Comparison of Lormetazepam and Midazolam Used as Sedatives for Patients That Require Intensive Care

Phase 4

Completed

• Conditions: Sedation in Intensive Care Unit Patients
• Interventions: Drug: Lormetazepam; Drug: Midazolam

• Registration Number: NCT02022592
• Lead Sponsor: Claudia Spies

Brief Summary

A goal directed , demand-driven administration of sedative drugs is an integral part of every intensive care treatment. During long-term application of sedatives, Midazolam is the most commonly used sedative in Europe.

One major objective is the problem of oversedation and agitation during an intensive care treatment due to the lack of controllability of available substances.

The Love-Mi RCT investigates the clinical controllability of Midazolam versus the newly available intravenous drug Lormetazepam.

Detailed Description

Midazolam is almost exclusively metabolized intrahepatically. The methyl-group at position 1 of the imidazole ring is oxidized by liver enzymes. The product is a-OH-midazolam. This reaction is catalyzed by a p450-dependent oxidase in the liver.

Active a-OH-midazolam is inactivated by a biotransformation type II reaction after conjugation. The water soluble, conjugated midazolam can be excreted by the kidney.

During an intensive care treatment, the p450 dependent metabolization is known to be a "bottleneck of elimination" as many drugs are inactivated by this pathway.

As the phase II (glucuronidation) is non-saturable in practice - the phase I reaction limits the metabolic capacity. This leads to unpredictable prolongation of midazolam effects.

In contrast, Lormetazepam is glucuronized directly at its OH-group during a phase II reaction. Since the glucuronidation is non-saturable, Lormetazepam is metabolized with nearly constant kinetics even if repeatedly administered.

Due to the pharmacokinetics we hypothesize that Lormetazepam has an improved controllability compared to midazolam. As this leads to less frequent agitation and over-sedation, we hypothesize that there are multiple beneficial clinical outcomes for patients treated with lormetazepam instead of midazolam.

Study Timeline

• Study First Submitted: 2013-12-12
• Study First Submitted QC: 2013-12-23
• Study First Posted: 2013-12-30
• Study Start: 2014-07-17
• Primary Completion: 2019-12-12
• Study Completion: 2020-03-12
• Status Verified: 2022-04
• Last Update Submitted: 2022-04-08
• Last Update Posted: 2022-04-13

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 84

Inclusion Criteria

• Mechanically ventilated ICU patients with the need for sedatives to achieve or maintain the intended target-RASS (surgical/ nonsurgical).
• Age ≥ 18 years
• Patients who are incapable of giving consent at study inclusion: Written informed consent by patient's legal representative or an independent medical consultant, patients give informed consent subsequent if they are capable.
• Patients who are able to give informed consent at study inclusion: Written informed consent by patients for planned postoperative prolonged ventilatory support who undergo heart surgery
• Consensable patients for inclusion: with necessary intubation with analgosedation

Exclusion Criteria

• Any bolus administration of benzodiazepines until 72hrs before inclusion (except from premedication due to anaesthesia).

• Continuous administration of benzodiazepines within the last 7 days before start of study drug application

• Titration phase: No way that a target RASS between -3 and 0 can be determined by the attending physician

• Known drug intolerance or allergy against lormetazepam, midazolam or one of the additional components.

• Addictive disorder

• Increased intracranial pressure

• Acute intoxication with alcohol, analgesics, sedatives, antipsychotics (neuroleptics, anti-depressives, lithium).

• Patients with cerebrale Pathology, which changes the controllability of sedation or die consciousness (e.g. patients known mental retardation due to syndromatic disorders or an infantile brain damage)

• Patients with a suspected or secured hypoxic brain damage

• Patients with intracranial surgery during actual hospital care

• Tetraplegic patients

• Myasthenia Gravis

• Cerebellar or spinal Ataxia

• Moribund patients with an expected lifespan of less than 24 hours.

• Sickle cell anaemia

• Thallassemia

• Enzyme related disorders that are associated with a severe decreased activity of UDP-glucoronyltransferase (e.g. M. Crigler- Najjar)

• Chronic liver insufficiency CHILD C with MELD Score > 17 before access to intensive care unit

• Diagnosed propofol intolerance/anamnestic propofol infusion Syndrome

• Known depression/suicidality

• Pregnancy (positive beta-HCG test from urine or positive beta-HCG laboratory test from serum (in anuric patients the serum beta-HCG test is obliged) or lactation

• Woman of child-bearing potential who are not using a highly effective contraception (Pearl - Index <1) until 3 months after study inclusion and during this trial

• Referral following an order of official authorities (court order or administrative decision) according to German Drug Law (AMG)

  §40 (1) 4

• Participation in clinical trials according to the German Drug Law (AMG) 30 days to and during the study

• Local staff

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Lormetazepam	Lormetazepam	The patient is treated on ICU not longer than 2 days. Dosage requirements according to Summary of product characteristics (Sedalam®).
Midazolam	Midazolam	The patient is treated on ICU not longer than 2 days. Dosage requirements according to Summary of product characteristics (Midazolam-ratiopharm®, Midazolam-hameln®).

Primary Outcome Measures

Name	Time	Method
Controllability of sedation	Up to 50 hours	Controllability of sedation is defined as the percentage share of measures where the actual depth of sedation (measured with the Richmond Agitation and Sedation Scale) (RASS)) matches the target depths of sedation. The individual sedation target is defined by the attending physician. . It will be measured until 5 days after terminationduring administration of study drug until 2 hours after its termination.

Secondary Outcome Measures

Name	Time	Method
Length of intensive care unit stay	During intensive care unit stay, an average of 14 days
Deviation from target Richmond agitation sedation scale (RASS)	Up to 8 days	During administration of study drug
Bedside measurement of Acetylcholinesterase activity (U/gHb)	Up to 8 days	The Acetylcholinesterase activity will be measured on every study day out of a blood sample (10µl); It will be measured until 5 days after termination of study drug.
SOFA (Sequential Organ Failure Assessment)	Up to 8 days
Concurrent medication for Analgesia and Sedation	Up to 8 days	dose/time.
Pain-Scores	Up to 28 days	NRS-V (Numeric Rating Scale -V) and FPS-R (Faces Pain Scale-Revised) and BPS (Behavioral Pain Scale) and BPS-NI (Non-Intubated BPS); according to German consensus guidelines
Delirium-screening-Instruments	Up to 28 days	CAM-ICU (Confusion Assessment Method for Intensive Care Unit) ICDSC ( Intensive Care Delirium Screening Checklist) Nu-DESC (Nursing Delirium Screening Scale)
Mortality	Up to 90 days
Length of hospital stay	During hospital stay, an average of 28 days
Follow-up treatment regarding Patient- Documentation-Management-System	During hospital stay, an average of 28 days	Discharge Mode
Number of changes in target Richmond agitation sedation scale (RASS)	Up to 56 hours	During administration of study drug
Wake-up-time	Up to 8 days	During administration of study drug until 5 days after its termination
Quality of Life	Up to 90 days	Questionnaire designed to measure quality of life (EQ-5D-3L)
Posttraumatic stress disorder	Up to 90 days	The Post-Traumatic Stress Syndrome 14-Questions Inventory
micro ribonucleic acid (rna)	Up to 24 hours	micro rna panel is analysed (only Center Charité)
Duration of mechanical ventilation and weaning from mechanical ventilation	Up to 8 days
Length of sedation	Up to 56 hours	During administration of study drug until 8 hours after its termination.
Cognition 1	Up to 28 days	Minimental State Examination (MMSE)
Depth of sedation 2	Up to 3 days	Depth of sedation 2 is measured by Electroencephalography and Electromyography (intensive care unit patients only Center Charité)
Pain threshold measurement	Up to 3 days	Automatic measurement of specific pain reflexes
Anxiety-Score	Up to 28 days	Faces Anxiety Scale score
Cognition 2	Up to 90 days	Mehrfach-Wortschatz-Intelligenztest (MWT)
Organ dysfunctions	Up to 8 days	It will be measured until 5 days after termination of study drug.
Depth of sedation 1	During the operation	Depth of sedation is measured by Electroencephalography and Electromyography (only surgical patients in the Centers Charité and Gießen)
Photomotor reflex	Up to 8 days	Photo motor reflex variations are measured by video pupillometry (only Center Charité)

Trial Locations

Locations (3)

Department of Anesthesiology and Intensive Care Medicine, Charité - University Medicine; 🇩🇪 Berlin, Germany

Clinic for Anesthesiology, Intensive Care Medicine and Painmanagement, Johann-Wolfgang-Goethe-University; 🇩🇪 Frankfurt, Frankfurt Am Main, Germany

Clinic for Operative Intensive Care Medicine and Intermediate Care, University of RWTH; 🇩🇪 Aachen, Germany