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Antidep

Antidep (Imipramine 25/75 mg) — first-generation TCA for depression, panic, paediatric enuresis ≥6 y. reference TCA — balanced 5-HT/NA reuptake blockade.

Medisch beoordeeld door Morgan Ellis — Apotheekonderzoeker · 8 jaar ervaring  · Laatst beoordeeld: mei 2026

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Antidep (Imipramine 25 / 75 mg) is a tricyclic antidepressant. Used for major depression, panic disorder, and (uniquely) paediatric nocturnal enuresis. Higher tolerability burden than SSRIs — second-line for most patients.

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What Antidep is and how it works

Antidep is a Imipramine-containing tablet supplied by Intas. Available strengths: 25 / 75 mg.

Imipramine was the first tricyclic antidepressant (Geigy, 1957) and remains a useful agent for major depression where SSRIs have failed, panic disorder, and — uniquely — paediatric nocturnal enuresis (bedwetting) where behavioural measures have failed.

Tricyclic antidepressants block the reuptake of serotonin and noradrenaline at presynaptic transporters, similar to SSRIs and SNRIs. Their tolerability disadvantage comes from off-target receptor blockade: muscarinic (anticholinergic side effects), histaminergic H1 (sedation, weight gain), and α1-adrenergic (orthostatic hypotension). They also block fast sodium channels in cardiac tissue — the basis for both their analgesic action and their cardiac toxicity in overdose.

Imipramine has the most balanced serotonin-noradrenaline reuptake inhibition of the TCAs and is the historical reference for newer agents.

Indicaties en dosering

IndicatieStartdoseringStreefdoseringMaximaal
Major depression (adult)25–50 mg HS100–200 mg/day300 mg
Panic disorder10 mg OD × 1 wk50–150 mg/day200 mg
Paediatric enuresis (≥6 y)1.0–1.5 mg/kg HS1.5–2.5 mg/kg HS2.5 mg/kg or 75 mg, whichever lower
Older adults10 mg HS30–50 mg/dayby tolerability

Belangrijke veiligheidsoverwegingen

Cardiac risk and overdose toxicity

TCAs prolong QRS and QT, and overdose is life-threatening — historically the most common cause of antidepressant fatalities. Baseline ECG before initiating in patients with known cardiac disease, on QT-prolonging therapy, or in older adults. Do not start in recent MI, conduction abnormality, uncompensated heart failure, or congenital long QT. Limit dispense quantities in patients at suicide risk — the therapeutic-to-toxic ratio is narrow.

Anticholinergic burden

Dry mouth, constipation, blurred vision, urinary hesitancy, cognitive slowing — universal at therapeutic doses. Avoid in narrow-angle glaucoma, BPH with significant retention, and dementia. Pair with chewing gum / sugar-free lozenges, fibre + fluid, and stool softeners.

Zwarte waarschuwing voor suïcidaliteit (onder 25)

All antidepressants carry an FDA black-box warning for increased suicidal ideation in patients under 25 — particularly relevant for clomipramine in adolescent OCD.

Veelvoorkomende bijwerkingen

  • Anticholinergic: dry mouth, constipation, blurred vision, urinary hesitancy.
  • Sedation: particularly doxepin and clomipramine; bedtime dosing helps.
  • Cardiovasculair: orthostatic hypotension (α1 block), tachycardia, conduction-interval prolongation.
  • Metabool: weight gain (5–10 kg over 12 months in many patients), increased appetite.
  • Sexual: reduced libido, delayed ejaculation (sometimes used clinically for premature ejaculation), erectile difficulty.
  • Withdrawal: taper over 4 weeks; abrupt cessation produces flu-like symptoms, GI upset, and sleep disturbance.

Geneesmiddelinteracties

  • MAOIs — absolute contraindication. 14-day washout each direction.
  • SSRIs / SNRIs — additive serotonergic risk; CYP2D6 inhibition by fluoxetine and paroxetine raises TCA levels.
  • QT-verlengende geneesmiddelen (azoles, macrolides, amiodarone, sotalol, methadone, ondansetron, antipsychotics) — additive risk.
  • Other anticholinergics (oxybutynin, benztropine, antihistamines, clozapine, olanzapine) — additive burden in older adults.
  • CNS depressants — additive sedation.
  • Tramadol, bupropion, fluoroquinolones — lower seizure threshold; additive seizure risk.

Zwangerschap, borstvoeding, pediatrie

TCAs are FDA pregnancy category C. Late-pregnancy exposure can produce neonatal anticholinergic withdrawal. Lactation: TCAs pass into breast milk in small amounts; nortriptyline and imipramine are the most-studied. Paediatric: imipramine is licensed from age 6 (enuresis) and clomipramine from age 10 (OCD); doxepin in adolescents only with specialist input.

Opslag

Store at 15–30 °C, away from direct sunlight, in original packaging. Keep out of reach of children — TCA paediatric ingestion is a medical emergency.

Veelgestelde vragen

How long until Antidep works?

TCAs typically show benefit within 2–4 weeks. The sleep and anxiety improvements often appear in week 1; the antidepressant effect builds over 4–6 weeks.

Why bedtime dosing?

Doxepin, clomipramine, and imipramine are all sedating. Bedtime dosing recruits the sedation as a side-effect benefit (sleep) instead of a side-effect burden (daytime drowsiness). It also reduces orthostatic hypotension by sleeping through the peak.

Is Antidep safe in older adults?

TCAs are on the Beers Criteria list of potentially inappropriate medications in older adults because of anticholinergic burden, orthostatic hypotension, and cardiac risk. They are not absolutely contraindicated but are generally second-line — SSRIs/SNRIs are preferred unless a specific benefit (e.g. pain, sleep) outweighs the risks.

Can I drink alcohol on Antidep?

Alcohol amplifies TCA sedation and orthostatic effects. Limit to occasional and modest consumption; avoid binge drinking entirely. The combination is not usually dangerous in moderation but feels worse than either alone.

What is the overdose risk?

TCAs are among the most lethal classes of medication in overdose — cardiac conduction collapse, seizures, and coma can occur at relatively low multiples of the therapeutic dose. Limit dispense quantities in patients at any suicide risk. If overdose is suspected, present to emergency immediately — sodium bicarbonate is the antidote for the cardiac toxicity but timing matters.

Will Antidep affect my driving?

Sedation and reaction-time impairment are common in the first 1–2 weeks. Avoid driving until steady-state tolerability is known. Some patients tolerate full doses indefinitely without driving impairment; others remain too sedated even at low doses.

Can Antidep be combined with an SSRI?

Generally no — combination raises serotonin syndrome risk and serum TCA levels (particularly with fluoxetine and paroxetine). The combination is sometimes used in refractory OCD or depression under specialist supervision with TDM, never empirically.

How do I taper Antidep?

Reduce by approximately 25–50% of the dose every 2 weeks. Withdrawal (sometimes called “TCA flu”) produces malaise, GI upset, and sleep disturbance — manageable with slower tapers. Talk to the prescriber before stopping.

Does Antidep cause weight gain?

Yes — most TCAs cause meaningful weight gain over 6–12 months, often 5–10 kg. Doxepin and amitriptyline are the worst; nortriptyline less so. If this is a major concern, raise it before initiation — an SSRI/SNRI may be a better fit.

Can Antidep be used for chronic pain?

Yes — TCAs (especially amitriptyline, nortriptyline, and imipramine) at low doses (10–75 mg) are first-line for diabetic peripheral neuropathy, post-herpetic neuralgia, and tension-type chronic headache. Sodium-channel blockade is the dominant mechanism. The analgesic effect is independent of the antidepressant effect and appears earlier (1–2 weeks).

Andere medicijnen voor geestelijke gezondheid

Medisch disclaimer. Deze pagina is educatief en geen vervanging voor persoonlijk medisch advies. Farmacotherapie voor geestelijke gezondheid dient te worden gestart, gecontroleerd en aangepast onder begeleiding van een gekwalificeerde clinicus. Als u of iemand die u kent in een suïcidale crisis verkeert, neem dan onmiddellijk contact op met de plaatselijke hulpdiensten, of bel de suïcidepreventielijn van uw land (VS/Canada: 988; VK: Samaritans 116 123; internationale lijst: findahelpline.com).

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