Methoxyflurane Versus Standard of Care for Acute Trauma-Related Pain in the Emergency Setting: Protocol for a Randomised, Controlled Study in Italy (MEDITA)

An estimated 38 million people attend European Emergency Departments (EDs) each year due to injuries, and many experience pain that is inadequately treated. Currently available painkillers (analgesics) have limitations such as being slow to work (oral medications), requiring needles (intravenous medications) or side effects (e.g., opioids). A new analgesic (methoxyflurane) is available in Europe for emergency relief of moderate-to-severe acute pain due to injury. Methoxyflurane is administered using a disposable hand-held inhaler, through which the patient can inhale and control their own level of analgesia. Methoxyflurane has been used in Australia and New Zealand for over 40 years, with nearly 6 million uses to date, but no large-scale trials have assessed its effectiveness compared with other analgesics in the emergency setting. A new trial (MEDITA—Methoxyflurane in Emergency Department in ITAly) will investigate the effectiveness and safety of methoxyflurane versus standard analgesic treatment in Italian emergency medical centres.

The MEDITA trial will enroll approximately 272 adult patients with limb injuries and/or suspected fractures who have moderate-to-severe pain when they are assessed in the ED or are assisted through the 118 Emergency system (pre-hospital and ambulance service). Patients will be randomly allocated to treatment with inhaled methoxyflurane or standard analgesic treatment; this will be intravenous morphine for patients with severe pain and intravenous paracetamol or ketoprofen for patients with moderate pain. The trial will compare reductions in patients’ pain intensity, how quickly pain relief is achieved, whether additional analgesics are required and the number and type of side effects between the two treatment groups.

The health burden of injury and trauma pain is significant; each year there are an estimated 38 million injury-related emergency department (ED) attendances across the European Union [1]. The prevalence of trauma-related pain has been reported as 70% of patients in the pre-hospital setting [2] and up to 91% in the ED [3, 4], with many patients still experiencing moderate-to-severe pain at discharge [3, 5]. Undertreatment of acute pain (oligoanalgesia) in trauma patients remains a widespread problem in the pre-hospital and ED settings; a study in the pre-hospital setting found the prevalence of oligoanalgesia to be 43% [6], while a study in the ED found that only 35.7% of patients received analgesia and 12.5% received adequate pain management [7]. Reasons for the undertreatment of pain include inadequate or under-assessment of pain, lack of training or guidance on pain management, insufficient time and resources, and reluctance to administer opioids [8‐10].

In Europe, commonly used analgesics for trauma pain include paracetamol, non-steroidal anti-inflammatory drugs (NSAIDs), nitrous oxide (N₂O) and opioids [2, 11], although there are regional and institutional variations. Current analgesics present several limitations in the treatment of trauma pain with respect to their routes of administration, strength of analgesia, side effect profiles and pharmacokinetic properties [8]. Paracetamol and NSAIDs are weak analgesics often used as first-line treatment of mild-to-moderate pain, but onset of action is slow when administered orally, while parenteral administration requires additional resources for cannulation and may be difficult in the pre-hospital emergency setting. There is also risk of overdose if the patient has already self-medicated before receiving medical assistance. N₂O is fast acting, but its canisters are bulky and heavy, making them unwieldy to transport and manoeuvre in emergency situations, [12] and must also be used with caution in patients with chest injury due to the risk or accumulation of gas and rapid worsening of pneumothorax if present [13]. Opioids are a highly effective treatment option for severe pain, but require additional resources for prescribing, administration, monitoring and observation due to their controlled status and challenging safety profile. A recent review has estimated the cost per patient of intravenous (IV) morphine administration in Europe at €18–28 (of which €14–22 is accounted for by workforce costs), rising to €121–132 when morphine-related adverse events (AEs) and IV-related complications are also considered [14]. Furthermore, there is often a general reluctance on the part of healthcare providers to prescribe opioids due to concerns over safety, dependence and abuse. According to the Italian Inter-societary Recommendations (SIAARTI, SIMEU, SIS 118, AISD, SIARED, SICUT, IRC) on emergency pain management, “The ideal pre-hospital analgesic should be simple to use, safe, effective, unaffected by transport times, have a rapid onset, a short duration of action, and be able to be titrated to achieve the desired effect in all patients” [15].

Low-dose methoxyflurane, a non-opioid, volatile fluorinated hydrocarbon, administered via a lightweight, disposable, hand-held inhaler (Penthrox^®; Medical Developments International Limited, Scoresby, Australia) has recently been approved in Europe for the emergency relief of moderate-to-severe pain in conscious adults with trauma and associated pain [16]. While use of methoxyflurane at higher doses for general anaesthesia was discontinued in the 1970s due to concerns about nephrotoxicity [17], administration of lower, analgesic doses of methoxyflurane is not typically associated with renal side effects [18]. Low-dose methoxyflurane has been widely used in Australia and New Zealand for over 40 years for short-term pain relief in both adults and children in emergency medicine, minor surgical and dental procedures [19, 20], with a total of over 5 million administrations worldwide to date [21].

The European approval for low-dose methoxyflurane was primarily based on a UK-based randomised, controlled trial (STOP!), which demonstrated significantly greater reductions in pain intensity, a rapid onset of action (median 4 min), along with significantly less use of rescue medication and high patient satisfaction with methoxyflurane compared with placebo in 300 patients aged ≥ 12 years with acute trauma pain [22], as well as in the adult-only subgroup [23]. With the exception of two smaller studies versus intramuscular tramadol [24] and placebo [25], other clinical data supporting low-dose methoxyflurane in the treatment of trauma pain are mainly from real-world observational or retrospective studies outside Europe [26‐30]. There is a need for better evidence from randomised trials using clinically relevant active controls. Therefore, a randomised controlled trial aiming to investigate the efficacy and safety of low-dose methoxyflurane analgesia compared with standard of care (SoC) in the treatment of acute trauma-related pain has been initiated in emergency units in Italy and is described in this paper.

Inhaled analgesic methoxyflurane has a number of characteristics that make it an attractive option as a pre-hospital and ED analgesic. It is portable, non-invasive, non-narcotic, simple to use and the patient can manage their own level of analgesia [16]. The STOP! study demonstrated a fast onset of pain relief for methoxyflurane (within 4 min) [22], comparable with the onset of both IV morphine [41] and inhaled N₂O [42], and high patient satisfaction with the efficacy and tolerability of treatment. Methoxyflurane does not interfere with most other anaesthetic or analgesic agents, and its effects are rapidly reversed once inhalation stops (within 3–20 min), thus it does not limit subsequent assessment and treatment options [16]. Low-dose methoxyflurane analgesia may therefore address an unmet need in the emergency setting and provide simple, fast and effective pain relief able to avoid unnecessary suffering and improve patient flow. With methoxyflurane having recently been licensed in Europe for use in adult patients with trauma-associated pain, it is anticipated that the results of this study, along with findings of other recent studies [34, 43], can provide additional clinical evidence to help inform treatment choices for acute trauma-related pain in the ED.