May be controlled by taking Madopar with some food or liquid or increasing the dose slowly.
- Gastro-intestinal bleeding has been reported with levodopa therapy.
- Isolated cases of loss or alterations of taste.
Skin:
- rarely allergic reactions such as pruritus and rash.
Cardiovascular:
- Occasional reports of cardiac arrhythmias and orthostatic hypotension (less frequently than with levodopa alone). Orthostatic disorders usually improve following dosage reduction.
Haematological:
- Rare cases of haemolytic anaemia, transient leucopenia and thrombocytopenia.
Neuropsychiatric:
- Psychiatric disturbances are common in Parkinsonian patients, including those treated with levodopa, including mild elation, anxiety, agitation, insomnia, drowsiness, depression, aggression, delusions, hallucinations, temporal disorientation and “unmasking” of psychoses.
- Levodopa is associated with somnolence and has been associated very rarely with excessive daytime somnolence and sudden sleep onset episodes.
- Patients treated with dopamine agonists and/or levodopa for treatment of Parkinson's disease, especially at high doses, have been reported as exhibiting signs of pathological gambling, increased libido and hypersexuality, generally reversible upon reduction of the dose of treatment discontinuation.
- Involuntary movements (e.g. choreiform or athetotic, oral dyskinesias, “paddling” foot) are common, particularly on long-term administration. These are usually dose-dependant and may disappear or become tolerable after dose adjustment.
Laboratory abnormalities:
- Transient rises in SGOT, SGPT and alkaline phosphatase values have been noted.
- Increase of gamma-Glutamyltransferase has been reported.
- Serum uric acid and blood urea nitrogen levels are occasionally increased.
Others:
- Flushing and sweating have been reported with levodopa.
- Urine passed during treatment may be altered in colour; usually red-tinged, this will turn dark on standing. These changes are due to metabolites and are no cause for concern.
Tolerance to Madopar varies widely between patients and is often related to the rate of dosage increases. With long-term administration, fluctuations in the therapeutic response may be encountered. They include “freezing” episodes, end-of-dose deterioration and the so-called “on-off” effect. Patients may be helped by dosage reduction or by giving smaller and more frequent doses.
4.9 Overdose
Symptoms and signs
Symptoms and signs of overdosage are qualitatively similar to the side-effects of Madopar in therapeutic doses but may be of greater severity.
Overdose may lead to cardiovascular side effects (e.g. cardiac arrhythmias), psychiatric disturbances (e.g. confusion and insomnia), gastro-intestinal effects (e.g. nausea and vomiting) and abnormal involuntary movements (see section 4.8)
Treatment
Monitor the patient's vital signs and institute supportive measures as indicated by the patient's clinical state. In particular patients may require symptomatic treatment for cardiovascular effects (e.g. antiarrhythmics) or central nervous system effects (e.g. respiratory stimulants, neuroleptics).
5. Pharmacological Properties
5.1 Pharmacodynamic Properties
Madopar is an anti-Parkinsonian agent. Levodopa is the metabolic precursor of dopamine. The latter is severely depleted in the striatum, pallidum and substantia nigra of Parkinsonian patients and it is considered that administration of levodopa raises the level of available dopamine in these centres. However, conversion of levodopa into dopamine by the enzyme dopa decarboxylase also takes place in extracerebral tissues. As a consequence the full therapeutic effect may not be obtained and side-effects occur.
Administration of a peripheral decarboxylase inhibitor, which blocks the extracerebral decarboxylation of levodopa, in conjunction with levodopa has significant advantages; these include reduced gastro-intestinal side-effects, a more rapid response at the initiation of therapy and a simpler dosage regimen. Madopar is a combination of levodopa and benserazide in the ratio 4:1 which in clinical trials has been shown to be the most satisfactory.
Like every replacement therapy, chronic treatment with Madopar will be necessary.
5.2 Pharmacokinetic Properties
Absorption
Low levels of endogenous levodopa are detectable in pre-dose blood samples. After oral administration of Madopar, levodopa and benserazide are rapidly absorbed, mainly in the upper regions of the small intestine and absorption there is independent of the site. Interaction studies indicate that a higher proportion of levodopa is absorbed when administered in combination with benserazide, compared with levodopa administered alone. Maximum plasma concentrations of levodopa are reached approximately one hour after ingestion of Madopar. The absolute bioavailability of levodopa from standard Madopar is approximately 98%.
The maximum plasma concentration of levodopa and the extent of absorption (AUC) increase proportionally with dose (50 – 200mg levodopa). The peak levodopa plasma concentration is 30% lower and occurs later when Madopar is administered after a standard meal. Food intake generally reduces the extent of levodopa absorption by 15% but this can be variable.
Distribution
Levodopa crosses the blood-brain barrier by a saturable transport system. It is not bound to plasma proteins. Benserazide does not cross the blood-brain barrier at therapeutic doses. Benserazide is concentrated mainly in the kidneys, lungs, small intestine and liver.
Metabolism
The 2 major routes of metabolism of levodopa are decarboxylation to form dopamine, which in turn is converted to a minor degree to norepinephrine and to a greater extent, to inactive metabolites, and O-methylation, forming 3-O-methyldopa, which has an elimination half-life of approximately 15 hours and accumulates in patients receiving therapeutic doses of Madopar. Decreased peripheral decarboxylation of levodopa when it is administered with benserazide is reflected in higher plasma levels of levodopa and 3-O-methyldopa.
Benserazide is hydroxylated to trihydroxybenzylhydrazine in the intestinal mucosa and the liver. This metabolite is a potent inhibitor of the aromatic amino acid decarboxylase.
Elimination
In the presence of the peripheral decarboxylase inhibitor, benserazide, the elimination half-life of levodopa is approximately 1.5 hours. In elderly patients the elimination half-life is slightly (25%) longer. Clearance of levodopa is 430ml/min.
Benserazide is almost entirely eliminated by metabolism. The metabolites are mainly excreted in the urine (64%) and to a small extent in faeces (24%).
5.3 Preclinical Safety Data
See section 4.6 Pregnancy and lactation.
6. Pharmaceutical Particulars
6.1 List Of Excipients
Capsule contents:
Microcrystalline cellulose (E460)
Povidone (E1201)
Talc (E553b)
Magnesium stearate (E572)
Mannitol (E421)
Capsule shell:
Gelatin
Indigo carmine (E132)
Titanium dioxide (E171)
Iron oxide (E172)
Printing Ink:
Black iron oxide (E172)
6.2 Incompatibilities
None known
6.3 Shelf Life
3 years.
6.4 Special Precautions For Storage
Do not store above 25°C. Store in the original package. Keep bottle tightly closed.
6.5 Nature And Contents Of Container
Madopar 50 mg/12.5 mg and Madopar 100 mg/25 mg: Amber glass bottles with HDPE cap and integral desiccant containing 100 capsules.
Madopar 200 mg/50 mg: Amber glass bottles with polyethylene closure with integrated desiccant containing 100 capsules.
6.6 Special Precautions For Disposal And Other Handling
No special requirements.
7. Marketing Authorisation Holder
Roche Products Limited, 6 Falcon Way, Shire Park, Welwyn Garden City, AL7 1TW, United Kingdom.
8. Marketing Authorisation Number(S)
Madopar 50 mg/12.5 mg: PL 00031/0125
Madopar 100 mg/25 mg: PL 00031/0073R
Madopar 200 mg/50 mg: PL 00031/0074
9. Date Of First Authorisation/Renewal Of The Authorisation
Madopar 50 mg/12.5 mg: Date of last renewal: 14 July 2002
Madopar 100 mg/25 mg: Date of last renewal: 5 July 2003
Madopar 200 mg/50 mg: Date of last renewal: 6 July 2003
10. Date Of Revision Of The Text
April 2009
Madopar is a registered trade mark
