Switching antidepressant treatment

Switching strategies available include: (1)

Cross-tapering

Gradually reduce and stop the first antidepressant whilst simultaneously starting the second at a low dose and gradually increasing. Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability.

Direct switching

Direct switches may be possible when antidepressants have similar pharmacology or mode of action. The second antidepressant should alleviate discontinuation symptoms of the first. Stop the first antidepressant and start the second at the usual therapeutic dose the next day.

Taper, stop and switch

Gradually reduce and then stop the first antidepressant; start the second immediately after stopping the first, usually on the next day.

Taper, washout and switch

Gradually reduce the dose of the first antidepressant and stop; wait for a period (the “washout”) before starting the second.

Stop, washout and switch

Stop the first antidepressant; wait for a period (the “washout”), before starting the second.

SSRI SWITCHING

Agomelatine

• From all except fluvoxamine;

Cross-taper

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability.

There is limited experience with this switch so extra caution is required. Although interactions are not expected, agomelatine is not expected to mitigate withdrawal reactions from stopping the SSRI.

Additional caution when switching from fluoxetine

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping as fluoxetine and its active metabolite have a long half-life.

• From fluvoxamine

Taper, washout and switch

Gradually reduce the dose of fluvoxamine and stop; wait 4 days before starting agomelatine.

Cross-tapering is not appropriate with this switch because fluvoxamine is a potent inhibitor of the liver enzyme CYP1A2 which is involved in the metabolism of agomelatine. There is therefore a risk of raised agomelatine levels in the body when they are administered together.

Clomipramine

Cross-tapering is not recommended and should only be undertaken if specialist advice is in place, this is because clomipramine is a potent serotonin reuptake inhibitor so there is a high risk of serotonin syndrome.

• From all except fluoxetine, fluvoxamine and paroxetine;

Taper, stop and switch

Gradually reduce the dose of the SSRI and stop. Start low dose clomipramine the following day.

• From fluoxetine

Taper, washout and switch

Gradually reduce the dose of fluoxetine to 20mg daily and stop; wait 14 to 21 days before starting low dose clomipramine. Clinicians should decide the duration of the washout period on a case-by-case basis.

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping, as fluoxetine and its active metabolite have a long half-life.

If switching from fluoxetine, caution is required as it is a potent inhibitor of the liver enzyme CYP2D6 which is involved in the metabolism of clomipramine. There is therefore a risk of raised clomipramine levels in the body when switching.

• From fluvoxamine or paroxetine

Taper, stop and switch

Gradually reduce the dose of fluvoxamine or paroxetine and stop. Start low dose clomipramine the following day.

Taper, washout and switch

Alternatively, gradually reduce the dose of fluvoxamine or paroxetine and stop; wait for a period before starting clomipramine. Clinicians should decide the duration of the washout period on a case-by-case basis.

Additional caution

If switching from fluvoxamine or paroxetine, caution is required because fluvoxamine is a potent inhibitor of the liver enzyme CYP1A2, and paroxetine is a potent inhibitor of the liver enzyme CYP2D6; these enzymes are involved in the metabolism of clomipramine. There is therefore a risk of raised clomipramine levels in the body when they are administered together.

Mirtazapine

Cross-taper

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability.

Additional caution when switching from fluoxetine

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping, as fluoxetine and its active metabolite have a long half-life.

Additional caution when switching from fluvoxamine

Start mirtazapine at a dose of 15mg daily. This caution is required because fluvoxamine is a potent inhibitor of the liver enzyme CYP1A2 which is involved in the metabolism of mirtazapine. There is therefore a risk of raised mirtazapine levels in the body when they are administered together.

Moclobemide

Taper, washout and switch

For any SSRI, you should gradually reduce the dose and stop. You will then need to wait for a period, dependent on the antidepressant being switched from (see below), before starting moclobemide.

Cross-tapering is not recommended due to the high risk of serotonin syndrome.

• From all except fluoxetine and sertraline

After stopping the SSRI, wait 7 days before starting moclobemide.

• From fluoxetine

After stopping fluoxetine, wait 5 to 6 weeks before starting moclobemide. Clinicians should decide the duration of the washout period on a case-by-case basis.

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping, as fluoxetine and its active metabolite have a long half-life.

• From sertraline

After stopping sertraline, wait 7 to 13 days before starting moclobemide. The manufacturer advises a 7 day washout period but 13 days may be considered to account for the long half-life of sertraline’s active metabolite. Clinicians should decide the duration of the washout period on a case-by-case basis.

Monoamine oxidase inhibitors (MAOIs)

Switching to an MAOI is always a complex switch and you should follow specialist advice.

Taper, washout and switch with specialist advice

For any SSRI, you should gradually reduce the dose and stop. You will then need to wait for a period (see below), dependent on the antidepressant being switched from, before starting the MAOI. The specialist will advise the duration of the washout period on a case-by-case basis taking into consideration the MAOI being started.

Cross-tapering is not recommended due to the high risk of serotonin syndrome.

• From all except fluoxetine

After stopping the SSRI, wait 7 to 14 days before starting the MAOI.

• From fluoxetine

After stopping fluoxetine, wait 5 to 6 weeks before starting the MAOI.

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping, as fluoxetine and its active metabolite have a long half-life.

Another SSRI

• From all except fluoxetine

Direct switch

A direct switch, i.e. stopping one antidepressant and then starting the new antidepressant the following day, is normally possible.

• From fluoxetine

Taper, washout and switch

Gradually reduce the dose of fluoxetine to 20mg daily and stop; wait 4 to 7 days before starting low dose SSRI. Clinicians should decide the duration of the washout period on a case-by-case basis.

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping, as fluoxetine and its active metabolite have a long half-life.

Serotonin and noradrenaline reuptake inhibitors (SNRIs)

• From all except fluoxetine

Direct switch

A direct switch, i.e. stopping one antidepressant and then starting the new antidepressant the following day, is normally possible.

Additional caution when switching from paroxetine

If switching from paroxetine, caution is required because it is a potent inhibitor of the liver enzyme CYP2D6 which is involved in the metabolism of duloxetine and venlafaxine. There is therefore a risk of raised duloxetine or venlafaxine levels in the body when they are administered together.

Additional caution when switching from fluvoxamine

If switching from fluvoxamine, caution is required because it is a potent inhibitor of the liver enzyme CYP1A2 which is involved in the metabolism of duloxetine. There is therefore a risk of raised duloxetine levels in the body when they are administered together.

• From fluoxetine

Taper, washout and switch

Gradually reduce the dose of fluoxetine to 20mg daily and stop; wait 4 to 7 days before starting the SNRI. Clinicians should decide the duration of the washout period on a case-by-case basis.

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping, as fluoxetine and its active metabolite have a long half-life.

If switching from fluoxetine, caution is required as it is a potent inhibitor of the liver enzyme CYP2D6 which is involved in the metabolism of duloxetine and venlafaxine. There is therefore a risk of raised duloxetine or venlafaxine levels in the body when switching.

Trazodone

Cross-taper

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability.

Additional caution when switching from fluoxetine or paroxetine

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping, as fluoxetine and its active metabolite have a long half-life.

If switching from fluoxetine or paroxetine, caution is required as they are potent inhibitors of the liver enzyme CYP2D6 which is involved in the metabolism of trazodone. There is therefore there is a risk of raised trazodone levels in the body when they are administered together.

Tricyclic antidepressants (TCAs) other than clomipramine

Switching to dosulepin requires specialist advice and should not be done in primary care due to the increased cardiac risk and toxicity in overdose.

• From all except fluoxetine, fluvoxamine and paroxetine

Cross-taper

Cross-tapering, starting with a low dose TCA can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability.

• From fluoxetine

Taper, washout and switch

Gradually reduce the dose of fluoxetine to 20mg daily and stop; wait 4 to 7 days before starting low dose TCA. Clinicians should decide the duration of the washout period on a case-by-case basis.

If switching from fluoxetine, caution is required as it is a potent inhibitor of the liver enzyme CYP2D6 which is involved in the metabolism of TCAs. There is therefore a risk of raised TCA levels in the body when switching.

Fluoxetine may still cause medicine interactions 5 or 6 weeks after stopping, as fluoxetine and its active metabolite have a long half-life.

• From fluvoxamine

Cross-taper

Cross-tapering, starting with a low dose TCA can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability. It could include:

• gradually reducing the dose of fluvoxamine
• then adding the low dose TCA
• then stopping fluvoxamine after 4 to 7 days. Clinicians should decide the duration of the washout period on a case-by-case basis.

Taper, washout and switch

Alternatively, gradually reduce the dose of fluvoxamine and stop; wait for a period before starting low dose TCA. Clinicians should decide the duration of the washout period on a case-by-case basis.

Additional caution

If switching from fluvoxamine, caution is required because it is a potent inhibitor of the liver enzyme CYP1A2 which is involved in the metabolism of TCAs. There is therefore a risk of raised TCA levels in the body when they are administered together.

• From paroxetine

Cross-taper

Cross-tapering, starting with a low dose TCA can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability. It could include:

• gradually reducing the dose of paroxetine to 10mg daily
• then adding the low dose TCA
• then stopping paroxetine after 4 to 7 days. Clinicians should decide the duration of the washout period on a case-by-case basis.

Taper, washout and switch

Alternatively, gradually reduce the dose of paroxetine and stop; wait for a period before starting low dose TCA. Clinicians should decide the duration of the washout period on a case-by-case basis.

Additional caution

If switching from paroxetine, caution is required because it is a potent inhibitor of the liver enzyme CYP2D6 which is involved in the metabolism of TCAs. There is therefore a risk of raised TCA levels in the body when they are administered together.

Vortioxetine

There is limited experience with this switch so extra caution is required to avoid serotonin syndrome.

• From all except fluoxetine

Direct switch

A direct switch, i.e. stopping one medicine and then starting the new medicine the following day, is normally possible.

Taper, washout and switch

Alternatively, gradually reduce the dose of the SSRI and stop; wait for a period before starting vortioxetine. Clinicians should decide the duration of the washout period on a case-by-case basis.

TCA SWITCHING

Agomelatine

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability. There is limited experience with this switch so extra caution is required. Although interactions are not expected, agomelatine is not expected to mitigate withdrawal reactions from stopping TCAs.

Mirtazapine

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks - the speed is determined by individual tolerability.

Moclobemide

Taper, washout and switch

For any TCA, you should gradually reduce the dose and stop. You will then need to wait for a period, dependent on the drug being switched from (see below), before starting moclobemide.

Cross-tapering is not recommended due to the high risk of serotonin syndrome.

• From TCAs other than clomipramine

After stopping the TCA, wait 7 days before starting moclobemide.

• From clomipramine

After stopping clomipramine, wait 7 to 21 days before starting moclobemide. The manufacturer for clomipramine suggests a washout period of 21 days whereas other sources suggest shorter periods. Clinicians should decide the duration of the washout period on a case-by-case basis.

Monoamine oxidase inhibitors (MAOIs)

Switching to an MAOI is always a complex switch and you should follow specialist advice.

Taper, washout and switch with specialist advice

For any TCA, you should gradually reduce the dose and stop. You will then need to wait for a period, dependent on the antidepressant being switched from (see below), before starting the MAOI. The specialist will advise the duration of the washout period on a case-by-case basis taking into consideration the MAOI being started.

Cross-tapering is not recommended due to the high risk of serotonin syndrome.

• From all except clomipramine and imipramine

After stopping the TCA, wait 7 to 21 days before starting low dose MAOI.

• From clomipramine or imipramine

After stopping clomipramine or imipramine, wait 21 days before starting low dose MAOI.

Selective serotonin reuptake inhibitors (SSRIs)

• From all except clomipramine

Cross-taper

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability. It could include:

• halving the dose of the TCA
• then adding the SSRI at the usual starting dose
• then slowly reducing and stopping the TCA over 5 to 7 days

Additional caution when switching to fluoxetine, fluvoxamine and paroxetine

If switching to fluoxetine, fluvoxamine or paroxetine, caution is required because fluvoxamine is a potent inhibitor of the liver enzyme CYP1A2 and fluoxetine and paroxetine are potent inhibitors of the liver enzyme CYP2D6; these enzymes are involved in the metabolism of TCAs. Although the TCA is being withdrawn, you should still be aware of the risk of raised TCA levels in the body when they are administered together.

• From clomipramine

Taper, stop and switch

Gradually reduce the dose of clomipramine and stop. Start a low dose SSRI the following day. If switching to fluoxetine it should be started at 10mg daily.

Cross-tapering is not recommended and should only be undertaken if specialist advice is in place, this is because clomipramine is a potent serotonin reuptake inhibitor so there is a high risk of serotonin syndrome.

TCAs to serotonin and noradrenaline reuptake inhibitors (SNRIs)

• From all except clomipramine

Cross-taper

Cross-tapering starting with a low dose SNRI can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability.

• From clomipramine

Taper, stop and switch

If switching from clomipramine, gradually reduce the dose of clomipramine and stop. Start low dose SNRI the following day.

Cross-tapering is not recommended and should only be undertaken if specialist advice is in place, this is because clomipramine is a potent serotonin reuptake inhibitor so there is a high risk of serotonin syndrome.

Trazodone

Cross-taper

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability. It should include:

• halving the dose of the TCA
• then adding trazodone
• then slowly reducing and stopping the TCA

Another TCA

Switching to dosulepin requires specialist advice and should not be done in primary care due to the increased cardiac risk and toxicity in overdose.

• From all except clomipramine

Direct switch

A direct switch, i.e. stopping one medicine and then starting the new medicine the following day, is normally possible.

• From clomipramine

Cross-taper

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability.

Vortioxetine

There is limited experience with this switch so extra caution is required to avoid serotonin syndrome.

• From all except clomipramine

Cross-taper

Cross-tapering can usually be undertaken cautiously over 2 to 4 weeks, the speed is determined by individual tolerability. It should include:

• halving the dose of the TCA
• then adding vortioxetine
• then slowly reducing and stopping the TCA

Taper, washout and switch

Alternatively, gradually reduce the dose of the TCA and stop; wait for a period before starting vortioxetine. Clinicians should decide the duration of the washout period on a case-by-case basis.

• From clomipramine

Cross-tapering is not recommended and should only be undertaken if specialist advice is in place, this is because clomipramine is a potent serotonin reuptake inhibitor so there is a high risk of serotonin syndrome.

Taper, stop and switch

If switching from clomipramine, gradually reduce the dose of clomipramine and stop. Start low dose vortioxetine the following day.

Taper, washout and switch

Alternatively, gradually reduce the dose of clomipramine and stop; wait for a period before starting vortioxetine. Clinicians should decide the duration of the washout period on a case-by-case basis.

Stopping antidepressant treatment

When stopping a person's antidepressant medication: (2)

• take into account the pharmacokinetic profile (for example, the half-life of the medication as antidepressants with a short half-life will need to be tapered more slowly) and the duration of treatment
• slowly reduce the dose to zero in a step-wise fashion, at each step prescribing a proportion of the previous dose (for example, 50% of previous dose)
• consider using smaller reductions (for example, 25%) as the dose becomes lower
• if, once very small doses have been reached, slow tapering cannot be achieved using tablets or capsules, consider using liquid preparations if available
• ensure the speed and duration of withdrawal is led by and agreed with the person taking the prescribed medication, ensuring that any withdrawal symptoms have resolved or are tolerable before making the next dose reduction
• take into account the broader clinical context such as the potential benefit of more rapid withdrawal if there are serious or intolerable side effects (for example, hyponatraemia or upper gastrointestinal tract bleeding)
• take into account that more rapid withdrawal may be appropriate when switching antidepressants
• recognise that withdrawal may take weeks or months to complete successfully
• the timing of when to stop antidepressant treatment is discussed in menu item below (length of antidepressant treatment)
• patients should be advised not to stop treatment suddenly or omit doses - patients should also be forewarned about possible symptoms that may occur when treatment is discontinued

Reference

1. NHS Specialist Pharmacy Service. Switching strategies for antidepressants. Published May 2024 (online)
2. NICE. Depression in adults: treatment and management. NICE guideline NG222. Published June 2022