ABSTRACT
Aim:
Intraoperative neurophysiological monitoring (IOM) has been increasingly used in surgeries associated with a risk of neurological impairment. Motor evoked potential (MEP), which is a part of intraoperative neurophysiological tests, evaluates motor function intraoperatively. Most anesthetic agents have negative effect on neurophysiologic recordings because of neuronal excitability changes. Our aim was to compare the effect of anesthetic methods consisting of volatile anesthetics and intravenous anesthetics (propofol + remifentanil) on eliciting of MEP during baseline recordings for spinal surgery which is a part of neurosurgical operations.
Methods:
Fifty patients (29 males and 21 females; 21 to 85 years) who underwent spinal surgery with IOM in our department between 2016 and 2018 were randomly chosen for retrospective evaluation. A multipulse stimulation technique (6-9 stimuli) was used for electrical stimulation.
Results:
There was a statistically significant difference in stimulus threshold in voltage stimulation between the two groups. In order to elicit muscle MEP, a higher voltage threshold had to be implemented for patients who had been given volatile anaesthesia compared to those who had been given total intravenous anesthesia (TIVA) (Mann-Whitney U test, p<0.005).
Conclusion:
TIVA is considered better than volatile for eliciting muscle MEPs in lower stimulus threshold. In addition, TIVA provides easy recording in all proximal and distal muscles.
Introduction
Intraoperative neurophysiological monitoring (IOM), which aims the best quality of life after surgery, has been increasingly used in new advanced concept of neurosurgery, cardiovascular surgery and thyroid surgery (1-4). Primary intraoperative neurophysiological studies are motor- and sensory-evoked potentials (MEP and SEP), electromyography and, electroencephalography. Among these, MEP presents the functionality of motor pathway from the cortex to muscles during the surgery. Loss of MEP and decreased MEP amplitude indicate postoperative motor worsening. Thus, MEP evaluation during surgery is necessary for patients with lesions that may affect the motor pathways. Most of anesthetic agents used intraoperatively change excitability of the neuroaxis at the cortical, subcortical and spinal levels and have negative effect on neurophysiological recordings (5).
This study aims to compare the effect of anesthetic methods consisting of volatile anesthetics and intravenous anesthetics (propofol + remifentanil) on eliciting MEP during spinal surgery.
Methods
Subject and Data Collection
Fifty patients who underwent spinal surgery with the aid of IOM were included in this study. Sevoflurane, which is one of the most commonly used volatile anesthetics, was used in 20 patients and propofol plus remifentanil in 30 patients. Demographical characteristics, neurological examination findings, diagnosis, surgical level, anesthesia type, and intraoperative neurophysiological recordings of 50 patients were retrospectively evaluated. Those having a hemoglobin level of <10 gr/dL and hematocrit concentration of <35% in preoperative evaluations were excluded.
Transcranial Motor Evoked Potentials
MEPs were elicited by stimulating the motor cortex from the scalp and recording from muscles. Stainless steel needle electrodes (13-19 mm, Xi’an Friendship Medical Company) and corkscrew electrodes were used for MEP responses respectively. Stimulation was performed using a multipulse stimulation technique based on a train of 6 to 9 stimuli with 4 ms interstimulus interval (ISI), pulse width of 50 µs, and an intensity between 200 V and 600 V, delivered at C1-C2 for right (R) extremity and C2-C1 for left (L). C3-C4/C4-C3 montage was used when not being gained with C1-C2/C2-C1 montage. Out of these two groups, the one with the lowest voltage threshold to elicit mMEP was used. Abductor pollicis brevis (APB), tibialis anterior (TA) and abductor halluces (AH) were recorded in all patients. Trapezius, deltoid, biceps brachi, extensor digitorum communis and iliopsoas, quadriceps femoris (QF), vastus lateralis, gastrocnemius, and sphincter ani externus muscles were added depending on surgical level. Evaluation was made for muscles having the lowest muscle threshold (APB, TA and, AH).
The Cadwell elite IOM system was used for neurophysiological recordings.
Total intravenous anesthesia (TIVA) using propofol (1.5-2 mg/kg for anesthesia induction and 6-10 mg/kg/h for maintenance) plus remifentanil (0.15 µg/kg/min) was used in 30 patients while inhalation anesthesia (sevoflurane, minimum alveolar concentration (MAC) maximum 0.5, BIS 40-60) was used in 20. A short-acting muscle relaxant (rocuronium, 0.5 mg/kg) was used only for endotracheal intubation. Satisfactory recovery from neuromuscular block was monitored by the train-of-four technique before MEP recording. In addition, mean arterial pressure, end-tidal carbon dioxide and oxygen concentration were monitored by the anesthesia team before eliciting MEP responses in all cases.
All procedures were performed in accordance with the 1964 Helsinki Declaration and its later amendments. Due to the fact that the study was retrospective, ethical committee approval was not obtained. Written informed consent was obtained from the patients.
Statistical Analysis
The statistical package for the social sciences (SPSS) 22.0 was used for data analysis. For descriptive statistics, the measures used were percentage distributions for categorical variables, and means (medians) with standard deviation (ranges) and, ranges for continuous variables. Frequency distributions were compared using the chi-square test and means by independent samples t-test and one-way analysis of variance (ANOVA) for normal variables, The Mann-Whitney U test and Kruskal-Wallis H test were used for non normal variables.
Results
The mean age of the patients (29 males and 21 females) was 48.7 years (range: 21-85 years). Bilateral extremities of 50 patients were evaluated, yielding a data set of 100. All patients had a hemoglobin level of >10g/dL. The diagnosis and surgical levels in the two groups are shown in Table 1.
TIVA Group
Eight patients had an intradural extramedullary mass, five had an intramedullary mass, two had an extradural mass, nine had stenosis, and six patients had fracture. Operation levels were at the cervical spinal level in 15, thoracal in nine and, lumbar in six. Fourteen patients had motor deficits preoperatively, with three of them having <3/5 motor power. Mean voltage value for TIVA group was 325 V, ranged from 170 to 450. In 60 extremities, APB-MEP was elicited in all except 2 which had severe motor paralysis. AH-MEP was not achieved in 6 (3 R, 3L) which had severe motor paralysis (<2/5) preoperatively and QF-MEP in 11 extremities, with eight out of 11 had motor paralysis at the preoperative neurological examination. MEP response variability was not detected in this group.
Volatile Group
Eight patients had an intradural extramedullary mass, 1- intradural intramedullary tumor, 1- extradural tumor, 7- stenosis, and 3- fracture. Operation levels in this group were cervical spinal level in 7, thoracal in 3, lumbar in 9 and, sacral in one. Seven patients had mild (>3/5) motor deficit preoperatively. Mean voltage value for volatile group was 423V, ranged from 330 to 600. MEP response variability was detected in two. R APB-MEP and bilateral proximal muscle MEPs (deltoid, biceps brachi) were elicited at the baseline recording in all except one having C1-C2 meningioma and no neurological deficit preoperatively. AH-MEP could not be elicited in one patient having severe motor deficit preoperatively and QF-MEP in 5 (3 R, 2 L) with three of those had motor deficit in preoperative neurological examination.
There was a statistically significant difference in stimulus threshold in voltage stimulation between the two groups (Mann-Whitney U test, p<0.005). Presence of motor deficit preoperatively did not have an impact on the increase of required voltage stimulation in the two groups.
Discussion
This study showed that voltage threshold to elicit mMEP with the multipulse stimulation technique--a train of 6 to 9 with an ISI of 4 ms, pulse width of 50 µs--in patients who had been given volatile anaesthesia was higher than that of TIVA. There are some studies evaluating suppressive effect of inhalation agents on MEPs (6). They generally pointed out reduction in MEP amplitude with volatile anesthetic usage in different MAC levels. In their study randomizing patients to three groups to receive halothane (HAL), isoflurane (ISO), or sevoflurane, Sekimoto et al. (6) reported that the amplitudes of MEPs were significantly reduced by all agents at 1.0 MAC, with the effect being less in HAL at 0.5 MAC. In this study, we focused on stimulus threshold for eliciting MEP response by the multipulse stimulation technique (6 to 9 stimuli with an ISI of 4 ms, pulse width of 50 µs) by sevoflurane agent at <0.5 MAC and TIVA. There was a statistically significant difference in stimulus threshold in voltage stimulation between the two groups (Mann-Whitney U test, p<0.005).
It is known that obtaining MEP response in lower extremities is difficult in patients with preoperative motor deficit. Chen et al. (7) reported that the success rate for obtaining reliable MEP response was 94.8% for upper extremities and 66.6% for lower extremities and it was only 39.1% for lower extremities in patients with preoperative motor deficit. This challenge could be demonstrated in patients who had been given volatile anaesthesia. In contrast, presence of preoperative motor deficit did not have an impact on the increase of required voltage stimulation in the two groups although provided MEP was much lower in patients with preoperative motor weakness in this study. This might be explained by very mild motor paralysis (>4/5) in our patients.
MEP response variability was detected in two patients of only volatile group in this study. Volatile agents decrease the possible motor neuron recruitment in anterior horn of the spinal cord and affect the propagation of a peripheral motor response negatively. Thus, volatile agents interfere with reliable MEP acquisition. Pelosi et al. (8) confirmed this situation in their study reporting that reliable recordings were present in 14 of 23 patients who received volatile agents and 28 of 29 who received propofol. In addition, bilateral MEP recruitment ratios were higher with propofol than with volatile anaesthesia. TIVA offers obvious advantages in obtaining MEP response and reliable acquisition during surgery.
Isofluran, enfluran, desfluran, sevoflurane and halotan are volatile anesthetics. In general, all have similar effects on evoked potentials. In this study, we evaluated the effect of sevoflurane on MEP acquisition and response variability. Volatile anaesthetics have an effect on pyramidal neurons, cortical interneurons, corticospinal axons and, alfa motor neuron (9-11). Inhibition via neocortical GABA-A receptors ensures cortical suppression (9,10). Suppressing effect on motor pathway at the corticospinal and spinal level is based on blocking synaptic transmission over alpha motor neurons in the spinal cord and depressing Na transmission at the Ranvier nodes of corticospinal axons (11). Propofol’s advantage over volatile anaesthesia is that it has a negligible effect on MEP at the spinal level. As seen in our study, MEP acquisition is achieved more easily and with lower voltage stimulation under TIVA.
Volatile anesthetics depress excitatory synaptic transmission by inhibiting presynaptic voltage-gated Na+ channels at clinical concentrations. In contrast, the intravenous anesthetic propofol inhibits Na+ channels only at supratherapeutic concentrations (12). Some new sedatives such as alpha2-agonist dexdemetomidine have been come up to decrease propofol dosage (13,14).
Study Limitations
All patients with and without motor weakness were included in this study. It would better to include patients with normal MEP findings without motor weakness for comparing the voltage stimulus thresholds for eliciting muscle MEPs between the two groups.
Conclusion
As a consequence, at a current time, TIVA is considered to be better than volatile anesthetic for monitoring muscle MEPs. Even in cases in which TIVA is used, however, it should be considered that higher levels of propofol may cause suppression on alpha motor neuron at the spinal level and thus misinterpretation of MEP loss or amplitude decreasing in this setting. With developing new anaesthetic agents, new studies aiming to evaluate their suppressing effect on MEPs and/or other evoked potentials would be required.