Citalopram, Dapoxetine, Escitalopram, Fluoxetine, Fluvoxamine, Paroxetine, Sertraline |
Issues for Surgery |
Risk of withdrawal symptoms if omitted (see Further Information). For depression, panic disorder, anxiety disorders, obsessive-compulsive disorder, bulimia nervosa or hot flushes in women with breast cancer - risk of loss of symptom control if omitted. Risk of serotonin syndrome if continued (see Interaction(s) with Common Anaesthetic Agents and Interaction(s) with other Common Medicines used in the Perioperative Period). Risk of QT-interval prolongation with citalopram or escitalopram if continued (see Interaction(s) with other Common Medicines used in the Perioperative Period). Risk of bleeding if continued (see Further Information). |
Advice in the Perioperative period |
Elective and Emergency Surgery Continue1, 2 – check sodium levels pre-operatively (see Further Information). Dapoxetine is licensed for on-demand treatment before anticipated sexual activity – although not needed in the perioperative period manufacturer advises potential for interactions if dose(s) taken in previous 7 days3 (see Interaction(s) with Common Anaesthetic Agents and Interaction(s) with other Common Medicines used in the Perioperative Period). Post-operative Advice If a long Nil by Mouth (NBM) period is anticipated, or if there are concerns with enteral absorption, advice on alternative preparations / routes should be sought from a Psychiatrist. Monitor electrolytes, particularly sodium, if risk factors for hyponatraemia (see Further Information). Patients undergoing Vagotomy or Gastrectomy |
Interaction(s) with Common Anaesthetic Agents |
CNS Excitation (Serotonin Syndrome) Some opioids act as weak serotonin reuptake inhibitors (SRIs) and can precipitate serotonin syndrome in conjunction with SSRIs. Symptoms of serotonin syndrome have been reported in patients taking SSRIs with the following opioids1, 2, 5, 6, 7: -
There is little evidence to suggest the above medications cannot be used safely and effectively with SSRIs, however, patients should be monitored closely and the possibility of serotonin toxicity considered if altered mental state, autonomic dysfunction or neuromuscular adverse effects are observed with concomitant treatment6. Neuromuscular blocking drugs (NMBDs) SSRIs reduce the normal activity of plasma cholinesterases; the action of mivacurium and suxamethonium may be prolonged as they are inactivated by hydrolysis by plasma cholinesterases. Other NMBDs with different mechanisms of metabolism or elimination are unlikely to be affected5, 6. There have been no published reports of this interaction in clinical practice, however, bear in mind in the event of an unexpected response to treatment6. Propofol Pronounced involuntary upper limb movements immediately after anaesthetic induction were reported in two females taking fluoxetine. It is not clear whether this is an interaction between fluoxetine and propofol or a rare, but previously reported, reaction to propofol6. Ropivacaine Fluvoxamine, a potent inhibitor of CYP1A2, significantly reduces plasma clearance of ropivacaine in vivo almost doubling the half-life. Prolonged administration of ropivacaine should be avoided in patients taking fluvoxamine6, 8. QT-Interval Prolongation (see also Interaction(s) with other Common Medicines used in the Perioperative Period) Anaesthetic agents that may be used in the perioperative period that are known to, or predicted to, prolong the QT-interval include5, 6: -
*monitor ECG with concurrent use if risk factors for QT-prolongation are also present (increasing age, female sex, cardiac disease, and some metabolic disturbances e.g. hypokalaemia) |
Interaction(s) with other Common Medicines used in the Perioperative Period |
CNS Excitation (Serotonin Syndrome) Opioids Methylthioninium chloride (methylene blue) Other medications
Monitor patients for symptoms of serotonin syndrome such as fever, tremors, diarrhoea, and agitation. Concurrent treatment should be stopped if serotonin syndrome occurs5. QT-Interval Prolongation Citalopram and escitalopram are known to cause QT-interval prolongation5, 6, 11, 12. Co-administration with other medicines known to prolong the QT-interval must be based on a careful assessment of the potential risks and benefits for each patient since the risk of torsade de pointes may increase. Medicines that may be used in the perioperative period that are known to prolong the QT-interval include5, 6:-
*monitor ECG with concurrent use if risk factors for QT-interval prolongation also present (increasing age, female sex, cardiac disease, and some metabolic disturbances e.g. hypokalaemia) Increased risk of bleeding (see also Further Information) Concomitant use of SSRIs with other medications that can increase the risk of bleeding e.g. Non-Steroidal Anti-inflammatory Drugs (NSAIDs) may have an additive effect1, 3, 4, 5, 6, 7, 11, 12, 13, 14, 15. If the combination of SSRI and NSAID cannot be avoided, gastroprotection with a H2-receptor antagonist or proton pump inhibitor should be considered for the duration of concomitant use, particularly in elderly patients (who seem at greater risk of SSRI-associated bleeding) or patients with a history of gastrointestinal bleeding5, 6, 11. Increased risk of hyponatraemia (see also Further Information) Concomitant use of SSRIs with NSAIDS may increase the risk of hyponatraemia5, 16. Codeine Fluoxetine and paroxetine (but not other SSRIs) are potent CYP2D6 inhibitors so are predicted to decrease the metabolism of codeine to morphine, possibly reducing its analgesic efficacy. With concomitant use monitor patients for a reduced response to codeine and consider using an alternative analgesic if this is observed4, 5, 6. Tramadol SSRIs can lower the seizure threshold; concurrent use with tramadol that also lowers the seizure threshold may have an additive effect on the risk of seizure6, 13. In addition tramadol may increase the risk of serotonin syndrome (see Interaction(s) with Common Anaesthetic Agents). Concomitant administration of tramadol with fluoxetine and paroxetine may result in reduced analgesic efficacy due to CYP2D6 inhibition6. |
Further Information |
Bleeding Serotonin released from platelets potentiates platelet aggregation. SSRIs can block platelets reuptake of serotonin from the bloodstream leading to serotonin depletion, impairment of haemostatic function and an increased risk of bleeding1, 16, 17. There are reports of prolonged bleeding time and / or bleeding abnormalities (gastrointestinal bleeding, gynaecological haemorrhages, ecchymoses, cutaneous or mucous bleedings) in patients receiving SSRIs1, 3, 4, 7, 11, 12, 13, 14, 15. This risk is further increased with concomitant use of other medications known to affect platelet function (see Interaction(s) with other Common Medicines used in the Perioperative Period). Observational studies suggest a link between SSRIs and an increased risk of perioperative bleeding, with one study indicating SSRIs increase the odds of in-hospital mortality, bleeding and readmission at 30 days; however, patient factors rather than medication factors could not be excluded as the cause1, 17. Other studies have shown increased need for red blood cell transfusions in patients having coronary artery bypass or orthopaedic surgery1, 7, 16, 17. However, a case-control study did not demonstrate an increase in blood loss following hip and knee arthroplasty18. Clinicians should be aware that SSRIs may contribute to perioperative bleeding, further research is needed to determine the significance of this17. Withdrawal Abruptly stopping or interrupting treatment with SSRIs is not recommended5, 16. Common withdrawal symptoms include dizziness, numbness, tingling, nausea, vomiting, headache, sweating, anxiety and sleep disorders. In some cases, withdrawal symptoms can be severe and disabling7, 16. Withdrawal reactions usually occur within 3 days of stopping an SSRI, although a delay of up to 2 weeks may be noted with fluoxetine due to its long half-life. Paroxetine and fluvoxamine are associated with a higher risk of withdrawal reactions, possibly due to their short half-lives7. The risk of withdrawal is increased if SSRIs are stopped suddenly after regular administration for more than 8 weeks5. Hyponatraemia Hyponatraemia, possibly as a result of inappropriate secretion of antidiuretic hormone has been associated with SSRIs1, 16. Caution is required in patients at increased risk of hyponatraemia, such as elderly, or volume depleted / dehydrated patients or patients treated with diuretics15, 16. |
References |
|