Treatment of major depression.

Adults

Escitalopram is administered as a single oral dose and may be taken with or without food.

 

Major Depression

The recommended dose is 10 mg (one 10 mg tablet) once daily. Depending on individual patient response, the dose may be increased to a maximum of 20 mg (one 20 mg tablet) daily.

 

Usually 2-4 weeks are necessary for antidepressant response, although the onset of therapeutic effect may be seen earlier. The treatment of a single episode of depression requires treatment over the acute and the medium term. After the symptoms resolve during acute treatment, a period of consolidation of the response is required. Therefore, treatment of a depressive episode should be continued for a minimum of 6 months.

 

Elderly Patients (> 65 years of age)

A longer half-life and a decreased clearance have been demonstrated in the elderly. 10 mg (one 10 mg tablet) is the recommended maximum maintenance dose in the elderly (see PHARMACOLOGY, Pharmacokinetics and PRECAUTIONS).

 

Children and Adolescents (< 18 years of age)

Safety and efficacy have not been established in this population. Escitalopram should not be used in children and adolescents under 18 years of age (see PRECAUTIONS).

 

Reduced Hepatic Function

An initial dose of 5 mg (half a 10 mg tablet) daily for the first two weeks of treatment is recommended. Depending on individual patient response, the dose may be increased to 10 mg (one 10 mg tablet) (see PRECAUTIONS).

 

Reduced Renal Function

Dosage adjustment is not necessary in patients with mild or moderate renal impairment. No information is available on the treatment of patients with severely reduced renal function (creatinine clearance < 20 mL/min) (see PRECAUTIONS).

 

Poor Metabolisers of CYP2C19

For patients who are known to be poor metabolisers with respect to CYP2C19, an initial dose of 5 mg (half a 10 mg tablet) daily during the first two weeks of treatment is recommended. Depending on individual patient response, the dose may be increased to 10 mg (one 10 mg tablet) (see PHARMACOLOGY, Pharmacokinetics and PRECAUTIONS, Interactions with Other Medicines).

 

Discontinuation

Significant numbers of discontinuation symptoms may occur with abrupt discontinuation of escitalopram. To minimise discontinuation reactions, tapered discontinuation over a period of at least one to two weeks is recommended. If unacceptable discontinuation symptoms occur following a decrease in the dose or upon discontinuation of treatment, then resuming the previously prescribed dose may be considered. Subsequently, the dose may be decreased but at a more gradual rate.

 

Hypersensitivity to citalopram, escitalopram and any excipients in the Escitalopram tablets (see PRESENTATIONS AND STORAGE CONDITIONS). Monoamine Oxidase Inhibitors Escitalopram should not be used in combination with monoamine oxidase inhibitors (MAOI) or the reversible MAOI (RIMA), moclobemide, or within 14 days of discontinuing treatment with a MAOI, and at least one day after discontinuing treatment with the reversible MAOI (RIMA), moclobemide. Similarly, at least 14 days should be allowed after stopping escitalopram before starting a MAOI or RIMA. Cases of serious reactions, such as potentially life-threatening serotonin syndrome (characterised by neuromuscular excitation, altered mental status and autonomic dysfunction) have been reported in patients receiving an SSRI in combination with a monoamine oxidase inhibitor (MAOI) or the reversible MAOI (RIMA), moclobemide, and in patients who have recently discontinued an SSRI and have been started on a MAOI (see PRECAUTIONS, Interactions with Other Medicines). Pimozide Concomitant use in patients taking pimozide is contraindicated (see PRECAUTIONS, Interactions with Other Medicines).

Clinical Worsening and Suicide Risk

The risk of suicide attempt is inherent in depression and may persist until significant remission occurs. This risk must be considered in all depressed patients.

 

Patients with depression may experience worsening of their depressive symptoms and/or the emergence of suicidal ideation and behaviours (suicidality) whether or not they are taking antidepressant medications, and this risk may persist until significant remission occurs. As improvement may not occur during the first few weeks or more of treatment, patients should be closely monitored for clinical worsening and suicidality, especially at the beginning of a course of treatment, or at the time of dose changes, either increases or decreases. Consideration should be given to changing the therapeutic regimen, including possibly discontinuing the medication, in patients whose depression is persistently worse or whose emergent suicidality is severe, abrupt in onset, or was not part of the patient’s presenting symptoms.

 

Patients (and caregivers of patients) should be alerted about the need to monitor for any worsening of their condition and/or the emergence of suicidal ideation/behaviour or thoughts of harming themselves and to seek medical advice immediately if these symptoms are present.

 

Patients with co-morbid depression associated with other psychiatric disorders being treated with antidepressants should be similarly observed for clinical worsening and suicidality.

 

Patients with a history of suicide-related events, or those exhibiting a significant degree of suicidal ideation prior to commencement of treatment, are at greater risk of suicidal thoughts or suicide attempts, and should receive careful monitoring during treatment.

 

Pooled analyses of 24 short-term (4 to 16-week), placebo-controlled trials of nine antidepressant medicines (SSRIs and others) in 4,400 children and adolescents with major depressive disorder (16 trials), obsessive-compulsive disorder (4 trials), or other psychiatric disorders (4 trials) have revealed a greater risk of adverse events representing suicidal behaviour or thinking (suicidality) during the first few months of treatment in those receiving antidepressants. The average risk of such events in patients treated with an antidepressant was 4%, compared with 2% of patients given placebo. There was considerable variation in risk among the antidepressants, but there was  a tendency towards an increase for almost all antidepressants studied. The risk of suicidality was most consistently observed in the major depressive disorder trials, but there were signals of risk arising from trials in other psychiatric indications (obsessive-compulsive disorder and social anxiety disorder) as well. No suicides occurred in these trials. It is unknown whether the suicidality risk in children and adolescent patients extends to use beyond several months. The nine antidepressant medicines in the pooled analyses included five SSRIs (citalopram, fluoxetine, fluvoxamine, paroxetine, sertraline) and four non-SSRIs (buproprion, mirtazapine, nefazodone, venlafaxine).

 

Pooled analyses of short-term studies of antidepressant medications have also shown an increased risk of suicidal thinking and behaviour, known as suicidality, in young adults aged 18 to 24 years during initial treatment (generally the first one to two months). Short-term studies did not show an increase in the risk of suicidality with antidepressants compared to placebo in adults beyond the age of 24 years, and there was a reduction with antidepressants compared to placebo in adults aged 65 years and older.

 

Symptoms of anxiety, agitation, panic attacks, insomnia, irritability, hostility (aggressiveness), impulsivity, akathisia (psychomotor restlessness), hypomania, and mania, have been reported in adults, adolescents and children being treated with antidepressants for major depressive disorder as well as for other indications, both psychiatric and non-psychiatric. Although a causal link between the emergence of such symptoms and either worsening of depression and/or emergence of suicidal impulses has not been established, there is concern that such symptoms may be precursors of emerging suicidality.

 

Families or caregivers of children and adolescents being treated with antidepressants for major depressive disorder or for any other condition (psychiatric or non-psychiatric) should be informed about the need to monitor these patients for the emergence of agitation, irritability, unusual changes in behaviour, and other symptoms described above, as well as the emergence of suicidality, and to report such symptoms to health care providers immediately. It is particularly important that monitoring be undertaken during the initial few months of antidepressant treatment or at times of dose increase or decrease.

 

Prescriptions for escitalopram should be written for the smallest quantity of tablets consistent with good patient management, in order to reduce the risk of overdose.

 

Akathisia / Psychomotor Restlessness

The use of SSRIs/SNRIs has been associated with the development of akathisia, characterised by a subjectively unpleasant or distressing restlessness and need to move often accompanied by an inability to sit or stand still. This is most likely to occur within the first few weeks of treatment. In patients who develop these symptoms, increasing the dose may be detrimental.

 

Haemorrhage

Bleeding abnormalities of the skin and mucous membranes have been reported with the use of SSRIs (including purpura, haematoma, epistaxis, vaginal bleeding and gastrointestinal bleeding). Escitalopram should therefore be used with caution in patients concomitantly treated with oral anticoagulants, medicinal products known to affect platelet function (e.g. atypical antipsychotics and phenothiazines, most tricyclic antidepressants, acetylsalicylic acid and non-steroidal anti-inflammatory medicinal products (NSAIDs), ticlopidine and dipyridamole) as well as in patients with a past history of abnormal bleeding or those with predisposing conditions. Pharmacological gastroprotection should be considered for high risk patients.

 

Hyponatraemia

Probably due to inappropriate antidiuretic hormone secretion (SIADH), hyponatraemia has been reported as a rare adverse reaction with the use of SSRIs. Especially elderly patients seem to be a risk group.

 

Seizures

The drug should be discontinued in any patient who develops seizures. SSRIs should be avoided in patients with unstable epilepsy and patients with controlled epilepsy should be carefully monitored. SSRIs should be discontinued if there is an increase in seizure frequency (see PRECAUTIONS, Pre-Clinical Safety).

 

Diabetes

In patients  with diabetes, treatment with an SSRI may alter glycaemic control, possibly due to improvement of depressive symptoms. Insulin and/or oral hypoglycaemic dosage may need to be adjusted.

 

Mania

SSRIs should be used with caution in patients with a history of mania/hypomania. SSRIs should be discontinued in any patient entering a manic phase.

 

ECT (Electoconvulsive Therapy)

There is limited published clinical experience of concurrent administration of SSRIs and ECT, therefore caution is advisable.

 

Effect on Ability to Drive and Use Machines

Escitalopram does not impair intellectual function and psychomotor performance. However, as with other psychoactive drugs, patients should be cautioned about their ability to drive a car and operate machinery.

 

Discontinuation

Discontinuation symptoms when stopping treatment are common, particularly if discontinuation is abrupt.

 

The risk of discontinuation symptoms may be dependent on several factors including the duration and dose of therapy and the rate of dose reduction. Dizziness, sensory disturbances (including paraesthesia and electric shock sensations), sleep disturbances (including insomnia and intense dreams), agitation or anxiety, nausea and/or vomiting, tremor, confusion, sweating, headache, diarrhoea, palpitations, emotional instability, irritability, and visual disturbances are the most commonly reported reactions. Generally these symptoms are mild to moderate, however, in some patients they may be severe in intensity.

 

They usually occur within the first few days of discontinuing treatment, but there have been very rare reports of such symptoms in patients who have inadvertently missed a dose.

 

Generally these symptoms are self-limiting and usually resolve within 2 weeks, though in some individuals they may be prolonged (2-3 months or more). It is therefore advised that escitalopram should be gradually tapered when discontinuing treatment over a period of several weeks or months, according to the patient’s needs (see DOSAGE AND ADMINISTRATION).

 

Cardiac Disease

Escitalopram has not been evaluated or used to any appreciable extent in patients with a recent history of myocardial infarction or unstable heart disease. Like other SSRIs, escitalopram causes a small decrease in heart rate. Consequently, caution should be observed when escitalopram is initiated in patients with pre-existing slow heart rate.

 

Impaired Hepatic Function

In subjects with hepatic impairment, clearance of escitalopram was decreased and plasma concentrations were increased. The dose of escitalopram in hepatically impaired patients should therefore be reduced (see PHARMACOLOGY, Pharmocokinetics and DOSAGE AND ADMINISTRATION).

 

Impaired Renal Function

Escitalopram is extensively metabolised and excretion of unchanged drug in urine is a minor route of elimination. At present no information is available for the treatment of patients with severely reduced renal function (creatinine clearance < 20 mL/min) and escitalopram should be used with caution in such patients (see DOSAGE AND ADMINISTRATION).

 

Pre-Clinical Safety

High doses of escitalopram, which resulted in plasma Cmax for escitalopram and metabolites at least 8-fold greater than anticipated clinically, have been associated with convulsions, ECG abnomalities and cardiovascular changes in experimental animals. Of the cardiovascular changes, cardiotoxicity (including congestive heart failure) was observed in comparative toxicological studies in rats following oral escitalopram or citalopram administration for 4 to 13 weeks and appears to correlate with peak plasma concentrations although its exact mechanism is not clear. Clinical experiences with citalopram, and the clinical trial experience with escitalopram, do not indicate that these findings have a clinical correlation

 

Paediatric Use (Children and Adolescents < 18 years)

The efficacy and safety of escitalopram has not been established in children and adolescents less than 18 years of age. Consequently, escitalopram should not be used in children and adolescents less than 18 years of age.

 

Use in the Elderly (> 65 years)

Escitalopram AUC and half-life were increased in subjects ≥ 65 years of age compared to younger subjects in a single-dose and a multiple-dose pharmacokinetic study. The dose of escitalopram in elderly patients should therefore be reduced (see DOSAGE AND ADMINISTRATION).

 

Carcinogenicity

No carcinogenicity studies were performed with escitalopram. However, other non-clinical studies suggest that the effects of escitalopram  can be directly predicted from  those of the citalopram racemate.

 

Citalopram did not show any carcinogenic activity in long-term oral studies using mice and rats at doses up to 240 and 80 mg/kg/day, respectively.

 

Genotoxicity

No genotoxicity studies were performed with escitalopram. However, other non-clinical studies suggest that the effects of escitalopram  can be directly predicted from  those of the citalopram racemate.

 

In assays of genotoxic activity, citalopram showed no evidence of mutagenic or clastogenic activity.

MAOIs

Co-administration with MAO inhibitors may cause serotonin syndrome (see CONTRAINDICATIONS).

 

Serotonin syndrome

Development of serotonin syndrome may occur in association with treatment with SSRIs and SNRIs, particularly when given in combination with MAOIs or other serotonergic agents. Symptoms and signs of serotonin syndrome include rapid onset of neuromuscular excitation (Hyperreflexia, incoordination, myoclonus, tremor), altered mental status (confusion, agitation, hypomania) and autonomic dysfunction (diaphoresis, diarrhoea, fever, shivering and rapidly fluctuating vital signs). Treatment with escitalopram should be discontinued if such events occur and supportive symptomatic treatment initiated.

 

Pimozide

Co-administration of a single dose of pimozide 2 mg to subjects treated with racemic citalopram 40 mg/day for 11 days caused an increase in AUC and Cmax of pimozide, although not consistently throughout the study. The co-administration of pimozide and citalopram resulted in a mean increase in the QTc interval of approximately 10 msec. Due to the interaction with citalopram noted at a low dose of pimozide, concomitant administration of escitalopram and pimozide is contraindicated (see CONTRAINDICATIONS).

 

Serotonergic Drugs

Co-administration with serotonergic drugs (e.g. tramadol, sumatriptan) may lead to an enhancement of serotonergic effects. Similarly, Hypericum perforatum (St John’s Wort) should be avoided as adverse interactions have been reported with a range of drugs including antidepressants.

 

Lithium and Tryptophan

There have been reports of enhanced effects when SSRIs have been given with lithium or tryptophan and therefore concomitant use of SSRIs with these drugs should be undertaken with caution.

 

Medicines Affecting the Central Nervous System

Given the primary CNS effects of escitalopram, caution should be used when it is taken in combination with other centrally acting drugs.

 

Medicines Lowering the Seizure Threshold

SSRIs can lower the seizure threshold. Caution is advised when concomitantly using other medicinal products capable of lowering the seizure threshold [e.g. antidepressants (tricyclics, SSRIs), neuroleptics (phenothiazines, thioxanthenes, butyrophenones), mefloquine, bupropion and tramadol].

 

Hepatic Enzymes

Escitalopram has a low potential for clinically significant drug interactions. In vitro studies have shown that the biotransformation of escitalopram to its demethylated metabolites depends on three parallel pathways (cytochrome P450 (CYP) 2C19, 3A4 and 2D6). Escitalopram is a very weak inhibitor of isoenzyme CYP1A2, 2C9, 2C19, 2E1, and 3A4, and a weak inhibitor of 2D6.

 

Effects of Other Drugs on Escitalopram in vivo

The pharmacokinetics of escitalopram was not changed by co-administration with ritonavir (CYP3A4 inhibitor). Furthermore, co-administration with ketoconazole (potent CYP3A4 inhibitor) did not change the pharmacokinetics or racemic citalopram.

 

Co-administration of escitalopram with omeprazole (a CYP2C19 inhibitor) resulted in a moderate (approximately 50%) increase in plasma concentrations of escitalopram and a small but statistically significant increase (31%) in the terminal half-life of escitalopram (see also DOSAGE AND ADMINISTRATION, Poor Metabolisers of CYP2C19).

 

Co-administration of escitalopram with cimetidine (moderately potent general enzyme inhibitor) resulted in a moderate (approximately 70%) increase in the plasma concentrations of escitalopram.

 

Thus, caution should be exercised at the upper end of the dose range of escitalopram when used concomitantly with CYP2C19 inhibitors (e.g. omeprazole, esomeprazole, fluoxetine, fluvoxamine, lansoprazole, and ticlopidine) or cimetidine. A reduction in the dose of escitalopram may be necessary based on clinical judgement (see also DOSAGE AND ADMINISTRATION, Poor Metabolisers of CYP2C19).

 

Effects of Escitalopram on Other Drugs in vivo

Escitalopram is an inhibitor of the enzyme CYP2D6. Caution is recommended when escitalopram is co-administered with medicinal products that are mainly metabolised by this enzyme, and that have a narrow therapeutic index, e.g. flecainide, propafenone and metoprolol (when used in cardiac failure), or some CNS acting medicinal products that are mainly metabolised by CYP2D6, e.g. antidepressants such as desipramine, clomipramine and nortritypline or antipsychotics like risperidone, thioridazine and haloperidol. Dosage adjustment may be warranted.

 

Co-administration with desipramine (a CYP2D6 substrate) resulted in a two-fold increase in plasma levels of desipramine. Therefore, caution is advised when escitalopram and desipramine are co-administered. A similar increase in plasma levels of desipramine, after administration of imipramine, was seen when given together with racemic citalopram.

 

Co-administration with metoprolol (a CYP2D6 substrate) resulted in a two-fold increase in plasma levels of metoprolol. However, the combination had no clinically significant effects on blood pressure and heart rate.

 

The pharmacokinetics of ritonavir (CYP3A4 inhibitor) was not changed by co-administration with escitalopram.

 

Furthermore, pharmacokinetic interaction studies with racemic citalopram have demonstrated no clinically important interactions with carbamazepine (CYP3A4 substrate), triazolam  (CY3A4 substrate),   theophylline   (CYP1A2   substrate),   warfarin   (CYP3A4   and   CYP2C9   substrate), levomepromazine (CYP2D6 inhibitor), lithium and digoxin.

 

Medicines that Interfere with Haemostasis (NSAIDs, Aspirin, Warfarin, etc)

Serotonin release by platelets  plays an important role in haemostasis. There is  an association between use of psychotropic drugs that interfere with serotonin reuptake and the occurrence of abnormal bleeding. Concurrent use of an NSAID, aspirin or warfarin potentiates this risk. Thus, patients should be cautioned about using such medicines concurrently with escitalopram.

 

Alcohol

The combination of SSRIs and alcohol is not advisable.

Effects on Fertility

No fertility studies were performed with escitalopram. However, other non-clinical studies suggest that the effects of escitalopram can be directly predicted from those of citalopram racemate.

 

In rats, female fertility was unaffected by oral treatment with citalopram doses which achieved plasma drug concentration slightly in excess of those expected in humans, but effects on male rat fertility have not been tested with adequate oral doses.

 

Use in Pregnancy (Category C)

Limited clinical data are available regarding exposure to escitalopram during pregnancy.

 

Neonates should be observed if maternal use of escitalopram continues into the later stages of pregnancy, particularly in the third trimester. If escitalopram is used until or shortly before birth, discontinuation effects in the newborn are possible. Abrupt discontinuation should be avoided during pregnancy.

 

Neonates exposed to escitalopram, other SSRIs (Selective Serotonin Reuptake Inhibitors), or SNRIs (Serotonin Norepinephrine Reuptake Inhibitors), late in the third trimester have developed complications requiring prolonged hospitalisation, respiratory support, and tube feeding. Such complications can arise immediately upon delivery. Reported clinical findings have included respiratory distress, cyanosis, apnoea, seizures, temperature instability, feeding difficulty, vomiting, hypoglycaemia, hypotonia, hypertonia, hyperreflexia, tremor, jitteriness, irritability, lethargy, constant crying, somnolence and difficulty sleeping. These features are consistent with either a direct toxic effect of SSRIs and SNRIs or, possibly, a drug discontinuation syndrome. In the majority of cases, the complications begin immediately or soon (< 24 hours) after delivery.

 

Epidemiological data have shown that the use  of SSRIS  in pregnancy, particularly use in late pregnancy, was associated with an increased risk of persistent pulmonary  hypertension of the newborn (PPHN). The risk of PPHN among infants born to women who used SSRIs late in pregnancy was estimated to be 4 to 5 times higher than the rate of 1 to 2 per 1000 pregnancies observed in the general population.

 

Oral treatment of rats with escitalopram during organogenesis at maternotoxic doses led to increased post-implantation loss and reduced foetal weight at systemic exposure levels (based on AUC) ca. 11-fold that anticipated clinically, with no effects seen at 6-fold. No teratogenicity was evident in this study at relative systemic exposure levels of ca. 15 (based on AUC).

 

There were no peri/postnatal effects of escitalopram following oral dosing of pregnant rats (conception through to weaning) at systemic exposure levels (based on AUC) ca. 2-fold than anticipated clinically. However, the number of stillbirths was increased and the size, weight and postnatal survival of offspring were decreased at a relative systemic exposure level ca. 5.

 

Because animal reproduction studies are not always predictive of human response, this drug should be used during pregnancy only if clearly needed and only after careful consideration of the risk/benefit.

 

Australian Categorisation Definition of Category C: Drugs, which owing to their pharmacological effects, have caused or may be suspected of causing, harmful effects on the human foetus or neonate without causing malformations. These effects may be reversible. Accompanying texts should be consulted for further details.

 

Use in Lactation

It is expected that escitalopram, like citalopram, will be excreted into human breast milk. Studies in nursing mothers have shown that the mean combined dose of citalopram and demethylcitalopram transmitted to infants via breast milk (expressed as a percentage of the weight-adjusted maternal dose) is 4.4 – 5.1% (below the notional 10% level of concern).

 

Plasma concentrations of these drugs in infants were very low or absent and there were no adverse effects. Whilst the citalopram data support the safety of use of escitalopram in breast-feeding women, the decision to breast-feed should always be made as an individual risk/benefit analysis.

Escitalopram does not impair intellectual function and psychomotor performance. However, as with other psychoactive drugs, patients should be cautioned about their ability to drive a car and operate machinery.

Adverse reactions observed with escitalopram are in general mild and transient. They are most frequent during the first one or  two weeks of treatment and usually decrease in intensity and frequency with continued treatment and generally do not lead to a cessation of therapy. Data from short-term placebo-controlled studies are presented below. The safety data from the long-term studies showed a similar profile.

 

Treatment-Emergent Adverse Events with an Incidence of ≥ 1% in Placebo-Controlled Trials

Figures marked with * in below table indicate adverse reactions where incidence with escitalopram is statistically significantly different from placebo (p < 0.05).

 

SYSTEM ORGAN CLASS AND PREFERRED TERM	PLACEBO		ESCITALOPRAM
	n	(%)	n	(%)
Patients Treated	1795		2632
Patients with Treatment Emergent Adverse Event	1135	(63.2)	1891	(71.8)
GASTROINTESTINAL SYSTEM DISORDERS
Nausea	151	(8.4)	481	(18.3)*
Diarrhoea	91	(5.1)	207	(7.9)*
Mouth Dry	74	(4.1)	152	(5.8)*
Constipation	42	(2.3)	71	(2.7)
Abdominal Pain	47	(2.6)	68	(2.6)
Vomiting	29	(1.6)	54	(2.1)
Dyspepsia	30	(1.7)	33	(1.3)
Flatulence	15	(0.8)	31	(1.2)

* = Statistically significant difference escitalopram vs. placebo (p < 0.05).

[gs] = gender specific

 

 

SYSTEM ORGAN CLASS AND PREFERRED TERM	PLACEBO		ESCITALOPRAM
	n	(%)	n	(%)
CENTRAL AND PERIPHERAL NERVOUS SYSTEM DISORDERS
Headache	305	(17.0)	506	(19.2)
Dizziness	64	(6.3)	147	(5.6)*
Paraesthesia	13	(0.7)	35	(1.3)
Migraine	17	(0.9)	23	(0.8)
Tremor	15	(0.8)	33	(1.3)
PSYCHIATRIC DISORDERS
Insomnia	82	(4.6)	245	(9.3)*
Somnolence	62	(3.5)	217	(8.2)*
Anorexia	12	(0.7)	56	(2.1)*
Libido decreased	21	(1.2)	102	(3.9)*
Anxiety	44	(2.5)	77	(2.9)
Appetite decreased	8	(0.5)	35	(1.3)*
Agitation	6	(0.3)	33	(1.3)*
Nervousness	13	(0.7)	25	(1.0)
Dreaming Abnormal	18	(1.0)	41	(1.6)
Impotence [gs]	4	(0.6)	22	(2.2)*
RESPIRATORY SYSTEM DISORDERS
Upper Respiratory Tract Infection	91	(5.1)	96	(3.6)
Coughing	18	(1.1)	24	(0.9)
Rhinitis	81	(4.8)	146	(5.5)
Sinusitis	24	(1.3)	46	(1.7)
Pharyngitis	44	(2.5)	57	(2.2)
Yawning	3	(0.2)	58	(2.2)*
Bronchitis	31	(1.7)*	26	(0.9)
BODY AS A WHOLE – GENERAL DISORDERS
Influenza-like Symptoms	65	(3.6)	87	(3.3)
Fatigue	62	(3.5)	230	(8.7)*
Back Pain	61	(3.4)	74	(2.8)
SKIN AND APPENDAGES DISORDERS
Sweating increased	27	(1.5)	145	(5.5)*
MUSCULOSKELETAL SYSTEM DISORDERS
Arthralgia	22	(1.2)	27	(1.0)
REPRODUCTIVE DISORDERS, FEMALE
Anorgasmia [gs]	3	(0.3)	47	(2.9)
METABOLIC AND NUTRITIONAL DISORDERS
Weight increase	20	(1.1)	45	(1.7)
REPRODUCTIVE DISORDERS, MALE
Ejaculation disorder [gs]	3	(0.5)	48	(4.7)*
Ejaculation failure [gs]	1	(0.2)	27	(2.7)*
CARDIOVASCULAR DISORDERS
Hypertension	24	(1.3)*	13	(0.5)
HEART RATE AND RHYTHM DISORDERS
Palpitations	15	(0.8)	30	(1.1)
Inflicted injury (unintended injury)	22	(1.2)	23	(0.8)

* = Statistically significant difference escitalopram vs. placebo (p < 0.05).

[gs] = gender specific

Adverse Events in Relation to Dose

The potential dose dependency of common adverse events (defined as an incidence rate of ≥ 5% in either the 10 mg or 20 mg escitalopram groups) was examined on the basis of the combined incidence of adverse events in two fixed dose trials. The overall incidence rates of adverse events in 10 mg escitalopram treated patients (66%) was similar to that of the placebo treated patients (61%), while the incidence rate in 20 mg/day escitaloram treated patients was greater (86%). Common adverse events that occurred in the 20 mg/day escitalopram group with an incidence approximately twice that of the 10 mg/day escitalopram group and approximately twice that of the placebo group are shown below.

Incidence of common adverse events* in patients with major depression receiving placebo, 10 mg/day escitalopram, or 20 mg/day escitalopram

 

ADVERSE EVENT                                     PLACEBO         10 mg/day Escitalopram          20 mg/day Escitalopram

                                                                    (n=311)                       (n=310)                                         (n = 125)

Insomnia                                                        4%                                       7%                                               14%

Diarrhoea                                                       5%                                       6%                                               14%

Dry mouth                                                      3%                                       4%                                                9%

Somnolence                                                   1%                                       4%                                                9%

Dizziness                                                         2%                                       4%                                                7%

Sweating increased                                    < 1%                                      3%                                                8%

Constipation                                                   1%                                       3%                                                6%

Fatigue                                                            2%                                       2%                                                6%

Indigestion                                                      1%                                       2%                                                6%

*  adverse events with an incidence rate of at least 5% in either escitalopram group and with an incidence rate in 20 mg/day escitalopram group that was approximately twice that of the 10 mg/day escitalopram group and the placebo group.

 

Vital Sign Changes

Escitalopram and placebo groups were compared with respect to (1) mean change from baseline in vital signs (pulse, systolic blood pressure, and diastolic blood pressure) and (2) the incidence of patients meeting criteria for potentially clinically significant changes from baseline in these variables. These analyses did not reveal any clinically important changes in vital signs associated with escitalopram treatment.

 

ECG Changes

Cases of QT prolongation have been reported during the post-marketing period with both c i t al opr am and es c i t al opr am . C i tal opr am  c an  c aus e  dos e - dependent  Q T  interval prolongation. In an ECG study, the observed change from baseline QTC (Fridericia correction) was 7.5 msec at the 20mg/day dose and 16.7 msec at the 60mg/day dose of citalopram. The effect of escitalopram on the QT interval was similarly studied at doses of 10mg/day and 30mg/day. The change from baseline QTc (Fridericia correction) was 4.3 msec at the 10mg/day dose and 10.7 msec with the above recommended dose of 30mg/day. The QTc interval prolongation observed with 60mg citalopram exceeded that observed with  30mg escitalopram. It is probable that the R-enantiomer and  its metabolites in racemic citalopram contribute to these effects.

 

Weight Changes

Patients treated with escitalopram in controlled trials did not differ from placebo-treated patients with regard to clinically important change in body weight.

 

Laboratory Changes

In clinical studies, there were no signals of clinically important changes in either various serum chemistry, haematology, and urinalysis parameters associated with escitalopram treatment compared to placebo or in the incidence of patients meeting the criteria for potentially clinically significant changes from baseline in these variables.

 

For abnormal laboratory changes registered as either uncommon events or serious adverse events from ongoing trials and observed during (but not necessarily caused by) treatment with escitalopram, please refer to “Other Events Observed During the Pre-Marketing Evaluation of Escitalopram”.

 

Other Changes Observed During the Pre-Marketing Evaluation of Escitalopram

Following is a list of WHO terms that reflect adverse events occurring at an incidence of < 1% and serious adverse events from ongoing trials. All reported events are included except those already listed in the table or elsewhere in the ADVERSE EFFECTS section, and those occurring in only one patient. It is important to emphasise that, although the events reported occurred during treatment with escitalopram, they were not necessarily caused by it.

 

Events are further categorised by body system and are listed below. Uncommon adverse events are those occurring in less than 1/100 patients but at least 1/1,000 patients.

 

Application Site Disorders

Uncommon:  otitis externa, cellulitis.

 

Body as a W hole

Uncommon: allergy, aggravated allergy, allergic reactions, asthenia, carpal tunnel syndrome, chest pain, chest tightness, fever, hernia, leg pain, limb pain, neck pain, oedema, oedema of extremities, peripheral oedema, rigors, malaise, syncope, scar.

 

Cardiovascular Disorders, General

Uncommon: hypertension aggravated, hypotension, hypertension, abnormal ECG.

 

Central and Peripheral Nervous System Disorders

Uncommon: ataxia, dysaesthesia, disequilibrium, dysgeusia, dystonia, hyperkinesia, hyperreflexia, hypertonia, hypoaesthesia, leg cramps, lightheadedness, muscle contractions, nerve root lesion, neuralgia, neuropathy, paralysis, sedation, tetany, tics, twitching, vertigo.

 

Gastrointestinal System Disorders

Uncommon: abdominal cramp, abdominal discomfort, belching, bloating, change in bowel habit, colitis, colitis ulcerative, enteritis, epigastric discomfort, gastritis, gastroesophageal reflux, haemorrhoids, heartburn, increased stool frequency, irritable bowel syndrome, melaena, periodontal destruction, rectal haemorrhage, tooth disorder, toothache, ulcerative stomatitis.

 

Hearing and Vestibular Disorders

Uncommon:  deafness, earache, ear disorder, otosalpingitis, tinnitus.

 

Heart Rate and Rhythm Disorders

Uncommon:  bradycardia, tachycardia.

 

Liver and Biliary System Disorders

Uncommon:  bilirubinaemia, hepatic enzymes increased.

 

Metabolic and Nutritional Disorders

Uncommon: abnormal glucose tolerance, diabetes mellitus, gout, hypercholesterolaemia, hyperglycaemia, hyperlipaemia, thirst, weight decrease, xerophthalmia.

 

Musculoskeletal System Disorders

Uncommon: arthritis, arthropathy, arthrosis, bursitis, costochondritis, fascitis plantar, fibromyalgia, ischial neuralgia, jaw stiffness, muscle cramp, muscle spasms, muscle stiffness, muscle tightness, muscle weakness, myalgia, myopathy, osteoporosis, pain neck/shoulder, tendinitis, tenosynovitis.

 

Myo-, Endo- and Pericardial and Valve Disorders

Uncommon: myocardial infarction, myocardial ischaemia, myocarditis, angina pectoris.

 

Neoplasm

Uncommon:  female breast neoplasm, ovarian cyst, uterine fibroid.

 

Platelet, Bleeding and Clotting Disorders

Uncommon:   abnormal  bleeding,  predominantly  of  the  skin  and  mucous  membranes,  including purpura, epistaxis, haematomas, vaginal bleeding and gastrointestinal bleeding.

 

Poison Specific Terms

Uncommon:  sting.

 

Psychiatric Disorders

Uncommon: aggressive reaction, amnesia, apathy, bruxism, carbohydrate craving, concentration impairment, confusion, depersonalisation, depression, depression aggravated, emotional lability, excitability, feeling unreal, forgetfulness, hallucination, hypomania, increased appetite, irritability, jitteriness, lethargy, loss of libido, obsessive-compulsive disorder, panic reaction, paroniria, restlessness aggravated, sleep disorder, snoring, suicide attempt, thinking abnormal.

 

Red Blood Cell Disorders

Uncommon:  anaemia hypochromic, anaemia.

 

Reproductive Disorders / Female

Uncommon: amenorrhoea, atrophic vaginitis, breast pain, genital infection, intermenstrual bleeding, menopausal symptoms, menorrhagia, menstrual cramps, menstrual disorder, premenstrual tension, postmenopausal bleeding, sexual function abnormality, unintended pregnancy, dysmenorrhoea, vaginal haemorrhage, vaginal candidiasis, vaginitis.

 

Reproductive Disorders / Male

Uncommon:  ejaculation delayed, prostatic disorder.

 

Resistance Mechanism Disorders

Uncommon: moniliasis genital, abscess, infection, herpes simplex, herpes zoster, infection bacterial, infection parasitic, infection (tuberculosis), moniliasis.

 

Respiratory System Disorders

Uncommon: asthma, dyspnoea, laryngitis, nasal congestion, nasopharyngitis, pneumonia, respiratory tract infection, shortness of breath, sinus congestion, sinus headache, sleep apnoea, tracheitis, throat tightness.

 

Skin and Appendages Disorders

Uncommon: acne, alopecia, dermatitis, dermatitis fungal, dermatitis lichenoid, dry skin, eczema, erythematous rash, furunculosis, onychomycosis, pruritus, psoriasis aggravated, rash, rash pustular, skin disorder, urticaria, verruca.

 

Secondary Terms

Uncommon: accidental injury, bite, burn, fall, fractured neck of femur, alcohol problem, traumatic haematoma, cyst, food poisoning, lumbar disc lesion, surgical intervention.

 

Special Senses Other, Disorders

Uncommon: dry eyes, eye irritation, taste alteration, taste perversion, visual disturbance,  ear infection NOS, vision blurred.

 

Urinary System Disorders

Uncommon: cystitis, dysuria, facial oedema, micturition frequency, micturition disorder, nocturia, polyuria, pyelonephritis, renal calculus, urinary frequency, urinary incontinence, urinary tract infection.

 

Vascular (Extracardiac) Disorders

Uncommon: cerebrovascular disorder, flushing, hot flush [gs], ocular haemorrhage, peripheral ischaemia, varicose vein, vein disorder, vein distended.

 

Vision Disorders

Uncommon: accommodation abnormal, blepharospasm, eye infection, eye pain, mydriasis, vision abnormal, vision blurred, visual disturbance.

 

White Cell and Reticuloendothelial System Disorders

Uncommon:  leucopenia.

 

In addition, the following adverse reactions have been reported with racemic citalopram (all of which have also been reported for other SSRIs):

 

Disorders of Metabolism and Nutrition:

Hyponatraemia, inappropriate ADH secretion (both especially in elderly women).

 

Neurological Disorders:

Convulsions, convulsions grand mal and extrapyramidal disorder, serotonin syndrome (typically characterised by a rapid onset of changes in mental state, with confusion, mania, agitation, hyperactivity, shivering, fever, tremor, ocular movements, myoclonus, hyperreflexia, and inco- ordination).

 

Skin Disorders:

Ecchymoses, angioedema.

 

Furthermore, a number of adverse reactions have been listed for other SSRIs. Although these are not listed as adverse reactions for escitalopram or citalopram, it cannot be excluded that these adverse reactions may occur with escitalopram. These SSRI class reactions are listed below:

 

Cardiovascular Disorders:              postural hypotension.

Hepatobiliary Disorders:                abnormal liver function tests.

Neurological Disorders:                  movement disorders.

Psychiatric Disorders:                     mania, panic attacks.

Renal and Urinary Disorders:         urinary retention.

Reproductive Disorders:                  galactorrhoea.

 

Other Events Observed During the Post-Marketing Evaluation of Escitalopram

Although no causal relationship to escitalopram treatment has been found, the following adverse events have been reported in association with escitalopram treatment in at least 3 patients (unless otherwise noted) and not described elsewhere in the ADVERSE EFFECTS section:

 

Stomatitis, drug interaction NOS, feeling abnormal, hypersensitivity NOS, non-accidental overdose, injury NOS.

 

In addition, although no causal relationship to racemic citalopram treatment has been found, the following adverse events have been reported to be temporally associated with racemic citalopram treatment subsequent to the marketing of racemic citalopram and were not observed during the pre-marketing evaluation of escitalopram or citalopram: acute renal failure, akathisia, anaphylaxis, choreoathetosis, delirium, dyskinesia, epidermal necrolysis, erythema multiforme, gastrointestinal haemorrhage, haemolytic anaemia, hepatic necrosis, myoclonus, neuroleptic malignant syndrome, nystagmus, pancreatitis, priapism, prolactinaemia, prothrombin decreased, QT prolonged, rhabdomyolysis, spontaneous abortion, thrombocytopenia, thrombosis, Torsades de  pointes, ventricular arrhythmia, and withdrawal syndrome.

 

Class effect

Epidemiological studies, mainly conducted in patients 50 years of age and older, show an increased risk of bone fractures in patients receiving SSRIs and TCAs. The mechanism leading to this risk is unknown.

In general, the main therapy for all overdoses is supportive and symptomatic use.

 

Toxicity

Clinical data on escitalopram overdose are limited and many cases involve concomitant overdoses of other drugs. In the majority of cases, mild or no symptoms have been reported. Doses between 400 and 800 mg of escitalopram alone have been taken without any severe symptoms. No fatalities or sequelae were reported in the few cases with a higher dose (one patient survived ingestion of either 2,400 or 4,800 mg).

 

Symptoms

Symptoms seen in reported overdose of escitalopram include symptoms mainly related to the central nervous system (ranging from dizziness, tremor and agitation to rare cases of convulsion and coma), the gastrointestinal system (nausea/vomiting), the cardiovascular system (hypotension, tachycardia, arrhythmia and ECG changes (including QT prolongation)), and electrolyte/fluid balance conditions.

 

Treatment

There is no specific antidote. Establish and maintain an airway, ensure adequate oxygenation and respiratory function. The use of activated charcoal should be considered. Activated charcoal may reduce absorption of the drug if given within one or two hours after ingestion. In patients who are not fully conscious or have impaired gag reflex, consideration should be given to administering activated charcoal via a nasogastric tube, once the airway is protected. Cardiac and vital signs monitoring are recommended along with general symptomatic supportive measures.

 

For management of a suspected drug overdose, contact your regional Poison Control Centre immediately.

Biochemical and behavioural studies have shown that escitalopram is a potent inhibitor of serotonin (5-HT)-uptake (in vitro IC50 2nM).

 

The antidepressant action of escitalopram is presumably linked to the potentiation of serotonergic activity in the central nervous system (CNS) resulting from its inhibitory effect on the reuptake of 5-HT from the synaptic cleft.

 

Escitalopram is a highly selective Serotonin Reuptake Inhibitor (SSRI). On the basis of in vitro studies, escitalopram had no, or minimal effect on noradrenaline (NA), dopamine (DA) and gamma aminobutyric acid (GABA) uptake.

 

In contrast to many tricyclic antidepressants and some of the SSRIs, escitalopram has no or very low affinity for a series of receptors including 5-HT1A, 5-HT2, DA D1 and DA D2 receptors, a1-, a2-, β-adrenoceptors, histamine H1, muscarine cholinergic, benzodiazepine, and opioid receptors. A series of functional in vitro tests in isolated organs as well as functional in vivo tests have confirmed the lack of receptor affinity.

 

Escitalopram has high affinity for the primary binding site and an allosteric modulating effect on the serotonin transporter.

 

Allosteric modulation of the serotonin transporter enhances binding of escitalopram to the primary binding site, resulting in more complete serotonin reuptake inhibition.

 

Escitalopram is the S-enantiomer of the racemate (citalopram) and is the enantiomer to which the therapeutic activity is attributed. Pharmacological studies have shown that the R-enantiomer is not inert but counteracts the serotonin-enhancing properties of the S-enantiomer in citalopram.

 

In healthy volunteers and in patients, escitalopram did not cause clinically significant changes in vital signs, ECGs, or laboratory parameters.

 

S-demethylcitalopram, the main plasma metabolite, attains about 30% of parent compound levels after oral dosing and is about 5-fold less potent at inhibiting 5-HT reuptake than escitalopram in vitro. It is therefore unlikely to contribute significantly to the overall antidepressant effect.

Absorption

Data specific to escitalopram are unavailable. Absorption is expected to be almost complete and independent of food intake (mean Tmax is 4 hours after multiple dosing). While the absolute bioavailability of escitalopram has not been studied, it is unlikely to differ significantly from that of racemic citalopram (about 80%).

 

Distribution

The apparent volume of distribution (Vd,β/F) after oral administration is about 12 to 26 L/kg. The binding of escitalopram to human plasma proteins is independent of drug plasma levels and averages 55%.

 

Metabolism

Escitalopram is metabolised in the liver to the demethylated and didemethylated metabolites. Alternatively, the nitrogen may be oxidised to form the N-oxide metabolite. Both parent and metabolites are partly excreted as glucuronides. Unchanged escitalopram is the predominant compound in plasma. After multiple dosing, the mean concentrations of the demethyl and didemethyl metabolites are usually 28-31% and < 5% of the escitalopram concentration, respectively. Biotransformation of escitalopram to the demethylated metabolite is mediated by a combination of CYP2C19, CYP3A4 and CYP2D6.

 

Elimination

The elimination half-life (t½β) after multiple dosing is about 30 hours and the oral plasma clearance (Cloral) is about 0.6 L/min.

Escitalopram and major metabolites are, like racemic citalopram, assumed to be eliminated both by the hepatic (metabolic) and renal routes with the major part of the dose excreted as metabolites in urine. Approximately 8.0% of escitalopram is eliminated unchanged in urine and 9.6% as the S-demethylcitalopram metabolite based on 20 mg escitalopram data. Hepatic clearance is mainly by the P450 enzyme system.

The pharmacokinetics of escitalopram are linear over the clinical dosage range. Steady state plasma levels are achieved in about 1 week. Average steady state concentrations of 50nmol/L (range 20 to 125 nmol/L) are achieved at a daily dose of 10 mg.

 

Reduced Hepatic Function

In patients with mild or moderate hepatic impairment (Child-Pugh Criteria A and B), the half-life of escitalopram was about twice as long and the exposure was about 60% higher than in subjects with normal liver function (see PRECAUTIONS and DOSAGE AND ADMINISTRATION).

 

Reduced Renal Function

While there is no specific data, the use of escitalopram in reduced renal function may be extrapolated from that of racemic citalopram. Escitalopram is expected to be eliminated more slowly in patients with mild to moderate reduction of renal function with no major impact on the escitalopram concentrations in serum, At present, no information is available for the treatment of patients with severely reduced renal function (creatinine clearance < 20 mL/min).

 

Elderly Patients (> 65 years)

Escitalopram pharmacokinetics in subjects > 65 years of age were compared to younger subjects in a single-dose and a multiple-dose study. Escitalopram AUC and half-life were increased by approximately 50% in elderly subjects, and Cmax was unchanged. 10 mg is the recommended dose for elderly patients.

 

Gender

In a multiple-dose study of escitalopram (10 mg/day for 3 weeks) in 18 male (9 elderly and 9 young) and 18 female (9 elderly and 9 young) subjects, there were no differences in AUC, Cmax and half-life between the male and female subjects. No adjustment of dosage on the basis of gender is needed.

 

Polymorphism

It has been observed that poor metabolisers with respect to CYP2C19 have twice as high a plasma concentration of escitalopram as extensive metabolisers. No significant change in exposure was observed in poor metabolisers with respect to CYP2D6 (see DOSAGE AND ADMINISTRATION).

High doses of escitalopram, which resulted in plasma Cmax for escitalopram and metabolites at least 8-fold greater than anticipated clinically, have been associated with convulsions, ECG abnomalities and cardiovascular changes in experimental animals. Of the cardiovascular changes, cardiotoxicity (including congestive heart failure) was observed in comparative toxicological studies in rats following oral escitalopram or citalopram administration for 4 to 13 weeks and appears to correlate with peak plasma concentrations although its exact mechanism is not clear. Clinical experiences with citalopram, and the clinical trial experience with escitalopram, do not indicate that these findings have a clinical correlation.

In addition, each tablet contains the following inactive ingredients: microcrystalline cellulose, lactose, magnesium stearate, croscarmellose sodium, butylated hydroxyanisole, hypromellose, hydroxypropylcellulose, macrogol 8000 and titanium dioxide.

None Applicable

24 months

Store below 30°C.

Primary packaging: Blister

Secondary packaging: Carton

None Applicable