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  • Educational Only: Not for clinical decision-making.
  • Verify Information: Always consult protocols and authoritative sources.
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Bedside Snapshot
  • Core dose: 5 mg/hr IV infusion; titrate by 2.5 mg/hr every 5–15 min to max 15 mg/hr; once at goal, may reduce to maintenance 3 mg/hr
  • Onset/duration: Onset 5–15 min; offset 30–60 min after stopping; half-life ~14 hr (but clinical effect shorter due to redistribution)
  • Key danger: Reflex tachycardia, hypotension, peripheral edema; avoid in severe aortic stenosis; extravasation can cause local irritation
  • Special: Dihydropyridine CCB; cerebral-selective vasodilation makes it preferred for hypertensive emergencies with stroke/ICH; titratable and predictable BP response
Brand & Generic Names
  • Generic Name: Nicardipine
  • Brand Names: Cardene, Cardene IV, Cardene SR
Medication Class

Dihydropyridine calcium channel blocker (CCB) - Predominantly arteriolar vasodilator with minimal direct myocardial depression at standard doses.

Pharmacology

Mechanism of Action:

  • Blocks L-type voltage-gated calcium channels in vascular smooth muscle
  • Produces preferential arteriolar vasodilation → decreases systemic vascular resistance (afterload) and blood pressure
  • Causes coronary vasodilation and can improve coronary blood flow
  • Minimal direct negative inotropy at usual doses, but reflex sympathetic activation may lead to tachycardia

Pharmacokinetics:

IV (Cardene IV):

  • Route/Absorption: 100% systemic availability by IV infusion (no bolus recommended for adults)
  • Onset: BP reduction within minutes after initiation
  • Time to near-steady effect: ~45 minutes at a fixed rate
  • Offset: About 50% loss of effect ~30 minutes after stopping the infusion; most effect gone by 30–60 minutes
  • Distribution: Protein binding >95%; Large apparent volume of distribution (~8 L/kg)
  • Metabolism: Extensive hepatic metabolism via CYP3A4 (also 2D6, 2C8, 2C19) to inactive metabolites
  • Elimination: Terminal half-life ~8–14 hours (clinical effect much shorter); Metabolites excreted ~50–60% in urine, remainder in feces

Oral (IR/SR):

  • Bioavailability: ~35% (first-pass metabolism)
  • Tmax: ~0.5–2 hours
  • Effective half-life: ~2–4 hours for BP effect; terminal ~8–9 hours
Indications

Educational only – follow current guidelines, institutional policies, and prescriber orders.

Primary IV indications (short-term use):

  • Short-term treatment of hypertension when oral therapy is not feasible (FDA-labeled indication)
  • Hypertensive emergency, especially:
    • Acute ischemic stroke when BP lowering is indicated (e.g., pre/post thrombolysis or thrombectomy)
    • Intracerebral hemorrhage (ICH) and subarachnoid hemorrhage (SAH) where tight BP control is important
    • Peri-operative hypertension and post-operative hypertension

Oral indications:

  • Chronic hypertension
  • Chronic stable angina
Conditions Treated
  • Hypertensive emergency/elevated BP requiring IV therapy
  • Acute ischemic stroke with BP above treatment thresholds (especially around thrombolysis or thrombectomy)
  • Intracerebral hemorrhage and subarachnoid hemorrhage needing controlled BP reduction
  • Peri-/post-operative hypertension
  • Chronic hypertension and stable angina (oral formulations)
Dosing & Administration

Dosing below is for education only. Always follow local protocols, prescriber orders, and institutional policies.

Available Forms:

  • IV concentrate: 2.5 mg/mL (e.g., 10 mL vials/ampules) – must be diluted
  • Premixed IV bags:
    • 20 mg in 200 mL (0.1 mg/mL)
    • 40 mg in 200 mL (0.2 mg/mL)
  • Oral formulations:
    • Immediate-release capsules: 20 mg, 30 mg
    • Sustained-release (SR): 30 mg, 60 mg

IV Nicardipine Dosing – Hypertensive Emergency (Adult):

Continuous IV infusion:

  • Initial rate: 5 mg/hr
  • Titration: Increase by 2.5 mg/hr every 5–15 minutes until target BP achieved
  • Usual maintenance range: 3–15 mg/hr
  • Maximum: 15 mg/hr

Approximate oral → IV conversion:

  • 20 mg PO q8h ≈ 0.5 mg/hr IV
  • 30 mg PO q8h ≈ 1.2 mg/hr IV
  • 40 mg PO q8h ≈ 2.2 mg/hr IV

Infusion rate examples (0.1 mg/mL premix):

Dose (mg/hr) Infusion Rate (mL/hr)
5 mg/hr 50 mL/hr
7.5 mg/hr 75 mL/hr
10 mg/hr 100 mL/hr
15 mg/hr (max) 150 mL/hr

Special Populations (general principles):

  • Renal impairment: Higher exposure; start at lower end, titrate slowly, monitor BP and renal function
  • Hepatic impairment: Decreased clearance; use lower starting dose, slower titration
  • Elderly: "Start low, go slow"

Oral Dosing (for completeness):

  • IR capsules – hypertension: 20 mg PO q8h; titrate every 3 days. Usual total daily dose 60–120 mg (e.g., 20–40 mg q8h)
  • SR – hypertension: 30 mg PO BID; titrate to 30–60 mg BID
Contraindications

Absolute Contraindications:

  • Advanced aortic stenosis – Afterload reduction can critically impair coronary perfusion and precipitate collapse
  • Known hypersensitivity to nicardipine or formulation components

Precautions:

  • Coronary artery disease / angina: Reflex tachycardia and reduced diastolic pressure can worsen angina
  • Heart failure / reduced EF: Generally tolerated but may worsen HF in severe LV dysfunction or when combined with beta-blockers; titrate cautiously
  • Hepatic impairment: Reduced metabolism → elevated levels; lower doses and slower titration required
  • Renal impairment: Increased exposure; cautious titration and close monitoring
  • Pregnancy: Used in some protocols for severe preeclampsia/eclampsia, but data remain limited; risk–benefit to be determined by obstetrics team
  • Peripheral line use: Risk of phlebitis, thrombosis, and extravasation; use large forearm vein or central line when possible, and rotate peripheral sites regularly
Critical Warning: In patients with advanced aortic stenosis, afterload reduction can critically impair coronary perfusion and precipitate cardiovascular collapse. This is an absolute contraindication.
Adverse Effects

Common:

  • Headache
  • Flushing
  • Dizziness
  • Hypotension
  • Tachycardia / palpitations
  • Nausea / vomiting
  • Peripheral edema (more with chronic oral therapy)
  • Infusion site reactions: pain, erythema, phlebitis

Serious / Less Common:

  • Severe hypotension → syncope, organ ischemia
  • Worsening angina or myocardial infarction in CAD
  • Heart failure exacerbation in severe LV dysfunction
  • Arrhythmias or AV block (rare)
  • Thrombophlebitis / venous thrombosis at infusion site
  • Rare hypersensitivity reactions; rare liver enzyme elevation
Drug Interactions

Nicardipine is a CYP3A4 substrate and moderate inhibitor, and also interacts with CYP2D6, 2C8, 2C19 and P-gp.

Immunosuppressants:

  • Cyclosporine: Nicardipine increases cyclosporine levels; monitor levels closely and reduce cyclosporine dose as needed
  • Tacrolimus: Similar considerations; monitor troughs and adjust therapy

CYP3A4 / P-gp Substrates and Modifiers:

  • Nicardipine may increase concentrations of CYP3A4 substrates (e.g., some statins and other narrow-therapeutic-index drugs)
  • Strong CYP3A4 inducers (e.g., rifampin, carbamazepine) may reduce nicardipine levels and blunt BP effect

Cimetidine:

  • Cimetidine can increase nicardipine plasma concentrations; monitor for hypotension and consider dose reduction

Beta-Blockers:

  • Combination is common but in patients with HFrEF or severe LV dysfunction, combined effects on contractility and afterload reduction may worsen HF; approach titration cautiously

Other Antihypertensives / Vasodilators:

  • Additive BP lowering with nitrates, other CCBs, ACEi/ARB, alpha-blockers, etc.; monitor BP and adjust doses accordingly
Monitoring

Clinical Monitoring:

  • Blood pressure: Every 5–15 minutes during initiation and titration; then at regular frequent intervals (often every 15–30 minutes). In high-risk patients, use invasive arterial monitoring when appropriate
  • Heart rate and rhythm: Monitor for tachycardia, bradycardia, arrhythmias
  • Symptoms: Assess for hypotension, chest pain, dyspnea, neurologic status changes
  • Infusion site: Monitor for erythema, pain, palpable cord, swelling (phlebitis or extravasation)

Laboratory / Additional Monitoring:

  • Renal function: SCr, BUN, urine output (important in hypertensive emergencies and stroke)
  • Liver function tests: With prolonged therapy
  • Drug levels where relevant: Cyclosporine, tacrolimus when co-administered
  • In neuro patients: Coordinate with neurology/neurosurgery on BP goals vs cerebral perfusion pressure
IV Compatibility & Administration: Compatible diluents for 0.1 mg/mL solution include 0.9% NaCl, 0.45% NaCl, D5W, D5W/0.45% NaCl, D5W/0.9% NaCl, D5W with KCl. Incompatible: Lactated Ringer's, Sodium bicarbonate solutions. Do not mix with other medications in the same line or bag. Prefer central line or large-bore forearm peripheral vein.
Clinical Pearls
Neuro drip of choice: Nicardipine's rapid onset, titratability, and reasonably quick offset make it a go-to infusion for acute ischemic stroke, ICH, and SAH where tight BP control is essential.
Volume load matters: With a 0.1 mg/mL premix, high rates (e.g., 15 mg/hr = 150 mL/hr) can contribute significant volume—be mindful in HF, renal failure, or neuro patients where fluid balance matters.
Reflex tachycardia: If BP improves but HR rises significantly (especially with chest pain), consider reducing the rate and ensuring appropriate beta-blockade as directed by the prescriber.
Check the line first: If BP "stops responding" and the rate is creeping up, inspect the IV site for infiltration or phlebitis before chasing the number with more drug.
BP goals in stroke are disease-specific: Ischemic stroke often tolerates higher BP unless tPA or endovascular therapy is planned, whereas ICH/SAH usually have stricter targets; follow current stroke/ICH guidelines and your local protocol.
MAP reduction rule of thumb: In most hypertensive emergencies, avoid dropping BP by more than about 25% of MAP in the first hour, then gradually lower over the next 24–48 hours, unless a specific condition (e.g., aortic dissection, some pregnancy-related emergencies) dictates otherwise.
References
  • 1. Alley, W. D., & Schick, M. A. (2023). Hypertensive emergency. In StatPearls. StatPearls Publishing. https://www.ncbi.nlm.nih.gov/books/NBK470371/
  • 2. Chiesi USA, Inc. (2018). Cardene I.V. (nicardipine hydrochloride) premixed injection [Prescribing information]. U.S. Food and Drug Administration.
  • 3. DrugBank Online. (n.d.). Nicardipine (DB00622). In DrugBank.
  • 4. Drugs.com. (2025, August 7). Nicardipine: Package insert / prescribing information. https://www.drugs.com/pro/nicardipine.html
  • 5. EBM Consult, LLC. (n.d.). Nicardipine (Cardene): Drug monograph. EBM Consult.
  • 6. Medscape. (n.d.). Cardene, Cardene IV (nicardipine) – dosing, indications, interactions, adverse effects, and more [Drug monograph]. Medscape Reference.
  • 7. Miller, J., McNaughton, C., Joyce, K., Binz, S., & Levy, P. (2020). Hypertension management in emergency departments. American Journal of Hypertension, 33(10), 927–934. https://doi.org/10.1093/ajh/hpaa068
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