Midodrine | Pharmacology Mentor

Generic Name

Midodrine

Mechanism

Prodrug → hydrolyzed in the liver to clonidine (active metabolite).
Selective α₁‑adrenergic stimulation on vascular smooth muscle → vasoconstriction.
Increases afterload and systolic/diastolic BP, reducing orthostatic symptoms.
No direct β‑blocking or central depressant effects; however, central α₁‑agonism contributes to the modest rise in heart rate.

Pharmacokinetics

Absorption: Oral bioavailability ~70 % (first‑pass hepatic metabolism).
Onset: Peak plasma ~4–5 h after dose; clinical effect starts 2–3 h.
Half‑life: 1.5–3 h for active metabolite; total duration of action ~4–6 h.
Metabolism: Primarily hepatic via aldehyde oxidase and xanthine oxidase.
Excretion: Renally → ~40 % unchanged; remaining metabolites renal and fecal.
Food interaction: High‑fat meals delay absorption; avoid food 2 h before dosing.

Indications

Primary: Symptomatic orthostatic (postural) hypotension in adults.
Secondary
Neurogenic orthostatic hypotension secondary to Parkinson’s disease, multiple system atrophy, or autonomic failure.
Hypotension associated with chronic hemodialysis (in select centers).
Post‑operatively when invasive BP support is contraindicated.

Contraindications

Contraindications
Severe atherosclerotic peripheral arterial disease.
Uncontrolled systemic hypertension (>200/110 mm Hg).
Suspected or established intracranial hemorrhage (risk of worsening).
Acute or chronic renal failure (eGFR <30 mL/min/1.73 m²) – use caution.
Warnings
Carotid bruits: elevate BP may precipitate transient ischemic attacks.
Heart failure: raise afterload, worsening congestion; use with caution.
Pregnancy: Category C; avoid if possible.
Concomitant MAO inhibitors → potential hypertensive crisis.

Dosing

Initiation: 2.5 mg PO QID × 2–3 days (≈20 mg/day).
Titrate: Increase by 2.5 mg QID at 2–3 day intervals based on orthostatic BP response.
Target: Max 20 mg QID (≈80 mg/day); never exceed 2.5 mg QID if adverse events present.
Timing: Administer 1–2 h before standing activities.
Dose‑reduction: Reduce frequency if supine hypertension develops.

Adverse Effects

Common
Piloerection (gooseflesh).
Facial flushing, itching, pruritus.
Supine hypertension (↑ systolic > 20 mm Hg).
Headache, dizziness, nausea.
Serious
Severe hypertensive crisis (rare).
Angioedema (rare).
Persistent supine hypertension leading to end‑organ damage.
Heart failure exacerbation in predisposed patients.
Monitoring for
Pulse rate changes; tachycardia >100 bpm warrants dose adjustment.
Supine vs upright BP differences > 20 mm Hg.

Monitoring

Blood Pressure
Supine BP at 2 h intervals for first 10–12 h after initiation.
Orthostatic BP (standing after 3 min) at each dose adjustment.
Heart Rate
Monitor for sinus tachycardia >100 bpm.
Renal Function
Serum creatinine eGFR; reevaluate if ≥30 % decline.
Adherence & Symptoms
Document orthostatic dizziness, edema, or palpitations.

Clinical Pearls

“Double‑check the timing.” Midodrine peaks 4–5 h; if patients report symptoms just before standing, they may have missed the dose—reinforce adherence to the 1‑2 h pre‑standing schedule.
Supine hypertension is predictable. Use a sliding scale: a rise of >20 mm Hg supine → reduce night‑time dosing or add a vasodilator (e.g., hydralazine) for nighttime BP control.
Avoid meals high in fat. Fats delay absorption, so patients should take midodrine on an empty stomach or wait at least 2 h.
Titrate cautiously in renal impairment. Because metabolism is hepatic but elimination is renal, in CKD (eGFR 30–60 mL/min/1.73 m²) start at lower doses (1.25 mg QID) and titrate slowly.
Consider alternate routes if GI absorption is poor. Though no IV formulation exists, switching to norepinephrine infusion might be necessary if oral bioavailability is compromised (e.g., severe GI disease).

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