Journal List > Clin Endosc > v.55(5) > 1516079463

Lee, Park, Park, Park, Bae, Seo, Lee, Chon, Chung, Choi, Lee, Kim, and Endoscopic Sedation Committee of the Korean Society of Gastrointestinal Endoscopy: New sedatives and analgesic drugs for gastrointestinal endoscopic procedures

Abstract

Procedural sedation has become increasingly common in endoscopy. Sedatives and analgesics induce anxiolysis and amnesia. In addition, an appropriate level of sedation is necessary for safe procedures including therapeutic endoscopy. Midazolam and propofol are the most commonly used drugs in sedative endoscopy. In recent years, the need to ascertain the safety and effectiveness of sedation has increased in practice. Therefore, new sedatives and analgesic drugs for optimal sedative endoscopy, have recently emerged. This article reviews the characteristics of sedatives and analgesics, and describes their clinical use in gastrointestinal endoscopy.

INTRODUCTION

Endoscopy plays a significant role in the diagnosis and treatment of gastrointestinal diseases. Sedation has been used in clinical practice to make the procedure more comfortable, and improve patient satisfaction by helping patients rest during the procedure. Although sedation is widely used for these benefits, it continues to pose some potential risks, requiring medical teams to closely monitor patients during the procedure. Currently, the most widely used agents for endoscopic sedation in Korea are midazolam and propofol.1 Propofol is commonly used for intravenous anesthesia in outpatient surgeries and examinations, due to advantages such as rapid induction and early return of consciousness. However, propofol also has disadvantages as it decreases both cardiovascular and respiratory parameters and lacks antagonists.2 The side effects of midazolam include hypoxemia, paradoxical responses, and delayed recovery. Therefore, there is a need for alternatives.3
Recently, newer sedatives that overcome these drawbacks have been discovered and subsequently applied in endoscopic sedation. New drugs such as etomidate, dexmedetomidine, and remimazolam, have emerged, and the benefits of ketamine and remifentanil have also been highlighted.4,5 This review will therefore discuss etomidate and other new sedatives that are receiving attention in clinical practice.

ETOMIDATE

Etomidate is a short-acting intravenous anesthetic that is indicated for the induction of anesthesia and sedation during short procedures. It is an imidazole derivative that acts as a gamma-aminobutyric acid (GABA)-A receptor agonist in the central nervous system to induce sedation. The drug is mainly distributed by binding to albumin in blood plasma, inducing the opening of the chlorine ion permeation channels of GABA-A receptors and amplifying the action of GABA for rapid sedation.6 Although etomidate is often compared with propofol, it was widely used in the field of general anesthesia even before the development of propofol. Its duration of action is slightly shorter than that of propofol because etomidate is redistributed to peripheral tissues such as muscles, and is metabolized by hepatic and plasma esterases. The resulting carboxylate metabolites are mostly excreted through the urine and bile, exhibiting an elimination half-life of 2–5 hours. Etomidate has an onset of action of 30–60 seconds, with peak effect at approximately 1 minute. Additionally, its action lasts for approximately 3–5 minutes, showing pharmacokinetic properties similar to those of propofol. When using etomidate, initial studies have recommended an induction dose of 0.1–0.2 mg/kg with additional 0.05 mg/kg every 3–5 minutes for maintenance. Although there are no dosage recommendations for etomidate in endoscopic sedation, sedation is mainly achieved using intermittent injections with an induction dose of 0.05 mg/kg, and additional 0.03–0.05 mg/kg for maintenance, in adult patients. In clinical practice, etomidate is mainly used in intensive care units and emergency medicine because it has a lower risk of respiratory depression or hypotension than other intravenous anesthetics.7-9 Thus, the advantages of etomidate include fast recovery, reduced impact on the cardiovascular system, and reduced respiratory failure. However, its disadvantages include pain associated with the injection as well as myoclonus. Additional administration of midazolam (0.015 mg/kg), magnesium sulfate, fentanyl (100–500 μg), or remifentanil (1 μg/kg) with etomidate may reduce the risk of myoclonus.7 The combination of propofol and etomidate can reduce the adverse effects of propofol or etomidate alone.10,11 Etomidate was approved in February 1999 by the US Food and Drug Administration (FDA) as an anesthetic agent.

DEXMEDETOMIDINE

Dexmedetomidine is a highly selective α2 agonist used for sedation in various procedures. It is 7–8 times more selective for the α2 receptor than clonidine.12 It is an anxiolytic, sedative, and pain reliever with an elimination half-life of approximately 2 hours and a distribution half-life of approximately 6 minutes. Dexmedetomidine activates 2-adrenoceptors and causes a decrease in sympathetic tone, with associated attenuation of neuroendocrine and hemodynamic responses to anesthesia; it also reduces anesthetic and opioid requirements. There are several review articles and meta-analyses of dexmedetomidine in the field of endoscopic sedation.13-16 The usual dose used for sedation is 1 μg/kg for 6–10 minutes, followed by an intravenous infusion of 0.5–0.8 μg/kg/hr. However, some patients may require combined sedation with midazolam (0.5–1 mg).17 Dexmedetomidine is considered safe for administration to patients with spontaneous breathing, while ensuring that chin lift maneuvers are performed to maintain their stable breathing. Patients receiving dexmedetomidine are easy to arouse and are less likely to develop delirium than those receiving midazolam.18 However, it still has adverse effects, including bradycardia and hypotension. Therefore, caution should be exercised when administering it to patients with bradycardia, arrhythmia, heart failure, and/or hypotension.19 In some cases, maintenance doses are prescribed without a loading dose. Although dexmedetomidine has fewer adverse effects on respiratory function than propofol, it bears the risk of inducing insufficient sedation during endoscopic procedures.14,15,20 In summary, dexmedetomidine may be useful for diagnostic endoscopy; additional agents, such as midazolam or fentanyl, may be required for more time-consuming procedures such as therapeutic endoscopy. Considering all of these, dexmedetomidine was approved in December 1999 by the FDA as a short-term sedative and analgesic.

REMIMAZOLAM

Remimazolam is a short-acting benzodiazepine used to induce and maintain procedural sedation. Remimazolam modulated the effects of GABA-A receptors to enhance the effects of GABA. The half-life of remimazolam is not prolonged after discontinuing continuous infusion.21 Therefore, the use of remimazolam as an analgesic in intensive care units offers some advantages over fentanyl. Unlike other sedatives that are mainly metabolized in the liver, remimazolam is metabolized by tissue esterases, regardless of their location in the body. Thus, it may be administered regardless of body weight, rapidly metabolizing in blood plasma and tissues.22 Remimazolam was observed to be well tolerated and effective after a single dose of 0.1–0.2 mg/kg or an initial dose of 5.0 mg during endoscopic procedures.23,24 If necessary, supplemental doses of 2.5 mg can be administered. However, at least 2 minutes must have elapsed after the initial dose, prior to the administration of any supplemental dose. Its onset of action is 1–3 minutes and its half-life is 7–8 minutes, which is slightly shorter than that of midazolam, and remains consistent even during continuous intravenous infusion. As such, patients recover quickly after discontinuation of remimazolam infusion. Notably, the benzodiazepine receptor antagonist flumazenil can be used to reverse the sedative effects associated with overdosing. Although the sedative efficiency of remimazolam is higher than that of midazolam, it is slightly lower than that of propofol.25 In a meta-analysis comparing remimazolam and midazolam, the remimazolam group showed excellent results in terms of procedure success rates, proper sedation maintenance, and use of antagonistic drugs.26 However, apnea or chest stiffness was observed in rare cases. In severe cases, chest or thoracic stiffness may affect jaw muscles. Remimazolam was approved for use by the FDA in July 2020; however, it should be used with caution, even during sedation, due to the risk of respiratory failure and hypoxia.

KETAMINE

Ketamine is a phencyclidine derivative that was first used in clinical practice in 1965.27 It is a rapid-acting general anesthetic and N-methyl-d-aspartate receptor antagonist. In terms of pharmacokinetics, ketamine fits a two-compartment model. Plasma concentration after intravenous infusion decreases rapidly at the early stage, which results in a slow elimination and distribution period that is suitable for endoscopy.28 Ketamine is mainly metabolized in the liver and its major metabolite is norketamine. It has an onset of action of less than 1 minute, reaching its peak effect at approximately 1 minute. Its action lasts for approximately 10–15 minutes, and the recommended induction dose is 0.5 mg/kg. Additional doses may be administered to patients after observing their degree of sedation. Ketamine is beneficial in preserving breathing and airway reflexes during endoscopy. The anesthetic state it produces has been termed “dissociative anesthesia” as it appears to selectively interrupt association pathways of the brain before producing a somesthetic sensory blockade. Ketamine also has anti-vagal effects; it increases the secretion of endogenous catecholamines, leading to excellent cardiopulmonary stability. Despite these advantages, the usefulness of ketamine as a sedative is limited because 10%–30% of patients experience hallucinations, visual distortions, and the sensation of floating during the recovery period. It is also associated with a 0.3% incidence of laryngospasms during endoscopic procedures. In the field of anesthesia, ketamine is usually administered with diazepam or midazolam. Currently, a combined administration of ketamine and midazolam is recommended for sedation rather than ketamine alone.29 In clinical practice, ketamine is considered as a useful drug with a low risk of apnea during pediatric sedation.30 The combination of midazolam and ketamine was most commonly used for pediatric endoscopic procedures. In procedural sedation for pediatric endoscopy, the sedation with midazolam 0.03 mg/kg + ketamine 0.65 mg/kg + propofol 2.5 mg/kg performed by an anesthesiologist was deeper and safer with fewer complications.31

FOSPROPOFOL

Fospropofol is a sedative-hypnotic agent used for monitored sedation during anesthesia care. It is a water-soluble prodrug of propofol, which is metabolized into propofol, formaldehyde, and phosphate by endothelial alkaline phosphatase.32 Due to these pharmacokinetic properties, it exhibits the same rise in blood concentration as propofol. However, the effect of fospropofol persists for 15–30 minutes, and its excretion is slightly slower than that of propofol. Its disadvantages include the risk of cardiovascular and respiratory failure, which are similar to those of propofol. Additionally, side effects include itching and perineal pain. Some studies have been conducted on its use in endoscopic sedation, with one study attempting sedation with various concentrations (2, 5, 6.5, or 8 mg/kg) in colonoscopic procedures.33 This study showed a high success rate for moderate sedation in patients who received 6.5 mg/kg, and the results were positive in terms of doctor and patient satisfaction. Although the FDA approved the use of fospropofol in May 2008, it was later required in December 2008 that it be used only by individuals trained in the administration of general anesthesia. Therefore, it is usually indicated for monitored anesthesia care sedation.

REMIFENTANIL

Remifentanil is a short-acting opioid analgesic and μ-opioid receptor agonist. It is metabolized by plasma and tissue esterases, and it has a short context-sensitive half-life of approximately 1–20 minutes.5 The metabolism of remifentanil is unaffected by changes in renal function; therefore, it is easier to predict its clinical action and corresponding recovery period of the patient. It typically induces slight amnesic effects. The optimal induction dose of remifentanil is 0.1–0.2 μg/kg for 2 minutes, and its maintenance dose is 0.025–0.1 μg/kg/min. Administering 0.5–2 mg of midazolam 2–3 minutes before remifentanil administration may lead to better sedative and amnesic effects. Its sedative effect persists for 3–6 minutes, and several studies have shown that it is effective in reducing pain during endoscopy, especially when it is necessary for the patient to remain conscious during colonoscopy.34 The opioid activity of remifentanil is antagonized by opioid antagonists such as naloxone. Compared to midazolam and meperidine for sedation during colonoscopy, remifentanil shows increased hemodynamic stability, reduced respiratory inhibition, faster recovery, and shorter discharge times.35 Considering these, remifentanil was approved by the US FDA in July 1996.

OLICERIDINE

Oliceridine is a new μ-opioid receptor agonist that avoids beta-arrestin pathways and enhances G-protein-coupled signaling pathways to exert analgesic effects.36 It acts through downstream signaling pathways to exert anti-nociceptive analgesia in patients experiencing severe acute pain. Oliceridine is primarily metabolized hepatically by CYP3A4 and CYP2D6.37 It shows significant analgesic benefits within 5–20 minutes of administration, with a half-life of approximately 1.3–3 hours. No dose adjustment was required for patients with renal impairment. Additionally, regardless of the patient’s body weight, sex, and age, the recommended dose is 1–3 mg by intravenous administration. If necessary, supplemental doses of 1 mg may be administered 15 minutes after the loading dose, for maintenance. Its onset of action of approximately 5 minutes is slightly slower than that of fentanyl. Oliceridine offers analgesic effects and has a reduced propensity to cause side effects associated with conventional opioids, including nausea, vomiting, respiratory failure, and/or constipation.38 Respiratory depression after administration of oliceridine is rare, particularly when using small doses. When administered with propofol as a sedative agent, it maintains sedation and reduces the required amount of propofol, thereby lowering the risk of cardiovascular side effects and respiratory failure. The combination of oliceridine and remimazolam is expected to have positive effects during colonoscopy. Its distribution tends to increase in patients with hepatic impairment, but this does not seem to have any effect on excretion.39 Therefore, oliceridine may be used in patients with hepatobiliary diseases. Oliceridine received the FDA’s breakthrough therapy designation in 2016 and was approved by the FDA in August 2020.37

CONCLUSIONS

Table 1 summarized the characteristics of sedative and analgesic drugs for gastrointestinal endoscopic procedure. Many endoscopists are looking for ideal drugs to be used in endoscopic sedation. Drugs such as etomidate, remimazolam, and dexmedetomidine may be useful for endoscopic sedation and may help improve procedural sedation in the future. However, it is also critical to understand the characteristics of these drugs and be aware of their strengths and risks in order to adequately prepare countermeasures. Considering the advantages and disadvantages of old and new drugs, it is necessary to have a thorough understanding of conventional drugs, before considering the introduction and application of new drugs, and to actively cope with recommended changes directed towards the most ideal sedation practice.

Notes

Conflicts of Interest

The authors have no potential conflicts of interest.

Funding

None.

Author Contributions

Conceptualization: JML, JKL, BWK; Data curation: YP, JMP, HHC, JYB; Formal analysis: HJP, JWC; Investigation: JML, YP, JYB; Methodology: JMP, SYS, JHL; Project administration: HJP, JWC, JKL, BWK; Resources: YP, JYB, SYS, JHL; Software: JWC, HKC, HHC; Supervision: JKL, BWK; Validation: HKC, SYS, JWC; Visualization: HJP, HKC, HHC; Writing–original draft: JML; Writing–review & editing: all authors.

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Table 1.
Characteristics of sedative and analgesic drugs for gastrointestinal endoscopic procedure
Drug Initial dose Repeat dose Onset Duration Pros Cons Reversal agent Analgesic effect
Etomidate 0.15 mg/kg 0.05 mg/kg q 2 min 30–60 sec 3–5 min Fast onset of action Myoclonus - -
Hemodynamic stability Adrenal suppression
Low risk of respiratory depression
Dexmedetomidine 1 μg/kg Continuous infusion of 0.2–0.7 μg/kg/hr 1 min 2–4 hr Ability to preserve spontaneous ventilation Slow onset and slow offset of effect Atipamezole ++
Remimazolam 0.05–0.075 mg/kg 0.2 mg/kg 30–60 sec 3–5 min Fast onset of action Flumazenil -
Short recovery time
Ketamine 1–2 mg/kg IV 0.5 mg/kg q 2 min 30–120 sec 15–30 min Analgesic effect Hallucination - ++
Ability to preserve spontaneous ventilation Increased salivation
Fospropofol 6.5 mg/kg 1.6 mg/kg 4–8 min 2–16 min Aqueous formulation Currently not available - -
Remifentanil 0.1–0.3 μg/kg 0.025–0.1 μg/kg/min 30–60 sec 3–6 min Hemodynamic stability Naloxone +++
Low risk of respiratory depression
Short recovery time
Oliceridine 1–3 mg 1 mg 5–20 min 1–3 hr No dose adjustment Slightly slow onset Naloxone +++
Low risk of respiratory depression

-, none; +, weak; ++, moderate; +++, strong; IV, intravenous.

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