Residual Neuromuscular Blockade Clinical Trial
Official title:
Reversal of Neuromuscular Blockade in Thoracic Surgical Patients
The majority of patients undergoing surgery receive neuromuscular blocking agents (NMBAs) in the operating room. Reversal of neuromuscular blockade at the conclusion of a general anesthetic is accomplished with cholinesterase inhibitors (primarily neostigmine). Although these drugs are often effective in enhancing recovery of muscle strength, the onset of effect is often slow (usually 15-30 minutes). More effective neuromuscular reversal agents are needed in clinical practice to enhance surgical and anesthetic management of perioperative patients. A new reversal agent (sugammadex) will likely be approved for clinical use in the United States next year. Unlike neostigmine, sugammadex is effective in providing rapid antagonism of all levels of neuromuscular blockade (typically within 2-4 minutes). The aim of this prospective observational study is to study neuromuscular and clinical recovery in 100 consecutive thoracic surgical patients receiving neostigmine, followed by a 100 consecutive thoracic surgical patients administered sugammadex (after the drug is approved by the FDA). In addition, after data on 100 patients reversed with neostigmine is collected, the data will be analyzed to compare patients with residual block (train-of four < 0.9) and without residual block (TOF </= 0.9)
Patients undergoing thoracic surgical procedures receive a general anesthetic in the
operating room. As part of this general anesthetic, patients are administered a neuromuscular
blocking agent (NMBA or muscle relaxant). NMBAs are used to facilitate placement of
endotracheal tubes (breathing tubes), provide muscle relaxation during surgery, and prevent
patient movement. Most thoracic surgeons request deep levels of muscle relaxation during
operative procedures. In particular, deeper levels of neuromuscular blockade are required to
prevent movement of the diaphragm (diaphragmatic contractions can interfere with the surgical
procedure).
Muscle contraction occurs when the neurotransmitter acetylcholine binds to the postjunctional
nicotinic acetylcholine receptor (nAChR). Non-depolarizing NMBAs inhibit neuromuscular
transmission primarily by competitively antagonizing or blocking the effect of acetylcholine
at the postjunctional nAChR. When high enough concentrations of NMBAs are present, binding to
the nAChR occurs, thus preventing acetylcholine from activating the receptor. Binding of
NMBAs to the nAChR occurs in a competitive fashion. If higher concentrations of acetylcholine
are present at the neuromuscular junction, acetylcholine will attach to the postsynaptic
receptor and facilitate neuromuscular transmission and muscle contraction. Conversely, if
higher concentrations of nondepolarizing NMBAs are present at the neuromuscular junction,
binding to the nAChR will preferentially occur, preventing muscle depolarization from
occurring.
The effects of NMBAs must be reversed at the end of surgery. One mechanism of antagonizing
the effects of NMBAs is to increase the concentration of acetylcholine at the neuromuscular
junction. This can be accomplished using an anticholinesterase drug which inhibits the enzyme
which breaks down acetylcholine at the neuromuscular junction (acetylcholinesterase). The
anticholinesterase drug which is most commonly used to reverse neuromuscular blockade is
neostigmine. At NorthShore University HealthSystem, all patients receiving a NMBA are
reversed with neostigmine at the conclusion of the surgical procedure. There are two
important limitations of anticholinesterase reversal agents, which are related to their
mechanism of action as described above. First, onset of action is slow. In the presence of
mild degrees of muscle relaxation (four responses to train-of-four (TOF) nerve stimulation
with a peripheral nerve stimulator, also known as a TOF count of 4), adequate reversal of
NMBAs takes approximately 10-15 minutes. However, in the presence of deeper neuromuscular
block (one response to TOF nerve stimulation, or TOF count of 1), complete reversal takes on
average 30-60 minutes. Second, profound neuromuscular blockade cannot be antagonized. If no
evidence of neuromuscular recovery is present at the end of surgery (no response to
peripheral nerve stimulation or a TOF count of 0), reversal agents are ineffective. In this
situation, the concentration of the NMBA at the neuromuscular junction is too high (NMBA will
preferentially bind to the nAChR over acetylcholine, and inhibition of acetylcholinesterase
cannot raise levels of acetylcholine enough to competitively antagonize the NMBA).
Despite the routine reversal of muscle relaxants in the operating room, patients often arrive
in the post anesthesia care unit (PACU) with evidence of residual muscle weakness (termed
residual neuromuscular blockade). Traditionally, residual neuromuscular blockade has been
measured and defined using quantitative neuromuscular monitoring devices. These devices use
electrical energy to stimulate the ulnar nerve; four stimuli are provided, and the response
to nerve stimulation at the thumb measured. The ratio of the fourth contraction is compared
to the first contraction to generate a TOF ratio (from 0-1.0 or 0-100%). Recent data suggests
that TOF ratios must recover to > 0.9 to exclude clinically significant residual
neuromuscular blockade. A number of clinical studies have demonstrated that approximately 40%
of patients given NMBAs in the operating room have objective evidence of muscle weakness (a
TOF ratio < 0.9) on admission to the PACU. It is likely that the incidence of residual
neuromuscular blockade is higher in thoracic surgical patients, since deeper levels of
neuromuscular blockade are required. However, no previous studies have specifically
investigated this patient population.
The presence of residual muscle weakness at the end of surgery, following tracheal extubation
(removal of the breathing tube), has been associated with a number of adverse postoperative
events. Patients with TOF ratios < 0.9 on admission to the PACU are at higher risk for
potentially life threatening airway events, including hypoxemia (low oxygen saturation),
airway obstruction, and postoperative pulmonary complications. In addition, patients with TOF
ratios < 0.9 often experience unpleasant symptoms of muscle weakness, such as blurry vision,
difficultly speaking and swallowing, and general weakness. Patient-perceived quality of
recovery from anesthesia and surgery is also significantly lower in patients admitted to the
PACU with TOF ratios < 0.9. Studies have also demonstrated that patients with TOF ratios <
0.9 take significantly longer to reach discharge criteria from the PACU, and achieve actual
PACU discharge.
Improved management of neuromuscular blockade in the operating can beneficially impact both
the incidence of residual neuromuscular blockade, as well as complications associated with
incomplete neuromuscular recovery. For example, the use of quantitative neuromuscular
monitoring, by allowing a more rational titration of NMBAs intraoperatively, has been
demonstrated to reduce the risk of admission to the PACU with a TOF ratio < 0.9. Furthermore,
the risk of hypoxemic events, airway obstruction, and unpleasant symptoms of muscle weakness
is diminished with quantitative monitoring.
Another potential method of reducing the risk of residual neuromuscular blockade, and the
complications associated with residual blockade, is through the use of a new class of NMBA
reversal agent. Sugammadex is a recently developed antagonist of steroidal NMBAs that acts
via a different mechanism than the anticholinesterase agents. Sugammadex (Org 25969) is a
modified γ-cyclodextrin and the first selective relaxant binding agent based on an
encapsulating principle for inactivation of a neuromuscular blocking agent. Sugammadex is a
cylindric compound with a lipophilic cavity and a hydrophilic exterior. This structure allows
the drug to take up lipophilic molecules in its core; sugammadex rapidly encapsulates
steroidal NMBAs like rocuronium that are present in the circulation. Rapid encapsulation of
rocuronium in the intravascular compartment results in a gradient which draws rocuronium away
from the neuromuscular junction (where it is also immediately encapsulated). This principle
for reversal of rocuronium- and vecuronium-induced neuromuscular block was first introduced
into clinical practice in 2008 and is now available for pediatric and adult anesthesia in a
majority of countries world-wide. The complex formation of sugammadex and rocuronium or
vecuronium occur at all levels of neuromuscular block (profound - shallow) and displays a
more rapidly-acting pharmacological profile as opposed to anticholinesterases for reversal of
effect. When appropriate dosing of sugammadex is used, all levels of neuromuscular blockade
can be reversed (TOF ratio > 0.9) within 2-4 minutes. Consequently, sugammadex may have the
potential to markedly reduce postoperative residual neuromuscular block in the PACU. In
addition, sugammadex may also reduce the incidence of adverse events related to incomplete
neuromuscular recovery. Sugammadex has been extensively investigated in a large number of
clinical trials and has been demonstrated to be significantly more effective and rapid in
reversing all levels of neuromuscular block, when compared to neostigmine. At the present
time, the safety profile of sugammadex appears similar to neostigmine, in both clinical
trials and in world-wide usage (over 4 million uses, per manufacturers report).
Sugammadex may offer several potential advantages in patients undergoing thoracic surgery.
Deep levels of neuromuscular blockade can be maintained until the end of the procedure, which
may facilitate the performance of the surgery. Sugammadex is effective in reversing deep
levels of blockade (even at a TOF count of 0 or "no twitches"), whereas neostigmine cannot
antagonize deep blockade. In addition, the time in the operating room may be shortened. It is
not uncommon for tracheal extubation to be delayed in this patient population due to the slow
onset of effect of neostigmine when moderate levels of neuromuscular block are present at the
time of reversal (TOF count of 1-3). Furthermore, patient recovery may be enhanced in the
PACU if the incidence of residual block is reduced with sugammadex. The aim of this
prospective observational investigation is to examine the effect of sugammadex (versus
neostigmine) on recovery following thoracic surgery. In addition, after data on 100 patients
reversed with neostigmine is collected, the data will be analyzed to compare patients with
residual block (train-of four < 0.9) and without residual block (TOF </= 0.9) The primary
outcome variable will be the incidence of residual block (measured with quantitative
neuromuscular monitoring) at the time of PACU admission. Secondary outcome measures will
include the incidence of residual block at tracheal extubation, the time from surgical
closure until tracheal extubation, the frequency of adverse respiratory events in the PACU,
the presence or absence of symptoms and signs of postoperative muscle weakness, and length of
stay in the operating room and PACU.
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