Efficacy and Safety of Penthrox® Combined With a Standard Analgesia (SoC) in Adult Patients Admitted to the Emergency Department With Moderate to Severe Pain Associated With Trauma

Mundipharma SAS360 enrolled

Overview

A phase 4 randomised, double-blind study to assess the efficacy and safety of Penthrox® used from the outset in multimodal analgesia, in combination with the standard analgesic protocol used in the department, for conscious adult patients presenting in an emergency department with moderate to severe pain associated with a trauma

On admission, the patient pain score will be measured using a numerical scale (NRS-11) to verify the eligibility of the patient in the study (NRS ≥ 4). At the time of randomisation, the patient's pain score will be measured using a VAS in order to verify the patient's eligibility for randomisation (VAS ≥ 40). Admissible patients will be randomised by IWRS (Interactive Web Response System) to receive: * Either Penthrox® + SoC * Or placebo + SoC (Figure 1). Randomisation will be stratified by sex, site and according to the baseline pain score (NRS 4-5 for a moderate-intensity pain versus NS 6-10 for a severe-intensity pain). The IWRS system will be based on the fact of including 50% patients with moderate pain and 50% patients with severe pain. Close weekly monitoring of this ratio will be set up. The decision to no longer include patients in one of the study subgroups according to pain, if necessary, or to change this ratio, will be made by the Study Sponsor and in agreement with the study investigator-coordinator and the study scientific committee. A minimum of 150 patients will be included in the severe pain subgroup (EN 6-10). The treatment (preparation of two inhalers, the second only being given to the patient on request) will only be administered once intermittently or continuously to patients on admission to the study (D0, T0). The pain score will be assessed using the VAS every 5 minutes up to 20 minutes, then at 30, 60, 90, and 120 minutes after the start of study treatment (T0). Patients will be assessed until their discharge from the emergency departments (hospitalization, transfer home, transfer to the operating room) or up to 120 minutes after the initial administration. A telephone interview will take place 14 (± 2) days after the first treatment administration to assess the medium-term safety of the product.

Study Type

INTERVENTIONAL

Allocation

RANDOMIZED

Purpose

TREATMENT

Masking

QUADRUPLE

Enrollment

360

Conditions

Pain, Acute

Interventions

MethoxyfluraneDRUG

PENTHROX 3mL inhalation vapour, liquid

Normal SalineDRUG

Placebo

Eligibility

Sex: ALLMin age: 18 Years

Medical Language ↔ Plain English

Inclusion Criteria: * Men and women aged 18 or older * Patients (in an emergency, parent or relative) who dated and signed their informed consent to participate in the study * Patients admitted to the emergency department due to a trauma * Patients having a pain score ≥ 4 measured using a numerical scale (NRS) at the time of admission to emergency departments. * Patients having a pain score ≥ 40 measured using the VAS at the time of randomisation. Exclusion Criteria: * Life-threatening conditions requiring immediate admission to the operating theatre or the intensive care unit; * Impaired consciousness according to the investigator regardless of the cause, including head trauma or drug or alcohol consumption; * Acute medicinal or alcohol intoxication, according to the investigator; * Pregnant woman or woman at risk of pregnancy and not using highly effective contraception methods or known lactation; * Analgesic treatment within 5 hours (8 h for sodium diclofenac) prior to admission, except for paracetamol, which is allowed; * Treatment with nitrous oxide within 5 hours before presentation at the emergency department; * Use of analgesics for chronic pain; * Prior use of Penthrox®; * Use of an investigational product one month before presentation at the emergency department; * Hypersensitivity to Penthrox® or any other fluoridated anesthetic; * History of signs of hepatic lesions after use of methoxyflurane or after anaesthesia by a halogenated hydrocarbon; * Malignant hyperthermia: Known malignant hyperthermia or patient genetic predisposition or patient or family history of serious adverse reactions; * Clinical evidence of respiratory depression according to the investigator; * Clinical evidence of cardiovascular instability according to the investigator; * Clinical renal or hepatic damage, according to the investigator, pre-existing or known; * Presence of any other clinical condition that can, according to the investigator's opinion, have an impact on the patient's ability to participate in the study or the results of the study. * Individuals protected by law

Locations (8)

CH Annecy Genevois

Annecy, France

GH Carnelle Porte de l'Oise

Beaumont-sur-Oise, France

Hôpital Avicenne - APHP

Bobigny, France

CHRU Lille

Lille, France

Outcomes

Primary Outcomes

time until pain relief defined by the duration between the start of the study treatment (T0) and pain relief

Measured on Pain intensity visual analogue scale (PI-VAS) 0-100 where 100 is the highest pain

Time frame: through study completion, maximum of 2 hours

Secondary Outcomes

Duration between the start of study treatment (T0) and pain relief reported by the patient

Pain measured on PI-VAS, 0-100 where 100 is the highest pain

Time frame: through study completion, maximum of 2 hours

Absolute Pain Intensity Difference (PID) measured using the PI-VAS at 5, 10, 15, 20 and 30 minutes after T0

PID for a given assessment time is equal to the VAS score at T0 minus the VAS score at each assessment time provided in the study. Pain measured on PI-VAS, 0-100 where 100 is the highest pain

Time frame: baseline to 5, 10, 15, 20 and 30 minutes

Relative Pain Intensity Difference measured using the PI-VAS at 5, 10, 15, 20 and 30 minutes after T0

Relative pain intensity difference for a given assessment time is equal to the VAS score at T0 minus the VAS score at each assessment time provided in the study divided by the VAS score at T0. Pain measured on PI-VAS, 0-100 where 100 is the highest pain

Time frame: baseline to 5, 10, 15, 20 and 30 minutes

Pain relief defined by pain intensity < 40 mm on the PI-VAS scale at 5, 10, 15, 20 and 30 minutes after T0

Pain measured on PI-VAS, 0-100 where 100 is the highest pain

Time frame: baseline to 5, 10, 15, 20 and 30 minutes

Response defined by pain reduction of 20 mm on the PI-VAS at 5, 10, 15, 20 and 30 minutes after T0

Pain measured on PI-VAS, 0-100 where 100 is the highest pain

Data from ClinicalTrials.gov

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