Background
Laryngoscopy and endotracheal intubation (ETI) are associated with sympathetic stimulation induced hemodynamic changes [
1]. The consequent increase in heart rate (HR) and blood pressure (BP) though short-lived may lead to myocardial infarction, cardiac arrhythmias, cardiac failure and cerebrovascular accidents in patients with underlying cardiovascular or cerebrovascular diseases [
1]. Premedication with various agents has been shown to attenuate this sympathetic response and its associated risk of arrhythmias and myocardial infarction [
1]. However, none of them is ideal and each of them is associated with its unique adverse effects like hypotension, bradycardia, chest rigidity or increased bronchomotor tone [
1].
Dexmedetomidine is a centrally acting α-2 adrenergic agonist with sedative, hypnotic, analgesic, anxiolytic, antisialagogue, antinociceptive and sympatholytic action [
2,
3]. Premedication with dexmedetomidine through intravenous, intramuscular and intranasal route has been shown to effectively attenuate hemodynamic response to laryngoscopy and ETI [
4‐
10]. However, its use is associated with adverse effects like hypotension and bradycardia with intravenous route and nasal irritation with intranasal route [
5‐
8,
11]. A 2021 systematic review and meta-analysis (SRMA) showed intravenous dexmedetomidine to significantly attenuate tracheal intubation associated increase in HR and BP but associated with significant risk of bradycardia and hypotension; recommending cautious evaluation while using it in daily practice [
4].
Nebulization provides an alternative route of dexmedetomidine premedication with high bioavailability through both nasal (65%) and oral mucosa (82%) and avoid a venipuncture as a prerequisite. Recent studies have shown nebulisation as a novel route of dexmedetomidine administration for attenuation of hemodynamic response to ETI [
12‐
14]. However, no current or planned systematic review evaluating the safety and efficacy of nebulized dexmedetomidine for blunting hemodynamic response to laryngoscopy and ETI in adult patients was identified.
Therefore, the present SRMA was conducted to systematically identify, collate, critically appraise and synthesize available evidence on dexmedetomidine nebulisation for attenuating hemodynamic response to laryngoscopy and ETI in adult patients (≥ 18 years) undergoing surgery under general anaesthesia. Our findings will help clinicians in evidence based decision-making and formulation of institutional guidelines.
Methods
This systematic review has been reported in accordance with the Preferred Reporting Items for Systematic reviews and Meta-analysis (PRISMA) 2020 standards [
15]. The protocol for this systematic review was registered prospectively in the International Prospective Register of Systematic Reviews (PROSPERO No. CRD42023403624).
Search strategy
A preliminary search helped in identifying thesaurus and free text terms for the key concepts (laryngoscopy, endotracheal intubation and dexmedetomidine). The thesaurus and free text terms for a similar concept were combined using Boolean operator “OR”. The search strings for different concepts were then combined using Boolean operator “AND”. A systematic and comprehensive literature search was performed in the following electronic bibliographic databases: PubMed, Embase and Embase Classic (OvidSP), Cochrane library (
https://www.cochranelibrary.com), Scopus (Elsevier), Web of Science (Clarivate) and Google Scholar from inception to 31st March 2023. The search strategy was limited to randomized controlled trials (RCTs) conducted in humans and published in English language. No date or age restrictions were applied. The search strategy was first formulated for Embase and later adapted for other databases. The search strategy and literature searches were formulated and conducted by one reviewer (MG) and re-ran by another experienced reviewer (UJ) to rule out syntax or any other error. The search strings for all the databases as they were run has been reported in the Supplementary file
1.
To ensure literature saturation, reference lists of included articles and relevant systematic reviews were screened and citation tracking of included articles (on Google scholar and Scopus) was done to identify any additional relevant article. Screening of reference lists and citation tracking continued until no new articles were identified.
Study selection
PICOS format helped operationalise the review question into key inclusion and exclusion criteria. RCTs comparing preoperative administration of dexmedetomidine nebulization with either placebo or no intervention for attenuating hemodynamic response (as measured by HR and BP at any time point up to 10 min after ETI) to laryngoscopy and ETI in adult patients (≥ 18 years of age) undergoing surgery under general anaesthesia with ETI were included. Studies evaluating dexmedetomidine nebulization in pediatric patients, adult patients undergoing tracheal intubation other than for surgery or dexmedetomidine administration through any other route were excluded. Non-randomized studies and evidence synthesis were not included, however, their reference lists were screened to identify any eligible study missed through database searching.
Studies identified through database search were transferred to EndNote reference manager software (V.20, Clarivate Analytics, Philadelphia, Pennsylvania, USA) for de-duplication. De-duplicated results were transferred to Rayyan (
www.rayyan.ai) in which two reviewers (MG, HT) independently performed title and abstract screening against the pre-defined inclusion and exclusion criteria (Table
1). Full texts of potentially eligible studies and studies where eligibility could not be determined from title/abstract screening were retrieved and screened independently by two reviewers (MG, HT) for inclusion. Any discrepancies were resolved through discussion and arbitrated by a third reviewer (PG) where necessary. An audit trail of all the disagreements, reasons for the same and resolutions made ensured trustworthiness of the process.
Table 1
Characteristics of RCTs included in meta-analysis
| 34.5 ± 5.23 | 31 | Dexmed 2 μg /kg in 5 ml NS 30 min before induction and laryngoscopy | 35 | 5 ml NS | 35 | Fentanyl 2 μg /kg, Propofol 2 mg/kg, Vecuronium 0.1 mg/kg IV | Control group had statistically higher values of HR, SBP, DBP, MAP after intubation at all time intervals compared to dexmedetomidine group. | No adverse event reported in either group | |
| 39.15 ± 11.25 | 72 | Dexmed 1 μg /kg in 3–4 ml NS 30 min before induction and laryngoscopy | 60 | 3–4 ml NS | 60 | Ondansetron 4 mg, Midazolam 1 mg, Fentanyl 2 μg g/kg, propofol 10 mg boluses, vecuronium 0.15 mg/kg IV | After laryngoscopy and intubation, a significant trend of decrease in HR in dexmedetomidine group versus control group at all time points. No difference in SBP response between two groups. | Post-operative nausea and vomiting in 3/57 patients in dexmedetomidine group and 1/59 in normal saline group. | Induction dose of propofol, intraoperative fentanyl consumption and mean isoflurane requirements were significantly less in dexmedetomidine group versus control group. |
| 29 ± 7.52 | 27 | Dexmed 1 μg /kg in 5 ml NS 10 min before shifting to OT | 25 | 5 ml NS | 25 | Glycopyrrolate 0.005 mg/kg IM, Fentanyl 2 μg/kg, Propofol 2 -2.5 mg/kg, atracurium 0.5 mg/kg IV | There was significantly reduced SBP, DBP, MAP at 1, 5 and 10 min after laryngoscopy and intubation in dexmedetomidine compared to control group. No difference between the two groups in terms of HR response. | No adverse event reported in either group | |
Suryawanshi 2022, India [ 18] | 43.41 ± 13.21 | 31 | Dexmed 1 μg /kg in 3–4 ml NS 30 min before induction and laryngoscopy | 30 | 3–4 ml NS | 30 | Glycopyrrolate 0.004 mg/kg IV, Inj. Midazolam 0.02 mg/kg IV and Inj. Fentanyl 1- 2 μg /kg IV, propofol 2 mg/kg, Succinylcholine 2 μg/kg IV | HR, SBP, DBP, MAP significantly lower in dexmedetomidine group at all time points studied as compared to the control group. | No adverse event reported in either group | Lower post-operative sore throat in dexmedetomidine group. |
Shrivastava 2022, India [ 19] | 38.97 ± 14.19 | 28 | Dexmed 1 μg /kg in 5 ml NS 30 min before induction and laryngoscopy | 50 | 5 ml NS | 50 | Alprazolam 0.5 mg Midazolam 1 mg, Fentanyl 2 μg/kg, propofol 1–2 mg/kg, Vecuronium 0.1 mg/kg IV | SBP, DBP, MAP and HR significantly lower in dexmedetomidine group compared to control group at 1, 5, 10 min. | No adverse event reported in either group | Nebulised dexmedetomidine has a dose sparing effect on induction dose of propofol. |
| 35.43 ± 7.97 | 43 | Dexmed 1 μg/kg in 3–4 ml NS 30 min before induction and laryngoscopy | 40 | 3–4 ml NS | 40 | Metoclopramide 10 mg IV, Ondansetron 8 mg, Fentanyl 1–2 μg/kg, Propofol 2 mg/kg, Succinylcholine 100 μg IV | SBP, DBP, MAP significantly lower in dexmedetomidine group compared to control group at 2,4,6,8 min. | No adverse event reported in either group | |
Outcome measures
The primary outcome measures analyzed were heart rate (HR) and systolic blood pressure (SBP) at baseline and at any time point till 10 min after ETI (as provided in the published report). Other additional outcomes included diastolic (DBP) and mean (MBP) blood pressure at any time point till 10 min after ETI. We also collected data on bradycardia (% of patients), hypotension (% of patients) and postoperative nausea (% of patients), vomiting (% of patients), respiratory depression (% of patients) or any other adverse outcome as reported in the study.
Two reviewers (MG and RR) independently extracted following data from included studies on a pre-piloted data extraction excel form designed specifically for this review: first author, publication year, inclusion and exclusion criteria, details of intervention and control group (dose, mode of nebulisation, duration of administration), number and demographic characteristics of participants in each group, surgical procedures, rate and reasons for dropout and outcome parameters. Following outcome parameters were retrieved: HR, SBP, DBP and MBP at baseline and at all time till 10 min (as provided in the published report) after ETI; drugs used at induction of anaesthesia and their doses, intraoperative bradycardia or hypotension (% patients) and postoperative nausea and vomiting (% patients). Corresponding authors of included studies were contacted through e-mail for any missing data. Any discrepancies between the reviewers in the extracted data were resolved through discussion.
Risk of bias assessment and rating certainty of evidence
Two reviewers (MG and RR) independently assessed each included study for risk of bias using Cochrane revised risk-of-bias tool for randomized trials (RoB 2) [
21,
22]. RoB-2 assessment was done using the RoB Excel Tool (
https://www.riskofbias.info/welcome/rob-2-0-tool/current-version-of-rob-2). The tool assesses each study for risk of bias on five domains: risk of bias arising from the randomization process, bias arising due to deviations from the intended interventions, bias arising due to missing outcome data, bias in measurement of outcome and bias in selection of the reported result. Each domain in individual studies was graded as “low risk of bias”, “some concerns” or “high risk of bias” for each included study graded across all domains [
21]. The overall risk of bias for individual studies was determined by highest RoB level in any domain. Any discrepancies were resolved by discussion and arbitrated by a third reviewer (PG) where necessary.
Two authors (MG and RR) independently rated the certainty of evidence according to the Grading of Recommendations, Assessment, Development and Evaluation (GRADE) working group system using the GRADEpro software (
https://www.gradepro.org). The quality of evidence was downgraded depending upon the degree of bias, inconsistency, indirectness and imprecision. Any disagreements were resolved through consultation and arbitrated by a third author if required (PG).
Statistical analysis
We performed inverse variance random-effect meta-analysis using RevMan 5.4.1 [Review Manager Version 5.4.1, The Cochrane Collaboration, 2020]. HR, SBP, DBP and MBP were treated as continuous variables and incidence of adverse effects (bradycardia, hypotension) as dichotomous variables. Continuous outcomes were reported as weighted mean difference with 95% Confidence Interval (CI). Significance was set at P < 0.05. Outcome heterogeneity between the studies was assessed using Cochran’s Q test and quantified with I-square statistic. I-square > 50% was considered as statistically significant heterogeneity between the studies. Sensitivity analysis was performed by removing studies using different doses of nebulized dexmedetomidine and observing its effect on outcome heterogeneity and effect estimate. Subgroup analysis was performed if there were more than equal to three studies using different doses of nebulized dexmedetomidine.
Discussion
The findings of this SRMA suggests that premedication with dexmedetomidine nebulization significantly attenuates the hemodynamic response to laryngoscopy and ETI in comparison to normal saline nebulization. Laryngoscopy and ETI are associated with sympathetic stimulation leading to various hemodynamic changes like tachycardia, hypertension and increase in intracranial pressure which could be life threatening in patients with underlying cardio- or cerebro-vascular comorbidities [
24]. The nebulized dexmedetomidine was found to reduce the mean HR as compared to normal saline at all the time points included (1, 2, 3, 4, 5, 6, 8, 10 min). Similar reduction was seen in SBP, DBP and MBP. However, the heterogeneity was found to be high across the studies. In sync with our findings, a recent RCT also found nebulized dexmedetomidine to effectively blunt the pressor response to laryngoscopy and ETI, better than that of nebulized fentanyl and equivalent to that of nebulized magnesium sulphate [
25]. Dexmedetomidine’s highly-selective agonistic action on presynaptic α2-adrenergic receptors and subsequent inhibition of norepinephrine release from the locus coeruleus has been hypothesized as the most putative mechanism for its hemodynamic stress response attenuating action [
26]. Intravenous dexmedetomidine also attenuates the hemodynamic responses to laryngoscopy and ETI but is associated with risk of bradycardia, hypotension and cardiac arrests [
4,
9,
10,
14,
27,
28]. De Cassai et al. in a recent SRMA of 99 RCTs involving 6833 patients found significant bradycardia in one out of every 12 patients [
4]. Nebulized dexmedetomidine provides an alternative route and was found to be devoid of these intra-operative adverse effects in this SRMA. Our findings corroborate with similar findings by other authors [
14]. The heart rate safety profile of nebulized versus IV dexmedetomidine might be advantageous in patients with low baseline HR such as those on pre-operative beta-blocker therapy [
13,
14]. Also, nebulized dexmedetomidine causes less postoperative sedation than IV dexmedetomidine which may be beneficial in resource-poor settings with inadequate postoperative monitoring facilities and in patients with obstructive sleep apnoea or chronic obstructive pulmonary disease in whom postoperative sedation might be detrimental [
14].
Other potential benefits of nebulized dexmedetomidine, as observed in included studies in this SRMA, involved reduction in the induction dose of propofol, intraoperative requirement of opioids and halogenated anaesthetics and incidence of postoperative sore-throat. However, low number of studies precluded meta-analysis of these outcome. Some of these advantages might be attributed to sedative and analgesic action of dexmedetomidine by virtue of its α2-agonistic action on the locus coeruleus [
3]. Its dose-sparing effect on opioid and anaesthetic requirements have been shown to be comparable with intravenous dexmedetomidine [
14]. Its short half-life and elimination life and easy acceptability in addition to its ability to provide a calm and sedated patient at induction, lower anaesthetic and analgesic requirements and devoid of adverse effects make nebulized dexmedetomidine an ideal premedication agent [
13,
29]. The sedative action of nebulized dexmedetomidine is particularly advantageous in pediatric patients in whom it has been shown to reduce separation anxiety, recovery time, postoperative agitation, postoperative nausea and vomiting and improve mask acceptance; with nebulized dexmedetomidine shown to be better compared with nebulized ketamine and midazolam [
3,
29,
30]. Another recent systematic review of 10 RCTs including 1233 patients established sedative efficacy of nebulized dexmedetomidine in pediatric patients undergoing medical examination or surgery [
3]. Nebulized dexmedetomidine has been shown to ease and improve acceptability of IV cannulation; difficult in pediatric population owing to small veins and physical agitation [
8,
31‐
33]. Postoperative sore throat is a common adverse effect after laryngoscopy and ETI and is associated with patient discomfort and dis-satisfaction after GA [
34]. Congruent with our findings, others have also shown nebulized dexmedetomidine to reduce postoperative sore throat, better than that of IV dexmedetomidine [
14]. This might be attributed to its anti-inflammatory action [
14].
Sensitivity analysis by excluding study using a higher dose of nebulized dexmedetomidine (2 μg/kg) did not reveal any major impact on the pooled effect estimate, suggesting against a dose-response effect. However, only one of the included RCT used a higher dose of dexmedetomidine precluding any conclusion on the dose-response effect of nebulized dexmedetomidine on the hemodynamic stress response. This warrants future studies comparing different doses of dexmedetomidine to confirm or refute any dose-response effect.
Limitations and strengths
This SRMA had few limitations. Exclusion of grey literature search and non-English studies might have led to missing out relevant articles. However, a comprehensive search of six (both uni-and multi-disciplinary) most relevant databases including google scholar (cataloguing both academic and grey literature) along with reference list and citation tracking were adopted to ensure that SR findings are informed by the best available evidence on the topic.
Secondly, only one-third of the included studies were at low risk of bias which reduced our certainty in the strength of evidence. This not only enable readers to view the available evidence in light of its quality but also provides useful insights for future triallists to improve the design and conduct of future RCTs to reduce the risk of biases identified in this SRMA.
Another limitation worth considering is the high heterogeneity observed in the effect estimates. A high I
2 value, for e.g. of 92% for HR at 1 min reflect that 92% of variance in the observed effect is due to variance in true effect and only 8% is due to variance in the sampling error. This was despite the study sample across the studies being quite homogenous with respect to the age, ASA physical status and surgeries as outlined in 3.2. Except for Hussain et al., all others used 1 μg/kg as the dose of dexmedetomidine. A sensitivity analysis performed after excluding Hussain et al. in fact increased the heterogeneity for HR at 1 min (I
2 from 92 to 94%). The main source of clinical heterogeneity evident among the studies was the use of anti-emetics, anti-cholinergic and benzodiazepines as premedication, some of which (e.g. midazolam) have themselves been shown to attenuate hemodynamic response to ETI [
35].
To the best of authors knowledge, this is the first SRMA to systematically and comprehensively evaluate efficacy and safety of dexmedetomidine nebulization for attenuating hemodynamic response to ETI. The strength of this SRMA lies in its transparent and rigorous methodology to identify, collate, appraise and synthesize the available evidence informing the review topic. Key review decisions were made in consultation with the Cochrane Handbook for Systematic Review of Interventions and the project advisory group comprising of both the subject and methodology experts [
36]. Two independent reviewer with arbitration and audit process was adopted at screening, data extraction, meta-analysis, risk of bias and GRADE assessment.
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