Excedrin
Excedrin
Generic Name
Excedrin
Mechanism
- Acetylsalicylic acid (ASA)
- Irreversible inhibitor of cyclooxygenase‑1 (COX‑1) and, at higher concentrations, COX‑2.
- Reduces prostaglandin synthesis, diminishing vasodilation, platelet aggregation, and nociceptive signaling.
- Acetaminophen
- Acts centrally by inhibiting COX‑3 and modulating serotonergic pathways.
- Provides antipyretic and analgesic effects without significant peripheral anti‑inflammatory activity.
- Caffeine
- A CNS stimulant and adenosine receptor antagonist.
- Enhances pain threshold, promotes vasoconstriction in cerebral vessels, and potentiates the analgesic efficacy of ASA and acetaminophen.
The synergistic effect of these agents results in rapid headache relief, with onset typically 5–15 minutes post‑dose.
Pharmacokinetics
| Parameter | Value / Notes |
| Absorption | Rapid; peak plasma concentrations in 30–60 min for ASA, 45–60 min for acetaminophen. |
| Distribution | Widely distributed with significant protein binding (~99 % for ASA, ~20–25 % for acetaminophen). |
| Metabolism |
• ASA → salicylic acid → glucuronidation and sulfation.
• Acetaminophen → N‑acetyl‑p‑aminophenol and N‑acetyl‑p‑aminophenol glucuronide. |
| Elimination | Renal excretion; half‑lives: ASA ~2 h, acetaminophen ~2–3 h. |
| Drug Interactions | CYP2E1 inhibitors/inducers affect acetaminophen metabolism; NSAIDs increase ASA plasma levels. |
Indications
- Primary headache disorders
- Acute migraine (with or without aura).
- Cluster headaches (in combination with NSAIDs).
- Tension‑type headache.
- Post‑operative or procedural pain
- Adjunctive analgesia for mild‑to‑moderate discomfort.
- OTC analgesic for general pain
- Includes menstrual cramps when combined with acetaminophen (Excedrin Fast‑Relief).
Contraindications
- Absolute contraindications
- Known ASA or salicylate hypersensitivity.
- Active peptic ulcer disease or significant GI bleeding.
- Hemorrhagic disorders; concurrent anticoagulant or antiplatelet therapy.
- Severe hepatic insufficiency (acetaminophen toxicity risk).
- Severe renal failure (ASA accumulation).
- Children and teenagers with viral infections (Reye syndrome risk).
- Pregnant women in the third trimester (ASA increased risk of premature closure of ductus arteriosus).
- Relative cautions
- Concomitant use of other caffeine sources (tea, cola, energy drinks).
- Chronic alcohol use increases bleeding and hepatotoxic risk.
- Elderly: higher sensitivity to caffeine‑induced tremor and hypertension.
Dosing
| Form | Typical Adult Dose | Frequency | Maximum Daily Dose |
| *Excedrin Extra Strength* (ASA 250 mg / acetaminophen 500 mg / caffeine 65 mg) | 2 tablets (500 mg ASA, 1000 mg acetaminophen, 130 mg caffeine) | Every 4–6 h as needed | 6 tablets/day (3000 mg ASA, 6000 mg acetaminophen, 780 mg caffeine) |
| *Excedrin® Migrane* (ASI‑AC) | 2 tablets | Every 4–6 h with pain | 6 tablets/day |
| *Excedrin® N* (no caffeine) | 2 tablets | Every 4–6 h | 6 tablets/day |
Note:
• Start with the lowest effective dose.
• For patients > 65 y or with renal/hepatic compromise, consider 1 tablet per dose and limit to 3–4 tablets/day.
• Re‑dose only after 30 min if pain persists; avoid exceeding 24 h.
Adverse Effects
- Common
- Nausea, dyspepsia, epigastric discomfort (ASA).
- Dysuria, abdominal pain (acetaminophen).
- Palpitations, tremor, insomnia, jitteriness (caffeine).
- Serious
- *GI* bleeding or ulceration—especially with chronic use or high doses.
- *Hepatotoxicity*—acetaminophen overdose or in hepatic impairment.
- *Cerebral hemorrhage*—long‑term high‑dose ASA.
- *Allergic reactions*—urticaria, rash, anaphylaxis (rare).
- *Caffeine toxicity*—seizures, arrhythmia in susceptible individuals.
- *Reye syndrome*—in children/teenagers with viral illnesses.
Monitoring
| Parameter | Frequency | Rationale |
| Blood pressure | Baseline; repeat if ≥ 120/80 mm Hg | Caffeine‑induced hypertension. |
| Liver function tests (ALT, AST) | Before > 3 days of consistent use in at‑risk patients | Detect early hepatotoxicity. |
| Renal function (Serum creatinine) | Prior to high‑dose or prolonged therapy | ASA clearance. |
| Signs of GI bleeding | Patient‑reported (hematochezia, melena) | Early detection of NSAID‑related ulceration. |
| Pulse and ECG | In patients with arrhythmia risk | Caffeine effects. |
Clinical Pearls
- Caffeine as a Pharmacologic Booster:
*Caffeine* amplifies analgesic effects by a 30–50 % reduction in requisite ASA/acetaminophen dose, allowing lower overall exposure to each active ingredient.
• Avoid OTC “Duplicate” Caffeine:
Patients frequently ingest multiple caffeine‑containing products (tea, soda, energy drinks). Document total daily caffeine intake; > 400 mg can precipitate neurotoxicity.
• Teratogenic Window:
ASA is linked to – particularly within the 12–20 weeks gestational window – premature ductus arteriosus closure. Use *Excedrin N* (no caffeine and no ASA) in early pregnancy, if analgesia is required.
• Pediatric Use:
*Excedrin* is contraindicated in children ≤ 12 y; instead, use acetaminophen or ibuprofen alone. ReBeast migrating to Reye syndrome; all children with viral infections should avoid ASA.
• Drug–Drug Interactions:
Concomitant ASA‑based NSAIDs increases bleeding risk; patients on warfarin must monitor INR. Acetaminophen’s CYP2E1 metabolism interacts with alcohol, leading to hepatotoxicity; caution during binge drinking.
• Rapid Onset vs. Relapse:
The first 4–6 h represents the period of maximum benefit. If headache recurs after initial response, give an additional dose 30 min later; if no relief, consider triptan therapy or triptan‑caffeine combos rather than repeated Excedrin.
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