Choice of Neuromuscular Blocking Drug

The choice of NMBD is influenced by its speed of onset, duration of action, route of elimination, and associated side effects, such as drug-induced changes in systemic arterial blood pressure, heart rate, or both. Rapid onset and brief duration of skeletal muscle paralysis, characteristic of SCh, are useful when tracheal intubation is the reason for administering an NMBD. Because of its rapid onset time, rocuronium is often used to facilitate tracheal intubation, but its duration of action is much longer than that of SCh. However, an approved indication for sugammadex is reversal of a profound neuromuscular blockade specifically from rocuronium or vecuronium. For example, if rocuronium were given to facilitate endotracheal intubation, but the trachea could not be intubated, sugammadex could reverse a profound neuromuscular blockade. Although SCh can be given intermittently, nondepolarizing NMBDs are usually selected when longer periods of neuromuscular blockade (e.g., more than 15 to 45 minutes) are needed. When rapid onset of skeletal muscle paralysis is not necessary, skeletal muscle relaxation can be induced by the administration of other long- or intermediate-acting nondepolarizing NMBDs to facilitate tracheal intubation.

Hypersensitivity Reactions

The overall incidence of life-threatening anesthetic-related hypersensitivity reactions ranges between 1/10,000 and 1/20,000 procedures and varies widely between countries. Although antibiotics are likely the most common cause, NMBDs are the triggering drugs in 11% to 35% of these reactions. Rocuronium and SCh are the most common offenders. Even though it does not release histamine, rocuronium was identified as producing an increased risk for hypersensitivity reactions in France and Norway, with no confirmation from other countries. More recently, a follow-up study from Norway of 83 cases of anaphylaxis during general anesthesia revealed that 77% of these reactions were mediated by immunoglobulin E and 93% were associated with NMBDs, with SCh being the most common drug. In an analysis of all allergic drugs used in anesthesia at the Mayo Clinic, antibiotics were the most common cause, with NMBDs being second at 11% of the reactions. There may be cross-sensitivity among all NMBDs because of the presence of a common antigenic component, the quaternary ammonium group. Anaphylactic reactions after the first exposure to an NMBD may reflect sensitization from previous contact with cosmetics or soaps that also contain antigenic quaternary ammonium groups. Sugammadex (see the section, “Antagonism of Nondepolarizing Neuromuscular Blocking Drugs” later in this chapter) was recently approved by the Food and Drug Administration (FDA). The delay in sugammadex’s approval was partly because of hypersensitivity concerns. The conclusion was that the most common signs of occasional cases of hypersensitivity were nausea and urticaria. However, sugammadex has been approved in Europe and other countries for several years. Treatment of a life-threatening hypersensitivity reaction requires immediate therapy including cardiopulmonary resuscitation and epinephrine (see Chapter 45 for details).

Prejunctional Receptors and Release of Acetylcholine

ACh is synthesized in the motor nerve terminal, and the protein synapsin anchors the ACh vesicle to the release site of the terminal. Some of the ACh is then released, and the rest is held in reserve for response to a stimulus. Presynaptic receptors, aided by calcium, facilitate replenishment of the motor nerve terminal, which can be stimulated by SCh and neostigmine and depressed by small doses of nondepolarizing NMBDs. Inhibition of these presynaptic nAChRs explains the fade in response to high-frequency repetitive stimulation such as tetanic or even train-of-four (TOF) stimulation.

Postjunctional Receptors

Postjunctional receptors are glycoproteins consisting of five subunits ( Fig. 11.2 ). The subunits of the receptor are arranged such that a channel is formed that allows the flow of ions along a concentration gradient across cell membranes. This flow of ions is the basis of normal neuromuscular transmission. Extrajunctional receptors retain the two α-subunits but may have an altered γ- or δ-subunit by the substitution of an ε-unit.

The postjunctional nicotinic cholinergic receptor consists of five subunits (α, α, β, γ, δ) arranged to form an ion channel.

From Taylor P. Are neuromuscular blocking agents more efficacious in pairs? Anesthesiology. 1985;63:1-3, used with permission.

The two α-subunits are the binding sites for ACh and are the sites occupied by NMBDs. For example, occupation of one or both α-subunits by a nondepolarizing NMBD causes the ion channel to remain closed, and ion flow to produce depolarization cannot occur. SCh attaches to α-sites and causes the ion channel to remain open (mimics ACh), thereby resulting in prolonged depolarization. Large doses of nondepolarizing NMBDs (large molecules) may also act to occlude the channel and in this way prevent the normal flow of ions. Neuromuscular blockade secondary to occlusion of the channels is resistant to drug-enhanced antagonism with anticholinesterase drugs. The lipid environment around cholinergic receptors can be altered by drugs such as volatile anesthetics, thus changing the properties of the ion channels. This probably accounts for the augmentation of neuromuscular blockade by volatile anesthetics.

Extrajunctional Receptors

Postjunctional receptors are confined to the area of the end plate precisely opposite the prejunctional receptors, whereas extrajunctional receptors (the ε-unit is replaced by γ-subunits) are present throughout skeletal muscles. Extrajunctional receptor synthesis is normally suppressed by neural activity. Prolonged inactivity, sepsis, and denervation or trauma (burn injury) to skeletal muscles may be associated with a proliferation of extrajunctional receptors. When activated, extrajunctional receptors stay open longer and permit more ions to flow, which in part explains the exaggerated hyperkalemic response when SCh is administered to patients with denervation or burn injury. Proliferation of these receptors also accounts for the resistance or tolerance to nondepolarizing NMBDs, as can occur with burns or prolonged (several days) immobilization (also see discussion under the section, “Hyperkalemia” ).

Characteristics of Blockade

SCh mimics the action of ACh and produces a sustained depolarization of the postjunctional membrane. Skeletal muscle paralysis occurs because a depolarized postjunctional membrane and inactivated sodium channels cannot respond to subsequent release of ACh (hence, the designation depolarizing neuromuscular blockade). Depolarizing neuromuscular blockade is also referred to as phase I blockade . Phase II blockade is present when the postjunctional membrane has become repolarized but still does not respond normally to ACh (desensitization neuromuscular blockade). The mechanism of phase II blockade is unknown but may reflect the development of nonexcitable areas around the end plates that become repolarized but nevertheless prevent the spread of impulses initiated by the action of ACh. With the initial dose of SCh, subtle signs of a phase II blockade begin to appear (fade to tetanic stimulation). Phase II blockade, which resembles the blockade produced by nondepolarizing NMBDs, predominates when the intravenous dose of SCh exceeds 3 to 5 mg/kg ( Table 11.1 ).

The sustained depolarization produced by the initial administration of SCh is initially manifested as transient generalized skeletal muscle contractions known as fasciculations . Furthermore, the sustained opening of sodium channels produced by SCh is associated with leakage of potassium from the interior of cells sufficient to increase plasma concentrations of potassium by about 0.1 to 0.4 mEq/L. With proliferation of extrajunctional nAChRs and damaged muscle membranes, many more channels will leak potassium and thereby lead to acute hyperkalemia.

Metabolism

Hydrolysis of SCh to inactive metabolites is accomplished by plasma cholinesterase (pseudocholinesterase) produced in the liver (see Fig. 11.4 ). Plasma cholinesterase has an enormous capacity to hydrolyze SCh at a rapid rate (ACh is metabolized even more rapidly by acetylcholinesterase) such that only a small fraction of the original intravenous dose reaches the NMJ. Because plasma cholinesterase is not present at the NMJ, the neuromuscular blockade produced by SCh is terminated by its diffusion away from the NMJ into extracellular fluid. Therefore, plasma cholinesterase influences the duration of action of SCh by controlling the amount of SCh that is hydrolyzed before reaching the NMJ. Liver disease must be severe before decreases in the synthesis of plasma cholinesterase are sufficient to prolong the effects of SCh. Potent anticholinesterases, as used in the treatment of myasthenia gravis, and certain chemotherapeutic drugs (nitrogen mustard, cyclophosphamide) may so decrease plasma cholinesterase activity that prolonged skeletal muscle paralysis follows the administration of SCh.

Adverse Side Effects

Adverse side effects after the administration of SCh are numerous and may limit or even contraindicate the use of this NMBD in certain patients (see Box 11.2 ). After 60 years of use, SCh continues to cause serious complications. SCh usually should not be given to patients 24 to 72 hours after major burns, trauma, and extensive denervation of skeletal muscles because it may result in acute hyperkalemia and cardiac arrest. Administration of SCh to apparently healthy boys with unrecognized muscular dystrophy has resulted in acute hyperkalemia and cardiac arrest. For this reason, the FDA has issued a warning against the use of SCh in children, except for emergency control of the airway.