World Journal of Emergency Medicine ›› 2019, Vol. 10 ›› Issue (1): 19-26.doi: 10.5847/wjem.j.1920-8642.2019.01.003
Special Issue: Trauma
• Original Articles • Previous Articles Next Articles
Bianca M. Wahlen1, Ayman El-Menyar2,3(), Mohammad Asim2, Hassan Al-Thani4
Received:
2018-07-18
Accepted:
2018-09-20
Online:
2019-03-15
Published:
2019-03-15
Contact:
Ayman El-Menyar
E-mail:aymanco65@yahoo.com
Bianca M. Wahlen, Ayman El-Menyar, Mohammad Asim, Hassan Al-Thani. Rapid sequence induction (RSI) in trauma patients: Insights from healthcare providers[J]. World Journal of Emergency Medicine, 2019, 10(1): 19-26.
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URL: http://wjem.com.cn//EN/10.5847/wjem.j.1920-8642.2019.01.003
Table 1
Comparison for the use of induction agent in trauma patients (n, %)
Induction agent | Total (n=102) | Emergency physicians (n=55) | Anaesthesiologists (n=47) | P value |
---|---|---|---|---|
Stable patients | ||||
Propofol | 76 (74.5) | 31 (56.4) | 45 (95.7) | 0.001 for all |
Etomidate | 21 (20.6) | 20 (36.4) | 1 (2.1) | |
Ketamine | 3 (2.9) | 2 (3.6) | 1 (2.1) | |
Midazolam | 2 (2.0) | 2 (3.6) | 0 (0.0) | |
Unstable patients | ||||
Etomidate | 51 (50) | 35 (63.6) | 16 (34.0) | 0.023 for all |
Ketamine | 25 (24.5) | 11 (20.0) | 14 (29.8) | |
Propofol | 22 (21.6) | 8 (14.5) | 14 (29.8) | |
Midazolam | 4 (3.9) | 1 (1.8) | 3 (6.4) |
Table 2
Comparison for the use of opioid in trauma patients (n, %)
Opioid | Total (n=102) | Emergency physicians (n=55) | Anesthesiologist (n=47) | P value |
---|---|---|---|---|
Stable patients | 0.093 for all | |||
Fentanyl | 94 (93.1) | 49 (89.1) | 45 (97.8) | |
Morphine | 5 (5.0) | 5 (9.1) | 0 (0.0) | |
Remifentanil | 1 (1.0) | 0 (0.0) | 1 (2.2) | |
No opioid | 1 (1.0) | 1 (1.8) | 0 (0.0) | |
Unstable patients | 0.005 for all | |||
Fentanyl | 80 (81.6) | 40 (72.7) | 40 (93.0) | |
Morphine | 2 (2.0) | 2 (3.6) | 0 (0.0) | |
Remifentanil | 2 (2.0) | 0 (0.0) | 2 (4.7) | |
No opioid | 14 (14.3) | 13 (23.6) | 1 (2.3) |
Table 3
Comparison for the use of muscle relaxant in trauma patients (n, %)
Muscle relaxant | Total (n=102) | Emergency physicians (n=55) | Anesthesiologist (n=47) | P value |
---|---|---|---|---|
Stable patients | ||||
Rocuronium | 57 (56.4) | 24 (44.4) | 33 (70.2) | 0.013 for all |
Suxamethonium | 43 (42.6) | 30 (55.6) | 13 (27.7) | |
Cis-Atracurium | 1 (1.0) | 0 (0.00) | 1 (2.1) | |
Unstable patients | ||||
Rocuronium | 62 (62) | 28 (52.8) | 34 (72.3) | 0.081 for all |
Suxamethonium | 36 (36) | 23 (43.4) | 13 (27.7) | |
Cis-Atracurium | 2 (2/0) | 2 (3.8) | 0 (0.0) |
Table 4
Sedative agents for RSI
Parameters | Etomidate | Midazolam | Ketamine | Propofol |
---|---|---|---|---|
Mechanism | Imidazole-derived, it acts directly on the GABA receptor complex, blocking neuroexcitation and producing anesthesia. | Benzodiazepines act on the GABA receptor complex. | It acts at many receptors causing a range of effects. It may stimulate the N-methyl-D-aspartate receptor at the GABA receptor complex, causing neuroinhibition and anesthesia. | It is a highly lipid-soluble, alkylphenol derivative that acts at the GABA receptor causing sedation and amnesia. |
Induction dose | IV push in a dose of 0.3 mg/kg | 0.1 to 0.3 mg/kg IV push | 1 to 2 mg/kg | 1.5 to 3 mg/kg IV |
Time to effect | 15 to 45 seconds | Approximately 30 to 60 seconds | 45 to 60 seconds | Approximately 15 to 45 seconds |
Duration of action | 3 to 12 minutes | 15 to 30 minutes | 10 to 20 minutes | 5 to 10 minutes |
Hemodynamic effect | As the most hemodynamically neutral of the sedative agents, it does not stimulate histamine release. | Midazolam (0.2 mg/kg) causes moderate hypotension, with an average drop in MAP 10% to 25%. | It stimulates catecholamine receptors and release of catecholamines causing increases in HR, contractility, MAP and cerebral blood flow. | It suppresses sympathetic activity, causing myocardial depression and peripheral vasodilation (drops MAP of≈ 10 mmHg) |
Analgesia | No analgesic effect. It does not blunt the noxious stimulation of the upper airway during laryngoscopy and intubation. | It does not provide analgesia but does possess anticonvulsant effects, making it an effective agent for RSI in patients with status epilepticus. | It excites opioid receptors within the insular cortex, putamen, and thalamus, producing analgesia. | No |
Effects | It decreases cerebral blood flow and cerebral metabolic oxygen demand, while preserving cerebral perfusion pressure. It is a sedative-hypnotic agent. It should not be used as an infusion or in repeated bolus doses for maintenance of sedation after intubation. Neuroexcitation can be reduced by postintubation sedation with propofol or a benzodiazepine In CVD or elevated intracranial pressure, it is often given during the pretreatment phase of RSI. | It causes sedation and amnesia. | It is a dissociative anesthetic agent. It provides analgesia along with its amnestic and sedative effects. It decreases the production of vascular nitric oxide, diminishing its vasodilatory effect, and inhibits nicotinic acetylcholine receptor. Ketamine may cause bronchodilation by stimulating the release of catecholamines. It preserves respiratory drive and has both a quick onset of action and analgesic properties. Use for "awake" intubation attempts, but not in paralyzed patients. | It reduces airway resistance. It does not prolong cardiac QT interval. It causes sedation and amnesia, but it does not cause analgesia. Its neuroinhibitory effects allows its use for patients with intracranial pathology (in hemodynamically stable cases). |
Side effects | It is a reversible inhibitor of 11-beta-hydroxylase, which converts 11-deoxycortisol to cortisol. It causes adrenal suppression, myoclonus, and evidence of regional cerebral excitation after intubation. | It induces hypotension. | In patients with hypertension and suspected ICP elevation, ketamine should be avoided. When ketamine is used with a GABA agonist, this rise in ICP may not occur. | |
Use in shock | Yes | No | Yes | No |
Use in bronchospasm | Yes | Yes | ||
Use in significant CVD | Yes | |||
Use in head injury or stroke | Yes | Yes | ||
GABA: gamma amino butyric acid; MAP: mean arterial pressure, HR: heart rate; CVD: cardiovascular disease; Data adopted from [ref 34]. |
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