<\/p>\n
Cotrip<\/strong> \u03c0\u03b5\u03c1\u03b9\u03ad\u03c7\u03b5\u03b9 amitriptyline 10 \/ 25 \/ 50 \/ 75 mg<\/strong> from a WHO-GMP certified manufacturer — a tertiary-amine tricyclic antidepressant (TCA)<\/strong> and the most widely-prescribed tricyclic worldwide and the classic first-line tricyclic for migraine prevention. Although FDA-approved only for depression, tricyclic antidepressants have decades of evidence-based use at lower doses for migraine prevention, chronic tension-type headache, neuropathic pain, fibromyalgia, and chronic insomnia associated with pain<\/strong>. For \u03c0\u03c1\u03cc\u03bb\u03b7\u03c8\u03b7 \u03b7\u03bc\u03b9\u03ba\u03c1\u03b1\u03bd\u03b9\u03ce\u03bd<\/strong>: start 10 mg nightly, titrate to 25-75 mg nightly (migraine-prevention range; lower than the 75-150 mg used for depression)<\/strong>. Full effect at 8-12 weeks. Reduces monthly migraine days by ~50% in responders. Sedation is markedly sedating<\/strong> (H1<\/sub> antagonism is strong) — always dose at night. For most patients this is a therapeutic benefit (improves disrupted sleep that perpetuates migraine), but can cause morning hangover.<\/strong> — always dose at night. Anticholinergic burden is strong<\/strong> — dry mouth, constipation, urinary hesitancy, blurred vision, memory effects. Can be dose-limiting especially in older patients.<\/strong> Contraindicated in recent MI, uncontrolled arrhythmias, QT prolongation, concurrent MAOI, narrow-angle glaucoma, severe hepatic impairment, and urinary retention \/ symptomatic BPH. Cardiac safety is the main consideration in patients over 50 — baseline ECG before starting is standard practice.<\/p>\n<\/div>\n Cotrip is an oral tablet of amitriptyline 10 \/ 25 \/ 50 \/ 75 mg<\/strong> from a WHO-GMP certified manufacturer, supplied in 30-180 tablet packs. Introduced in 1961 under the brand name Elavil<\/strong>; remains on the WHO Essential Medicines List for depression, neuropathic pain, and migraine.<\/p>\n Amitriptyline is a tertiary-amine tricyclic antidepressant (TCA)<\/strong> — one of the classic drugs of modern psychopharmacology. In contemporary clinical practice, tricyclics have largely been displaced by SSRIs for first-line depression treatment, but they remain a cornerstone of neurology and pain medicine at doses well below the antidepressant range, particularly for migraine prevention, chronic tension-type headache, and neuropathic pain.<\/p>\n The exact mechanism of tricyclic antidepressants in migraine prophylaxis is multi-modal:<\/p>\n The migraine-prevention dose (25-75 mg nightly (migraine-prevention range; lower than the 75-150 mg used for depression)) is substantially lower than the antidepressant dose (75-150 mg nightly). This is important for three reasons: (1) lower doses minimise side effects, (2) the analgesic mechanism appears to be achieved at doses insufficient for antidepressant effect, and (3) it means Cotrip can be used for migraine prevention without necessarily being effective as an antidepressant. For patients with comorbid migraine and depression<\/strong>, doses toward the higher end address both conditions simultaneously.<\/p>\n Tricyclic antidepressants are titrated from very low starting doses<\/strong> to minimise anticholinergic and sedative side effects. Patience is essential — reaching therapeutic effect usually takes 8-12 weeks.<\/p>\nWhat Is Cotrip?<\/h2>\n
How Amitriptyline Prevents Migraine<\/h2>\n
\n
\u0395\u03b3\u03ba\u03b5\u03ba\u03c1\u03b9\u03bc\u03ad\u03bd\u03b5\u03c2 \u03ba\u03b1\u03b9 \u0392\u03b1\u03c3\u03b9\u03c3\u03bc\u03ad\u03bd\u03b5\u03c2 \u03c3\u03b5 \u0391\u03c0\u03bf\u03b4\u03b5\u03af\u03be\u03b5\u03b9\u03c2 \u03a7\u03c1\u03ae\u03c3\u03b5\u03b9\u03c2<\/h2>\n
\n
Cotrip Dosage for Migraine Prevention<\/h2>\n