Citalopram theoretically causes side effects by increasing the concentration of
serotonin in other parts of the body (e.g., the intestines). Other side effects, such as increased apathy and emotional flattening, may be caused by the decrease in
dopamine release associated with increased serotonin. Citalopram is also a mild
antihistamine, which may be responsible for some of its sedating properties. Citalopram is associated with a higher risk of arrhythmia than other
SSRIs. Citalopram and other SSRIs can induce a
mixed state, especially in those with undiagnosed
bipolar disorder.
Post-SSRI sexual dysfunction Sexual dysfunction is a common side effect of citalopram and other SSRIs. In some patients, these effects persist after discontinuation of the drug, a condition known as
post-SSRI sexual dysfunction (PSSD). Characteristic symptoms include genital numbness, pleasureless or weak orgasm, loss of libido, and
erectile dysfunction; non-sexual symptoms such as
emotional blunting and cognitive impairment may also occur. The
DSM-5 noted in 2013 that serotonin reuptake inhibitor-induced sexual dysfunction may persist after the agent is discontinued. A 2023 retrospective cohort study of over 12,000 males estimated the risk of irreversible sexual dysfunction at approximately 0.46% of patients treated with serotonergic antidepressants, including SSRIs, though the actual prevalence remains uncertain and the condition is likely underreported. A 2023 systematic review found that citalopram was the second most frequently reported SSRI in PSSD case reports, after
escitalopram. In 2019, the
European Medicines Agency's
Pharmacovigilance Risk Assessment Committee (PRAC) recommended that product labels for all SSRIs and SNRIs, including citalopram, be updated to state that sexual dysfunction may be long-lasting even after treatment is stopped.
Health Canada followed with similar label updates in 2021.
Abnormal heart rhythm In August 2011, the FDA announced, "Citalopram causes dose-dependent
QT interval prolongation. Citalopram should no longer be prescribed at doses greater than 40 mg per day". A further clarification, issued in March 2012, restricted the maximum dose to 20 mg for subgroups of patients, including those older than 60 years and those taking an inhibitor of cytochrome P450 2C19.7.
Endocrine effects As with other SSRIs, citalopram can cause an increase in serum
prolactin level. Citalopram has no significant effect on insulin sensitivity in women of reproductive age and no changes in glycaemic control were seen in another trial.
Exposure in pregnancy Antidepressant exposure (including citalopram) during pregnancy is associated with shorter duration of
gestation (by three days), increased risk of preterm delivery (by 55%), lower birth weight (by 75 g), and lower
Apgar scores (by <0.4 points). Antidepressant exposure is not associated with an increased risk of spontaneous abortion. It is uncertain whether there is an increased prevalence of septal heart defects among children whose mothers were prescribed an SSRI in early pregnancy.
Overdose Overdosage may result in vomiting, sedation, disturbances in heart rhythm, dizziness, sweating, nausea, tremors, and rarely amnesia, confusion, coma, or convulsions. It is the most dangerous of SSRIs in overdose.
Suicidality In the United States, citalopram carries a
boxed warning stating it may increase suicidal thinking and behavior in those under age 24. Electric shock-like sensations are typical for SSRI discontinuation. Withdrawal symptoms can occur when this medicine is suddenly stopped, such as
paraesthesiae, sleeping problems (difficulty sleeping and intense dreams), feeling dizzy, agitated or anxious, nausea, vomiting, tremors, confusion, sweating, headache, diarrhea, palpitations, changes in emotions, irritability, and eye or eyesight problems. Treatment with citalopram should be reduced gradually when treatment is finished. == Interactions ==