The state of general anaesthesia is one in which various behavioural end points can be distinguished, including amnaesia, hypnosis (defined as lack of perceptive awareness to non-noxious stimuli), analgaesia, immobility, and blunting of autonomic reflexes produced by general anaesthetics acting on the neuronal loci (20). When a subject is put into this state, a volatile anaesthetic acts on the central nervous system to produce two irreversible conditions: immobility and amnaesia. These drugs may produce some other reversible and clinically useful conditions, like unconsciousness, relaxation, suppression of autonomic reflexes, or analgaesia, but none of these are essential to the definition of the anaesthetic state since they are merely side effects (10).
The hypnogenic centre in the preoptic area of the hypothalamus is responsible for the sleep-promoting neurons. The state of rapid eye movement (REM) sleep is characterised by a high-frequency, low-amplitude rhythm on the electroencephalogram (EEG) but minimal or absent electromyogram (EMG) activity. The effect of amnaesia is produced by abolishing hippocampal neurons and basolateral nucleus of the amygdala. While consciousness is modulated by thalamus, midbrain reticular formation and thalamocortical system. To do this, tools such as BIS (Bispectral Index) allow assessing the consciousness and depth of anaesthesia (20).
Analgaesia is difficult to measure precisely during general anaesthesia, but haemodynamic reactivity, such as increased heart rate and blood pressure, may suggest failure in achieving it in an anaesthetised patient. However, these parameters do not show adequate specificity for an independent measurement of the intensity or magnitude of pain during the perioperative period (14, 30, 35). The analgaesic component of anaesthesia can be indirectly monitored for variations in sympathetic and parasympathetic tone as an objective way of evaluating the balance between nociception and antinociception (3, 12).
Several methods have been implemented to quantify the nociception–antinociception balance in the anaesthetised patient in a more reliable way,
PTA index values range from 0 to 100. An index of 50–70 suggests the absence of nociception; values close to 100 correspond to a predominant parasympathetic tone (low level of stress) or opioid overdose; and values below 50 correspond to a predominant sympathetic tone (anticipating haemodynamic responses) associated with a high level of stress or nociceptive pain in dogs undergoing surgical procedures. The PTA index can also be used to predict immediate postoperative analgaesia (4, 6).
The ANI index has been validated for use in human medicine as a non-invasive tool to assess pain during the immediate postoperative period, as it correlates significantly with pain intensity (6). It has been evaluated during general anaesthesia in adults and children as an intraoperative tool (17) and for labour pain evaluation, and exhibited significant changes between periods with and without pain (22). However, equivalent studies in animal medicine using the PTA index have not been undertaken.
The objective of this study was to rectify this deficiency in knowledge by determining the utility of the PTA index for assessment of analgaesia during the postoperative period in female dogs undergoing ovariohysterectomy. We hypothesised that the PTA index could be used to assess pain response, as its dynamic variation can be used as a signal of a haemodynamic response associated with pain.
This was a randomised, prospective, blinded clinical study.
During surgery, this concentration was increased or decreased based on the depth of anaesthesia required for surgery based on clinical signs, including absence of the palpebral reflex, relaxed jaw tone, and mean arterial pressure of 60–90 mmHg. Immediately after induction, fentanyl was administered (5 μg/kg b.w. IV; Fenodid, PiSA Farmacéutica) and constantly infused at 5 μg/kg b.w./h. At the end of surgery, fentanyl infusion was discontinued. The dogs were mechanically ventilated at an initial respiratory rate (RR) of 15 breaths per minute and a tidal volume of 12–15 mL/kg b.w. adjusted to maintain end-tidal carbon dioxide tension (ETCO2) of 35–45 mmHg, which was facilitated by administration of rocuronium (0.6 mg/kg b.w. IV; Lufcuren, PiSA Farmacéutica). All anaesthetic and surgical procedures were performed by the same anaesthetist and surgeon. Postoperatively for 48 h, paracetamol was administered to the designated group dogs every 8 h in doses of 15 mg/kg b.w. orally, and carprofen (4 mg/kg b.w.) and meloxicam were administered to the appropriate subjects every 24 h, IV. In this period, the dose of meloxicam was reduced to 0.1 mg/kg b.w.
During anaesthesia, heart rate (HR), ETCO2 and pulse oximetry were monitored. A 22-gauge catheter was aseptically placed in the dorsal metatarsal artery and attached to a transducer (DTX plus DT 4812; Becton Dickinson Critical Care Systems Pte. Ltd., Singapore) for direct monitoring of arterial blood pressure (systolic blood pressure (SBP), diastolic and mean). Thermal support was provided throughout the surgery to maintain the temperature in physiological ranges (36–38°C) (Equator Convective Warming Device, Smiths Medical, Inc., Minneapolis, MN, USA). Neuromuscular function was monitored
The PTA monitor displays a graphic recording of the derivative II of the electrocardiogram (ECG),
The PTA index was calculated according to the following formula:
PTA = (100*[α *AUCmin + β] / 12.8)*100/161 where α and β values have been empirically determined as 5.1 and 1.2, respectively, to maintain the consistency of the respiratory influence on the R–R interval series of the ECG; AUCmin is the minimum area under the curve; and 100/12.8 and 100/161 are coefficients for different species determined to obtain PTA values between 0 and 100, with 100/161 being specific to the dog (7, 28).
HRV was evaluated
The PTA monitor continuously shows the instantaneous/immediate PTA index, as well as the average/mediate PTA index values collected over 120 s and 240 s. The PTA index was continuously measured through a window of 64 s after each measurement (4, 6, 22, 27, 28). The PTA monitor was calibrated with the canine-specific coefficients already described. Once the ECG electrodes were placed, the criteria for considering a PTA index measurement valid was the monitor recording good signal quality. For each postoperative analgaesia assessment interval, HRV was recorded for 5 min with the patient standing, at which time the average/mediate PTA index value was recorded. At the same postoperative examination times, the validated University of Melbourne Pain Scale (UMPS) score was evaluated (34).
In this study, we estimated that nine dogs for any group were sufficient to assert that a difference of 20 PTA index scores (65 ± 15
Fig. 1 depicts the PTA indices measured for the three study groups. It should be noted that the mean PTA indices measured for all three study groups and at all assessment intervals were similar. The baseline PTA index for GPARAC was 65 ± 8, for GCARP it was 65 ± 7, and for GMELOX it was 62 ± 5. During the postoperative period, the PTA index was 65 ± 9 for GPARAC, 63 ± 8 for GCARP, and 65 ± 8 for GMELOX (Fig. 1). We detected no statistically significant difference between either baseline values or between treatments (P = 0.99 and P = 0.97), respectively.
Postoperative PTA values during different treatment times with carprofen, meloxicam, and paracetamol
The P value comparing the PTA indices between treatments was 0.97 and the P value comparing baseline values to post-operative values was 0.99
For 26 dogs, postoperative PTA indices were within normal parameters. Four dogs (one dog in GPARAC and GMELOX and two dogs in GCARP) required rescue analgaesia as subjects with PTA indices between 40 and 49 (moderate pain) and a score > 10 in UMPS. The scores on this scale for the three study groups during the postoperative period are listed in Table 1. These results were used in this investigation as a reference for the evaluation and validation of the clinical utility of the PTA index in conscious animals. The sensitivity, specificity and negative predictive value are presented in Table 2, which shows that PTA index has a greater capacity to recognize pain-free states associated with comfort and postoperative analgaesia. Therefore, with the determination of these diagnostic characteristics, it was possible to establish that individuals who manifested pain could be recognised through the measurement of PTA index and by clinical observation performed by UMPS.
UMPS scores during the postoperative period in GPARAC, GCARP, and GMELOX
Postoperative period (hours) | |||||||||||
---|---|---|---|---|---|---|---|---|---|---|---|
1 | 2 | 4 | 6 | 8 | 12 | 16 | 20 | 24 | 36 | 48 | |
GPARAC | 5.5±0.8 | 4.5±0.8 | 3.0±0.6 | 3.0±0.4 | 2.0±0.4 | 2.0±0.4 | 1.5±0.3 | 1.0±0.3 | 1.0±0.3 | 0.0±0.2* | 0.0±0.2* |
GCARP | 4.5±1.4 | 4.0±0.6 | 3.0±0.3 | 2.0±0.3 | 2.0±0.3 | 1.0±0.4 | 1.0±0.4 | 0.5±0.4 | 0.0±0.4* | 0.0±0.1* | 0.0±0.1* |
GMELOX | 5±0.9 | 3.5±0.8 | 3.0±0.4 | 2.5±0.3 | 1.5±0.5 | 0.5±0.3 | 0.5±0.3 | 0.0±0.1* | 0.0±0.1* | 0.0±0.0* | 0.0±0.0* |
(*) Statistically significant differences from the first evaluation (P = 0.001)
No statistically significant differences were found between treatments (P = 0.99)
Intrinsic diagnostic characteristics of the PTA index during the evaluation of postoperative analgaesia
Percentage | |
---|---|
Sensitivity | 40% |
Specificity | 98.46% |
Negative predictive value | 99.07% |
The process of pain assessment during the postoperative period is affected by factors in the assessor such as their age and sex, pharmacological knowledge of analgaesic medication, attitude toward pain, clinical experience of its identification and ability to quantify and manage it. Therefore, observations of pain should be made consistently by the same person (14, 31). These human factors have led to tools that evaluate the sympathetic–parasympathetic tone balance attracting special interest (18, 32), as one of the first responses of an organism to surgical stress is an increase in sympathetic tone and a decrease in parasympathetic tone, which influences HRV (23, 29).
In the case of a predominant parasympathetic tone, each inhalation briefly increases HR and concomitantly decreases the R–R interval of the ECG, which can cause a wide variation in the R–R pattern. Conversely, in the case of a predominant sympathetic tone, the HR increases, but the effect of respiratory arrhythmia on the R–R pattern diminishes, which results in a filtered band with little variation that allows the evaluation of the analgaesia–nociception balance (7, 16, 17). Thus, in the present study, the PTA index calculated for the GPARAC, GCARP, and GMELOX groups indicated that patients exhibited postoperative analgaesia.
Mansour
The PTA index during the intraoperative period has also been evaluated in male dogs subjected to castration and females undergoing ovariohysterectomy, where a significant difference was observed and the PTA values were higher (indicative of a lower degree of nociception) in males (61 ± 19) than in females (50 ± 17), as well as in patients where an epidural block was used (57 ± 19
Recently, Aguado
Given that the studies or reports carried out so far in dogs are scarce, articles related to the postoperative period in humans where the ANI has been used as a tool to measure patients’ pain will be used in the discussion. In a prospective observational study of 200 individuals undergoing orthopaedic surgery, Boselli
This usefulness is consistent with that described by Ledowski
In the present study, four analgaesic rescues were performed where the values in the PTA index resolved to moderate pain. These patients also presented a score > 10 in UMPS. In this regard, the ability of the PTA index to detect pain in patients who manifest it clinically (the index’s sensitivity) has been reported by other researchers (3, 28) where it fluctuated between 77% and 86%; specificity ranged from 72% to 86%, and the negative predictive value was 92% (3). These results were similar to those calculated in the present study. Therefore, the PTA index appears to be a reliable tool to measure the degree of analgaesia.
In human medicine, there are more studies where the activity of the parasympathetic tone is evaluated through the capacity of the ANI monitor to detect nociceptive stimulation (16, 17), but there are questions regarding the use of a similar index in animals due to species variations of the sympathovagal balance. Nevertheless, HRV measurements that were described in dogs had similar values to those reported in humans, with a low frequency of 0.004–0.15 Hz and a high frequency of 0.15–0.5 Hz (30), which allows comparison of the results obtained in this study with those cited by various researchers in human studies.
In practice, there are factors external to nociception that can influence the reading of the PTA index, such as age, species, the increased vagal tone in brachycephalic breeds, arrhythmia, apnoea, fewer than 8 respiratory cycles/min, the operation of a pacemaker, pathologies (e.g. epilepsy or cerebrovascular accident) or medications (e.g. atropine or vasopressors such as dobutamine and sedatives such as medetomidine or dexmedetomidine) that interrupt the regulation of the autonomic nervous system (3, 5, 9, 13, 37). However, at least in humans, there is evidence that intravenous ketamine microdose infusion contributes to analgaesia without affecting the ANI index under clinical conditions (2). The PTA index therefore helps to assess whether there is an analgaesic sub or overdose condition during the perioperative period (24, 26).
The PTA index as applied in this study could also have been misrepresentative during the first minutes of postoperative evaluation after extubation, since the evaluation of nociception with this type of tool that assesses the autonomous cardiovascular control of HRV in real time has previously aggregated data related to negative emotional states (including pain, stress, anxiety and aggressiveness) in dogs (19, 21, 38). The dogs in this study were assessed by the anaesthetist during recovery and deemed to be calm and comfortable, which should have minimised autonomic responses that affect the PTA index; this was also evidenced by the low number of dogs that exhibited a PTA index indicative of pain.
This study offers some significant benefits for pain assessment in conscious patients or in the postoperative period, however, this research has some limitations that require discussion. For example, the dogs included in this study have a potentially different variability of nervous system activity due to size, age and breed, so future studies should consider a homologation of these factors. Additional studies are needed to validate the use of the PTA index to rate postoperative pain when considering other forms of nociceptive stimuli, since the present study only examined healthy dogs after elective surgery. Also, it is recommended that in future investigations, the use of this device should be considered against other analgaesic options, such as the new opioid agonist related to the selective activation of the β-arrestin signalling pathway called oliceridine (36), a drug that has recently been approved for perioperative pain control as an alternative to morphine or fentanyl, and opioids that influence HRV and have shown properties that can modify the PTA index values. Likewise, the PTA monitor also has some limitations in conscious patients, since the electrocardiogram signal can be altered by the animal’s movements (28). Finally, the PTA monitor does not show the dynamic value of the HRV, and consequently it must be calculated based on the static values provided by the same monitor. In this study, this restricted PTA reporting to only the median/average values.
In conclusion, our findings suggest that the PTA index represents an objective measurement of comfort and analgaesia during the postoperative period, since it showed a clinical relationship with the UMPS; therefore, it is a tool that could help monitor the haemodynamic responses associated with pain or stress.