Flexeril
Flexeril
Generic Name
Flexeril
Mechanism
Flexeril (*cyclobenzaprine*) acts centrally as a short‑acting muscle relaxant. It inhibits the transmission of nerve impulses in the brainstem and spinal cord, producing a relaxation of reflex muscle tone. This is achieved by blocking excitatory neurotransmitters (especially glutamate) and potentiating inhibitory pathways (GABAergic). The result is a reduction of voluntary and involuntary muscle contraction without direct effects on muscle fibers.
Pharmacokinetics
- Absorption – Rapid oral absorption; peak plasma concentration in 1–2 h.
- Distribution – Widely distributed, high protein binding (~92 %).
- Metabolism – Hepatic metabolism via CYP2D6 to hydroxylated metabolites.
- Elimination – Renally excreted (≈80 % unchanged); half‑life 2.6–4.0 h; prolonged in hepatic impairment.
- Drug–drug interactions – Inhibits or is inhibited by CYP2D6 substrates (e.g., fluoxetine, paroxetine).
Indications
- Acute neuromuscular spasm associated with musculoskeletal disorders
- Post‑operative or pre‑operative muscle spasm relief (≤ 3 weeks use)
- Adjunctive therapy for chronic low‑back pain or cervical spine pain when combined with physical therapy
Contraindications
- Hypersensitivity to cyclobenzaprine or phenylpiperazine moiety
- Severe hepatic or renal impairment (dose adjustment required)
- Pregnancy – Category C; use only if benefits outweigh risks
- Breastfeeding – excreted in milk; consider safe alternatives
- Concomitant MAOIs – risk of serotonin syndrome or hypertensive crisis
- Severe cardiac conduction disease – may prolong QT interval
- Geriatric patients – increased sensitivity to CNS depression; start at lowest dose
Dosing
| Condition | Dose | Titration | Max Daily Dose | Duration |
| Adults | 5 mg PO q8h | Increase by 5 mg/day as needed | 30 mg/day | ≤ 3 weeks |
| Elderly | 2.5 mg PO q8h | ↑1 mg increments | As above | Same limitation |
| Pediatric (≥ 12 yr) | Start at 2–5 mg PO q8h | Titrate to 10 mg/day | 30 mg/day | ≤ 2 weeks |
• Take with food to reduce GI upset.
• Taper rapidly if used > 3 weeks to avoid withdrawal.
Adverse Effects
- Common: drowsiness, dry mouth, dizziness, constipation, blurred vision
- Serious: increased seizure risk (especially in epilepsy), marked hypotension, arrhythmias, serotonin syndrome (with serotonergic agents)
Monitoring
- Blood pressure and heart rate on initiation and after dose adjustments
- Mental status for sedation or agitation
- Liver function tests if long‑term use or known hepatic disease
- Pregnancy test in women of childbearing potential
- Kidney function if renally impaired
Clinical Pearls
- Short‑term use only: *Flexeril* is intended for < 3 weeks; chronic pain should rely on multimodal therapy (NSAIDs, physical therapy, CBT).
- Avoid in substance‑misuse: Its benzodiazepine‑like effects can lead to misuse; screen patients with addiction history.
- Taper, don’t stop: Abrupt discontinuation may provoke rebound spasm or withdrawal; taper 5 mg every 3–5 days.
- CYP2D6 genotyping: Poor metabolizers may experience prolonged drug levels, increasing CNS depression.
- Combining with other CNS depressants (alcohol, benzodiazepines, opioids) → additive sedation; use caution and dose reduction.
- Swelling in limbs: If severe edema develops, consider fluid restriction or diuretic introduction as cyclobenzaprine may worsen fluid retention.
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• *This drug card is intended for educational purposes. Always refer to the latest prescribing information and institutional guidelines before clinical use.*