CALCIUM CHANNEL BLOCKERS

CALCIUM CHANNEL BLOCKERS

1. BASIC PHYSIOLOGY & MECHANISM

Calcium channels in cardiovascular system

L-type Ca²⁺ channels → predominant in:

Cardiac myocytes
SA node & AV node
Vascular smooth muscle

Function

Ca²⁺ influx →
→ myocardial contraction (inotropy)
→ nodal conduction (chronotropy, dromotropy)
→ vascular tone

Mechanism of Action

CCBs block L-type Ca²⁺ channels → ↓ intracellular Ca²⁺

Effects:

Site	Effect
Heart	↓ contractility (negative inotropy)
SA node	↓ HR (negative chronotropy)
AV node	↓ conduction (negative dromotropy)
Vessels	Vasodilation (↓ SVR)

2. CLASSIFICATION

Non-Dihydropyridines (Cardioselective)

Verapamil
Diltiazem

More effect on heart

Dihydropyridines (Vasoselective)

Amlodipine
Nifedipine
Nicardipine
Clevidipine
Nimodipine

More effect on vascular smooth muscle

3. COMPARISON

Feature	Non-DHP	DHP
HR	↓↓↓	↑ (reflex tachycardia)
Contractility	↓↓↓	Minimal
AV conduction	↓↓↓	No effect
Vasodilation	Moderate	Marked
ICU use	Arrhythmia control	Hypertensive emergencies

4. ICU INDICATIONS

A. Tachyarrhythmias

AF with RVR
SVT (rate control)

Drug of choice:Diltiazem (preferred),Verapamil

B. Hypertensive emergencies

Neurocritical care (ICH, SAH)
Aortic dissection (with β-blocker)
Postoperative hypertension

Preferred IV agents:Nicardipine,Clevidipine

C. Subarachnoid hemorrhage (SAH)

Prevent vasospasm

DOC:Nimodipine

Improves neurological outcome (NOT mortality)

D. Coronary vasospasm (Prinzmetal angina)

DHP preferred

E. Pulmonary hypertension (selected patients)

Only vasoreactive group

F. NOT preferred in:

Cardiogenic shock
Severe LV dysfunction

5. DOSING IN ICU

Diltiazem (AF with RVR)

Bolus: 0.25 mg/kg IV
Repeat: 0.35 mg/kg
Infusion: 5–15 mg/hr

Verapamil

Bolus: 5–10 mg IV slow
Higher risk of hypotension

Nicardipine

Start: 5 mg/hr IV
Titrate: +2.5 mg/hr every 5–15 min
Max: 15 mg/hr

Clevidipine

Start: 1–2 mg/hr
Rapid titration (every 90 sec)
Max: 16–32 mg/hr

Lipid emulsion (like propofol)

Nimodipine (SAH)

60 mg PO/NG every 4 hours
If hypotension → reduce dose

6. ADVERSE EFFECTS

Cardiovascular

Hypotension
Bradycardia
AV block
Worsening heart failure

Others

Peripheral edema
Constipation (verapamil)
Flushing, headache

Severe toxicity

→ CCB overdose:

Shock
Bradycardia
Hyperglycemia (key differentiator from β-blocker toxicity)

7. CCB TOXICITY

Pathophysiology

↓ insulin release → hyperglycemia
↓ cardiac contractility
Vasodilation

MANAGEMENT

Stepwise approach:

IV Calcium

Calcium gluconate / chloride

High-dose insulin euglycemia therapy (HIET)

Improves myocardial metabolism

Vasopressors-Noradrenaline,Adrenaline

Lipid emulsion therapy
Pacing (if bradycardia)
ECMO (refractory shock)

8. DRUG INTERACTIONS

Dangerous combinations

CCB + β-blocker → severe bradycardia/heart block
With digoxin → ↑ digoxin levels
CYP3A4 inhibitors → ↑ toxicity

9. SPECIAL ICU PEARLS

✔ Clevidipine preferred when:

Need rapid titration
Short half-life needed

✔ Nicardipine preferred in:

Neuro ICU (stable BP control)

✔ Diltiazem vs β-blocker:

Use Diltiazem if:

Asthma/COPD
β-blocker contraindicated

✔ Nimodipine:

Give even if normotensive SAH
Avoid IV (risk of collapse)