Quality of Life Clinical Trial
Official title:
Improved Muscle Metabolism by Combination of Muscle Activation and Protein Substitution: a Randomized, Outcome-assessor Blinded, Proof-of-concept Study (IMEMPRO)
NCT number | NCT05919940 |
Other study ID # | IMEMPRO |
Secondary ID | |
Status | Recruiting |
Phase | N/A |
First received | |
Last updated | |
Start date | June 27, 2023 |
Est. completion date | January 15, 2025 |
Intensive Care Unit Acquired Weakness (ICUAW) describes muscle weakness that occurs in around 40% of patients during an intensive care stay. The morbidity and mortality of these patients is significantly increased over a 5-year period. The aim of this study is to investigate the combined effect of early enteral high-protein nutrition and early muscle activation on muscle atrophy in critically ill patients. The study will include 40 patients (20 intervention, 20 observation) with requirement for enteral nutrition at time of inclusion. In the intervention group the maximum possible level of mobilization is carried out and muscles are activated twice a day using neuromuscular electrical stimulation (NMES). The nutrition plan of the intervention group is based on the applicable guidelines for intensive care medicine with exception of increased protein intake. The control group receives therapy without deviating from the standard according of the DGEM guideline. The study aims to show that the decrease in muscle mass is significantly less than in the control group (primary hypothesis) via ultrasound of the rectus femoris muscle and in case of given consent muscle biopsy. As secondary hypothesis it is examined whether the combination of early high protein intake and muscle activation improves muscle strength and endurance.
Status | Recruiting |
Enrollment | 40 |
Est. completion date | January 15, 2025 |
Est. primary completion date | October 31, 2024 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: - critically ill adults (= 18 years of age) - newly admitted to the ICU (<48h) - mechanically ventilated, expected to remain for at least 72h - enteral nutrition is feasible Exclusion Criteria: - a BMI > 30 - expected death or withdrawal of life-sustaining treatments - prior neuromuscular disease (e.g. paresis, myopathies, neuropathies) - injury or disease preventing neuromuscular electrical stimulation or early mobilization (e.g., elevated intracranial pressure, unstable spine) - a pacemaker or other electronic implant - allergy to components of NMES adhesive - have been dependent during activities of daily living prior to the hospital admission - a language barrier |
Country | Name | City | State |
---|---|---|---|
Germany | Charité - Universitätsmedizin Berlin | Berlin | |
Germany | Klinikum rechts der Isar, School of Medicine, Technical Universtity of Munich | Munich | Bavaria |
Lead Sponsor | Collaborator |
---|---|
Technical University of Munich | Berlin Institute of Health, Fresenius Kabi, University Medicine Greifswald |
Germany,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Other | in-hospital mortality | Mortality during the Hospital stay | until 90-day Follow-up | |
Other | Hospital LOS | Length of stay in the hospital | until 90-day Follow-up | |
Other | ICU-LOS | Length of stay in the ICU | until 90-day Follow-up | |
Other | Hospital mortality | Mortality during Hospital stay | until 90-day Follow-up | |
Other | Duration of Mechanical ventilation | Duration of invasive mechanical ventilator dependency | until 90-day Follow-up | |
Other | ICU mortality | Mortality during ICU stay | until 90-day Follow-up | |
Other | enzyme function in the rectus femoris | Spectrophotometry will be done in muscle samples. All samples will be screened for influence of Intensive Care Unit Acquired Weakness (ICUAW) and correlation with blood metabolome changes. | according to biopsy inbetween day 1-7 | |
Other | protein content in the rectus femoris | Western Blot will be done in muscle samples. All samples will be screened for influence of Intensive Care Unit Acquired Weakness (ICUAW) and correlation with blood metabolome changes. | according to biopsy inbetween day 1-7 | |
Other | geneexpression in the rectus femoris | qPCR (quantitive polymerase chain reaction) will be done in muscle samples. All samples will be screened for influence of Intensive Care Unit Acquired Weakness (ICUAW) and correlation with blood metabolome changes. | according to biopsy inbetween day 1-7 | |
Other | Muscle morphology of the rectus femoris | Light-and Electron-Microscopy will be done in muscle samples. All samples will be screened for influence of Intensive Care Unit Acquired Weakness (ICUAW) and correlation with blood metabolome changes. | according to biopsy inbetween day 1-7 | |
Primary | Change in cross sectional area (?CSA) of the rectus femoris | Change in muscle mass between study inclusion and study day 14; measured as change of the cross sectional area (?CSA) of the rectus femoris muscle via ultrasound. | day 1 (study inclusion) and 14 days | |
Secondary | change in muscle thickness of the rectus femoris | change in muscle thickness from study inclusion until 90-day follow-up, measured via ultrasound. | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | change in echogenicity of the rectus femoris | change in echogenicity from study inclusion until 90-day follow-up, measured via ultrasound. | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | change of the pennation angle of the rectus femoris | change of the pennation angle from study inclusion until 90-day follow-up, measured via ultrasound. | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | change of the muscle strength, measured by the Medical Research Council score (MRC-score) | change of the muscle strength, measured by the Medical Research Council score (MRC-score) from study inclusion until 90-day follow-up | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | change of the muscle strength, measured by handgrip dynamometry | change of the muscle strength, measured by handgrip dynamometry from study inclusion until 90-day follow-up | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | change in muscle endurance | change in muscle endurance, measured by the 6-minute walking test up to 90-day follow-up | up to 90 day follow up | |
Secondary | change in physical physical function | change in physical physical function, measured by the Short Physical Performance Battery up to 90-day follow-up | up to 90-day follow-up | |
Secondary | development of quality of life | development of quality of life, measured by the Short Form-36 up to 90-day follow-up | up to 90-day follow-up | |
Secondary | change in Skeletal muscle mass | change in Skeletal muscle mass, measured with bioelectrical impedance analysis up to 90-day follow-up. | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | change in extracellular volume | change in extracellular volume, measured by the Body impedance analysis | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | change in the REE (Resting Energy Expenditure) | change in the REE (Resting Energy Expenditure), measured by indirect calorimetry | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | urea-to-creatinine ratio | urea-to-creatinine ratio from blood sample | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | Identify possible predictors of muscle wasting in urine metabolomics at ICU admission | Among the urine metabolomics that will be measured, identify metabolites or combinations of metabolites whose high or low concentration(s) at ICU admission associate(s) with the amount of muscle loss. These metabolites are candidate biomarkers that could be used to identify individuals at risk of large muscle wasting and may give further insights into the mechanisms of muscle wasting. | day 1 (study inclusion) until 90-day Follow-up | |
Secondary | Identify possible predictors of muscle wasting in the blood metabolome at ICU admission | Among the blood metabolome that will be measured, identify metabolites or combinations of metabolites whose high or low concentration(s) at ICU admission associate(s) with the amount of muscle loss. These metabolites are candidate biomarkers that could be used to identify individuals at risk of large muscle wasting and may give further insights into the mechanisms of muscle wasting. | day 1 (study inclusion) until 90-day Follow-up |
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