Neostigmine basics

What it is (core concept)

Neostigmine is an acetylcholinesterase inhibitor used to reverse non-depolarising neuromuscular blockade (e.g., rocuronium, vecuronium, atracurium).
It increases acetylcholine at the neuromuscular junction so acetylcholine can outcompete the relaxant at nicotinic receptors.
It also increases acetylcholine at muscarinic receptors (heart, airways, gut) → unwanted side effects unless an antimuscarinic is co-administered.

When to use it (typical scenarios)

At the end of surgery when you want to reverse residual paralysis from a non-depolarising muscle relaxant.
Most appropriate when there is evidence of partial recovery (e.g., TOF count 4 with fade, or TOF ratio still <0.9).
If there is minimal/no spontaneous recovery (deep block), neostigmine may be ineffective or slow; consider waiting for recovery or using sugammadex for aminosteroid relaxants if appropriate and available.

When NOT to rely on neostigmine

Deep neuromuscular block (e.g., post-tetanic count only, or TOF count 0–1): neostigmine may not achieve timely/complete reversal.
As a substitute for neuromuscular monitoring: always use objective monitoring where possible.
To treat airway obstruction or hypoventilation in PACU without confirming residual neuromuscular blockade—assess and manage ABCs first.

Dosing (practical starter approach)

Common adult dose range: 0.02–0.07 mg/kg IV (i.e., 20–70 micrograms/kg), guided by depth of block and local policy.
Typical ‘routine’ dose often used for moderate residual block: ~0.04–0.05 mg/kg IV (check departmental practice).
Maximum commonly quoted dose: 5 mg total (beyond this, benefit plateaus and side effects increase).
Give with an antimuscarinic: glycopyrrolate (commonly) or atropine, to reduce bradycardia/bronchospasm/secretions.

Antimuscarinic pairing (why and how)

Neostigmine increases muscarinic activity → bradycardia, bronchospasm, salivation, increased gut motility.
Glycopyrrolate is commonly paired (less CNS penetration; tends to give smoother heart rate control).
Many departments use a fixed ratio mixture or give separately; ensure both drugs are drawn up and administered together (or antimuscarinic just before) to avoid marked bradycardia.

Onset, peak, and what to expect

Onset is not immediate; expect several minutes for meaningful improvement (often ~5–10 minutes depending on depth of block).
Reversal is faster and more reliable when some spontaneous recovery is already present.
Do not extubate purely because you have given neostigmine—confirm recovery clinically and (ideally) with objective TOF ratio ≥0.9.

Monitoring and extubation readiness

Use quantitative neuromuscular monitoring if available (acceleromyography/electromyography). Aim for TOF ratio ≥0.9 before extubation.
Clinical tests (head lift, hand grip) are unreliable for excluding residual paralysis—use them as supportive, not definitive, signs.
Check ventilation (tidal volumes, ETCO2), airway reflexes, and overall anaesthetic depth/analgesia before extubation.

Side effects (what you might see)

Cardiac: bradycardia, conduction block, rarely severe bradyarrhythmia—risk higher if antimuscarinic omitted or delayed.
Respiratory: bronchospasm, increased secretions (important in reactive airways).
GI/GU: increased gut motility, nausea, abdominal cramping; may increase bladder tone.
Paradoxical weakness can occur if given when already fully recovered (cholinergic excess at the neuromuscular junction).

Practical steps for a safe ‘first time’

Confirm which relaxant was used and when the last dose was given; check TOF/neuromuscular monitor early (don’t wait until drapes are off).
Decide if neostigmine is appropriate based on depth of block; if deep block, plan to wait or use an alternative strategy per local policy.
Draw up neostigmine and antimuscarinic, label clearly, and have resuscitation drugs available (e.g., atropine) in case of bradycardia.
After giving reversal, allow time, reassess TOF ratio, ventilation, and clinical signs; only then proceed to extubation.

What does neostigmine reverse?

– Reverses non-depolarising neuromuscular blockers (e.g., rocuronium, atracurium). – It does NOT reverse depolarising block from suxamethonium.

Why must I give an antimuscarinic with it?

– Neostigmine increases acetylcholine everywhere. – Muscarinic effects include bradycardia, bronchospasm, secretions. – Glycopyrrolate or atropine reduces these risks.

When is neostigmine likely to work best?

– When there is partial spontaneous recovery. – Ideally: TOF count 4 with fade (or TOF ratio still <0.9).

When might neostigmine be a poor choice?

– Deep block (TOF 0–1): reversal may be slow/incomplete. – If rapid, reliable reversal is needed and sugammadex is appropriate/available (for aminosteroid relaxants).

How do I judge if reversal is complete?

– Best: quantitative TOF ratio ≥0.9. – Also assess: adequate ventilation, airway reflexes, alertness (as appropriate), and no signs of weakness.

How long should I wait after giving it?

– Allow several minutes; commonly ~5–10 minutes depending on depth of block. – Re-check TOF ratio and ventilation before extubation.

What are the common side effects to watch for on the monitor?

– Bradycardia (especially if antimuscarinic omitted/delayed). – Increased secretions/bronchospasm. – Nausea or abdominal cramping post-op.

Can I give neostigmine if the patient is already fully reversed?

– Avoid routine ‘top-up’ dosing if TOF ratio is already ≥0.9. – Excess acetylcholine can cause paradoxical weakness and more side effects.

What should I do if the patient is still weak in PACU?

– Treat as ABC problem first: airway support, oxygen, ventilation. – Check neuromuscular function (quantitative TOF if available). – Consider residual block, opioid effect, sedation, hypothermia, metabolic issues; escalate early.