Effectiveness and Adverse Events of Gabapentinoids as Analgesics for Patients with Burn Injuries: A Systematic Review with Meta-Analysis and Trial Sequential Analysis
Abstract
:1. Introduction
2. Materials and Methods
2.1. Protocol and Registration
2.2. Search Strategy
2.3. Selection Criteria
- (i)
- Population: patients with burn wounds;
- (ii)
- Intervention: gabapentinoids (gabapentin, pregabalin or mirogabalin);
- (iii)
- Comparison: control group regimen;
- (iv)
- Outcomes: (a) pain score, (b) opioid consumption and (c) adverse effects.
2.4. Data Extraction
2.5. Statistical Analysis
2.6. Quality Assessment and Certainty of Evidence
3. Results
3.1. Literature Search
3.2. Study Characteristics
3.3. Risk of Bias Assessment
3.4. Primary Outcomes: Pain Score
3.5. Primary Outcomes: Opioid Consumption
3.6. Secondary Outcomes: Adverse Events
3.7. CoE by GRADE Methodology
4. Discussion
5. Conclusions
Supplementary Materials
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Acknowledgments
Conflicts of Interest
Appendix A
References
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Participants Characteristics | Interventions | Comparison | Outcomes | |||||||
---|---|---|---|---|---|---|---|---|---|---|
Study | Year | Country | Funding | Study Design | Baseline Analgesics | Experimental Groups (n) | Administration | Control Group (n) | Outcome Analysed | Study Follow-Up |
Gray et al. [17] | 2011 | Australia | Pfizer Australia and Royal Brisbane and Women’s Hospital Foundation | Single-centre, double-blind RCT (ISRCTN56448626) | Acetaminophen, opioid (oral, PCA) | Pregabalin (34) | 75 mg–300 mg BID, PO, 28 days * | Placebo (33) | NPS (0–10) Opioid consumption | Weekly, up to 4 weeks |
Rimaz et al. [19] | 2012 | Iran | None declared | Double-blind, placebo-controlled RCT | IV morphine (PCA) | Gabapentin (25) | 1200 mg, single dosing, PO | Placebo (25) | VAS (0–100) Opioid consumption Adverse effects | 24 h |
Wibbenmeyer et al. [21] | 2014 | USA | None declared | Single-centre, double-blind, placebo-controlled RCT (NCT01265056) | Acetaminophen, NSAIDs and morphine | Gabapentin (27) | 1200 mg once, followed by 300–1200 mg TID, PO * | Placebo (26) | NRS (0–10) Adverse effects | Pain: day 3 or discharge Opioids: until first clinic visit |
Juozapavičienė et al. [20] | 2015 | Lithuania | None declared | Single-centre, parallel-designed RCT | IV morphine (PCA) | Gabapentin (24) | 1200 mg/day PO | Control (29) | VAS (0–100) Opioid consumption Adverse effects | Up to 72 h |
Jones et al. [18] | 2019 | USA | Pfizer Inc. | Single-centre, double-blind, placebo-controlled RCT | IV and oral opioids | Pregabalin (32) | 150 mg BID PO * 300 mg BID PO * | Placebo (19) | VAS (0–100) Opioid consumption Adverse effects | Days 9, 25, 90 and 180 |
Adverse Events | Gabapentin | Pregabalin | Pooled | LFK Index | ||||
---|---|---|---|---|---|---|---|---|
No. of Trials | RR (95% CI) IVhet Model | Bayesian Analysis (95% CrI) | No. of Trials | RR (95% CI) IVhet Model | RR (95% CI) IVhet Model | Bayesian Analysis (95% CrI) | ||
Dizziness | 3 | 3.035 (0.925, 9.952) | 1.62 (0.338, 6.28) | 1 | 3.030 (0.153, 59.967) | 3.034 (1.006, 9.147, I2 = 0%) | 1.58 (0.413, 5.25) | −2.69 |
Nausea | 3 | 0.791 (0.358, 1.750) | 0.628 (0.256, 1.43) | 1 | 0.202 (0.009, 4.724) | 0.729 (0.338, 1.575, I2 = 0%) | 0.419 (0.075, 1.33) | −2.93 |
Drowsiness | 3 | 3.255 (1.135, 9.335) | 1.69 (0.285, 6.06) | 0 | N/A | 3.255 (1.135, 9.335, I2 = 0%) | 1.69 (0.285, 6.06) | −4.38 |
Diarrhoea | 2 | 0.359 (0.034, 3.831) | 1.01 × 10−0.7 (8.79 × 10−21, 0.125) | 0 | N/A | 0.359 (0.034, 3.831, I2 = 0%) | 1.01 × 10−0.7 (8.79 × 10−21, 0.125) | N/A |
Constipation | 2 | 0.993 (0.183, 5.394) | 0.806 (0.340, 2.20) | 0 | N/A | 0.993 (0.183, 5.394, I2 = 0%) | 0.806 (0.340, 2.20) | N/A |
Urinary retention | 3 | 1.542 (0.260, 9.135) | 0.475 (0.0633, 2.67) | 0 | N/A | 1.542 (0.260, 9.135, I2 = 0%) | 0.475 (0.0633, 2.67) | −0.39 |
Pruritus | 3 | 1.094 (0.329, 3.641) | 0.337 (0.0343, 2.06) | 1 | 0.119 (0.015, 0.942) | 0.625 (0.134, 2.908, I2 = 38%) | 0.444 (0.0643, 1.98) | −2.11 |
Certainty Assessment | No. of Patients | Effect | Certainty | |||||||
---|---|---|---|---|---|---|---|---|---|---|
No. of Studies | Study Design | Risk of Bias | Inconsistency | Indirectness | Imprecision | Other Considerations | Gabapentinoids | Control | Absolute (95% CI) | |
Pain score reduction 24 h | ||||||||||
3 | Randomised trials | Very serious a | Not serious | Not serious | Not serious | Publication bias strongly suspected b | 76 | 80 | MD 1.06 lower (1.47 lower to 0.65 lower) | ⨁◯◯◯ Very low |
Pain score reduction 72 h to 9 days | ||||||||||
3 | Randomised trials | Serious c | Not serious | Not serious | Not serious | Publication bias strongly suspected b | 102 | 92 | MD 0.82 lower (1.16 lower to 0.48 lower) | ⨁⨁◯◯ Low |
Pain score reduction 3 weeks | ||||||||||
2 | Randomised trials | Serious d | Not serious | Not serious | Very serious e | Publication bias strongly suspected b | 78 | 63 | MD 0.44 lower (1.31 lower to 0.42 higher) | ⨁◯◯◯ Very low |
Opioid consumption 24 h | ||||||||||
2 | Randomised trials | Very serious a | Not serious | Not serious | Not serious | Publication bias strongly suspected b | 49 | 54 | MD 13.34 mg/day lower (22.16 lower to 4.52 lower) | ⨁◯◯◯ Very low |
Opioid consumption 72 h to 9 days | ||||||||||
3 | Randomised trials | Very serious f | Not serious | Not serious | Not serious | Publication bias strongly suspected b | 102 | 92 | MD 7.87 mg/day lower (14.82 lower to 0.91 lower) | ⨁◯◯◯ Very low |
Opioid consumption 3 weeks | ||||||||||
1 | Randomised trials | Serious d | Not serious | Not serious | Serious g | None | 46 | 44 | MD 2.12 mg/day fewer (9.74 fewer to 5.5 more) | ⨁⨁◯◯ Low |
Certainty Assessment | No. of Patients | Effect | Certainty | ||||||||
---|---|---|---|---|---|---|---|---|---|---|---|
No. of Studies | Study Design | Risk of Bias | Inconsistency | Indirectness | Imprecision | Other Considerations | Gabapentinoids | Control | Relative (95% CrI) | Absolute (95% CrI) | |
Dizziness | |||||||||||
4 | Randomised trials | Very serious a | Not serious | Not serious | Very serious b | Publication bias strongly suspected c | 11/108 (10.2%) | 3/99 (3.0%) | RR 1.58 (0.41 to 5.25) | 18 more per 1000 (from 18 fewer to 129 more) | ⨁◯◯◯ Very low |
Nausea | |||||||||||
4 | Randomised trials | Very serious a | Not serious | Not serious | Serious d | Publication bias strongly suspected c | 8/108 (7.4%) | 12/99 (12.1%) | RR 0.419 (0.075 to 1.330) | 70 fewer per 1000 (from 112 fewer to 40 more) | ⨁◯◯◯ Very low |
Drowsiness | |||||||||||
3 | Randomised trials | Very serious a | Not serious | Not serious | Very serious b | Publication bias strongly suspected c | 17/76 (22.4%) | 6/80 (7.5%) | RR 1.690 (0.285 to 6.060) | 52 more per 1000 (from 54 fewer to 379 more) | ⨁◯◯◯ Very low |
Diarrhoea | |||||||||||
2 | Randomised trials | Very serious a | Not serious | Not serious | Serious d | None | 0/52 (0.0%) | 2/51 (3.9%) | RR 0.000 (0.000 to 0.125) | -- per 1000 (from 34 fewer to --) | ⨁◯◯◯ Very low |
Constipation | |||||||||||
2 | Randomised trials | Very serious a | Not serious | Not serious | Serious d | None | 2/52 (3.8%) | 2/51 (3.9%) | RR 0.806 (0.340 to 2.200) | 8 fewer per 1000 (from 26 fewer to 47 more) | ⨁◯◯◯ Very low |
Urinary retention | |||||||||||
3 | Randomised trials | Very serious a | Not serious | Not serious | Very serious b | None | 2/76 (2.6%) | 1/80 (1.3%) | RR 0.4750 (0.0633 to 2.6700) | 7 fewer per 1000 (from 12 fewer to 21 more) | ⨁◯◯◯ Very low |
Pruritus | |||||||||||
4 | Randomised trials | Very serious a | Not serious | Not serious | Serious d | Publication bias strongly suspected c | 5/108 (4.6%) | 5/99 (5.1%) | RR 0.4440 (0.0643 to 1.9800) | 28 fewer per 1000 (from 47 fewer to 49 more) | ⨁◯◯◯ Very low |
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Chiang, L.-J.; Lai, P.-C.; Huang, Y.-T. Effectiveness and Adverse Events of Gabapentinoids as Analgesics for Patients with Burn Injuries: A Systematic Review with Meta-Analysis and Trial Sequential Analysis. J. Clin. Med. 2023, 12, 5042. https://doi.org/10.3390/jcm12155042
Chiang L-J, Lai P-C, Huang Y-T. Effectiveness and Adverse Events of Gabapentinoids as Analgesics for Patients with Burn Injuries: A Systematic Review with Meta-Analysis and Trial Sequential Analysis. Journal of Clinical Medicine. 2023; 12(15):5042. https://doi.org/10.3390/jcm12155042
Chicago/Turabian StyleChiang, Liang-Jui, Pei-Chun Lai, and Yen-Ta Huang. 2023. "Effectiveness and Adverse Events of Gabapentinoids as Analgesics for Patients with Burn Injuries: A Systematic Review with Meta-Analysis and Trial Sequential Analysis" Journal of Clinical Medicine 12, no. 15: 5042. https://doi.org/10.3390/jcm12155042
APA StyleChiang, L. -J., Lai, P. -C., & Huang, Y. -T. (2023). Effectiveness and Adverse Events of Gabapentinoids as Analgesics for Patients with Burn Injuries: A Systematic Review with Meta-Analysis and Trial Sequential Analysis. Journal of Clinical Medicine, 12(15), 5042. https://doi.org/10.3390/jcm12155042