Video: Nondepolarizing (Competitive) Neuromuscular Blockers: Mechanism of Action

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7.3 : Nondepolarizing (Competitive) Neuromuscular Blockers: Mechanism of Action

Nondepolarizing neuromuscular blockers bind to the nAChR on the motor end plate to prevent membrane depolarization and muscular contractions.

Most nondepolarizing blockers resemble the endogenous ligand ACh, and so they competitively bind to the nAChR. However, unlike ACh, their bulky structure prevents the conformational changes necessary for receptor activation.

As a result, ion channels remain closed, preventing muscle end plate depolarization. This leads to neuromuscular transmission blockade and muscle relaxation.

The induced effect can be reversed by administering AChE enzyme inhibitors. They block AChE, and inhibit degradation of ACh elevating its concentration.

However, when the nondepolarizing blockers are administered in large doses, they block the sodium channel pore as well. This results in an intense neuromuscular blockade, which is difficult to reverse using AChE inhibitors.

Nondepolarizing neuromuscular blockers induce paralysis by competitively blocking nicotinic acetylcholine receptors at the muscle end plate. Examples include pancuronium, mivacurium, vecuronium, and rocuronium. These quaternary ammonium derivatives are administered intravenously, are poorly absorbed, and are excreted via the kidneys.

Competitive antagonists prevent acetylcholine from binding to its receptor, inhibiting membrane depolarization. Without conformational changes or intrinsic activity, ion channels remain closed, blocking neuromuscular transmission and causing muscle relaxation.

The antagonistic effect can be overcome by increasing acetylcholine concentration using acetylcholinesterase (AChE) inhibitors. Elevated acetylcholine displaces the blocker, restoring neuromuscular transmission. However, the blockers can directly block Na⁺ channels at high doses, resulting in irreversible neuromuscular blockade unresponsive to AChE inhibitors.

Tags

Nondepolarizing Neuromuscular Blockers Mechanism Of Action Nicotinic Acetylcholine Receptors Pancuronium Mivacurium Vecuronium Rocuronium Competitive Antagonists Membrane Depolarization Neuromuscular Transmission Acetylcholinesterase Inhibitors Muscle Relaxation Na Channels Irreversible Neuromuscular Blockade

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