DEANXIT Film-coated tablet Ref.[28299] Active ingredients: Flupentixol Melitracen

Source: Υπουργείο Υγείας (CY)  Publisher: Lundbeck Hellas A.E., Spyrou Kyprianou, 20 CHAPO CENTRAL, 3rd floor P.C 1075, Nicosia, Cyprus

5.1. Pharmacodynamic properties

Pharmacotherapeutic group: Antidepressants – Tricyclic antidepressant (melitracen) and neuroleptic of the thioxanthene group (flupentixol)
ATC-code: N06CA02

Deanxit consists of two well known and well proven compounds:

Flupentixol is a neuroleptic of the thioxanthene group with anxiolytic and antidepressant properties when given in small doses.

Melitracen is a tricyclic antidepressant with activating properties in low doses. It has similar pharmacological properties as amitriptyline but is less sedative.

In combination the compounds render a preparation with antidepressant, anxiolytic and activating properties.

5.2. Pharmacokinetic properties

Flupentixol

Flupentixol is a mixture of two geometric isomers, the active cis(Z)-flupentixol and trans(E)-flupentixol, approximately in the ratio of 1:1.

Absorption

Oral administration results in maximum serum levels in about 12 hours. Oral bioavailability is about 40%.

Distribution

The apparent volume of distribution (Vd)β is about 14.1 l/kg.

The plasma protein binding is about 99%.

Biotransformation

The metabolism of flupentixol proceeds along three main routes – sulphoxidation, side chain N-dealkylation and glucuronic acid conjugation. The metabolites are devoid of psychopharmacological activity. Flupentixol dominates over metabolites in brain and other tissues.

Elimination

The elimination half-life (T½β) is about 61 hours and the mean systemic clearance (Cls) is about 0.29 l/min.

Flupentixol is excreted mainly with faeces, but also to some degree with the urine. When tritium labelled flupentixol was administered to man the excretion pattern shows the excretion via faeces to be about 4 times the urinary excretion.

In nursing mothers flupentixol is excreted in small amounts with the breast milk. The ratio milk conc./serum conc. in women is on an average 1.3.

Linearity

The kinetics is linear. Steady state plasma levels are achieved in about 7 days. The mean minimum steady state level corresponding to 5 mg flupentixol orally once-a-day was about 1.7 ng/ml (3.9 nmol/l).

Older people

Pharmacokinetic investigations have not been done in elderly patients. However, for the related thioxanthene drug, zuclopenthixol, the pharmacokinetic parameters are widely independent of the age of the patient.

Reduced hepatic function

No data available.

Reduced renal function

Based on the above characteristics for elimination it is reasonable to assume that reduced kidney function is likely not to have much influence on the serum levels of parent drug.

Melitracen

Absorption

Oral administration results in maximum serum levels in about 5 hours. Oral bioavailability is not known.

Distribution

The apparent volume of distribution (Vd)β is not known. The plasma protein binding in rats is about 89%.

Biotransformation

The metabolism of melitracen proceeds mainly by demethylation and hydroxylation. The main active metabolite is the secondary amine, litracen.

Elimination

The elimination half-life (T½β) is about 62 hours in man. The systemic clearance (Cls) is not known.

In rats melitracen is excreted mainly with faeces, but also to some degree with the urine. The excretion pattern showed the excretion via faeces to be about 2½ times the urinary excretion.

It is not known whether melitracen is excreted with breast milk.

Older people

No data available.

Reduced hepatic function

No data available.

Reduced renal function

No data available.

5.3. Preclinical safety data

Acute toxicity

Flupentixol has low acute toxicity, but the acute toxicity of tricyclic antidepressants including melitracen is high.

Chronic toxicity

In chronic toxicity studies there were no findings of concern for the therapeutic use of flupentixol or melitracen.

Reproduction toxicity

In preclinical fertility studies in rats, where flupentixol and melitracen were administered separately slight effects on fertility were noted. Flupentixol slightly affected the pregnancy rate of female rats, whereas melitracen slightly repressed fertility and fecundity of male rats. Effects were seen at doses well in excess of those applied during clinical use.

Combination of flupentixol and melitracen did not induce major malformations or affect pregnancy and embryofoetal development in rats or rabbits. In mice melitracen was associated with lower foetal body weight, but no major malformations were noted.

No effect on parturition or postnatal development of melitracen was noted in mice or rats.

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