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NCT04737369 Clinical Trial

Multimodal Neuromonitoring

Traumatic Brain Injury Clinical Trial

MMNM

Official title:
Multimodal Neuromonitoring: an Explorative Study in Neurocritical Care Patients

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT04737369
Other study ID # MMNM01
Secondary ID
Status Recruiting
Phase
First received
Last updated
Start date December 1, 2020
Est. completion date December 1, 2025

Study information
Verified date January 2021
Source Medical University of Vienna
Contact Johannes Herta, MD PhD
Phone +43 (0)1 40400-25770
Email johannes.herta@meduniwien.ac.at
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

Theoretical Framework & Background Cortical spreading depressions (CSD) and seizures, are crucial in the development of delayed cerebral ischemia and poor functional outcome in patients suffering from acute brain injuries such as subarachnoid hemorrhage. Multimodal neuromonitoring (MMNM) provides the unique possibility in the sedated and mechanically ventilated patients to record these electrophysiological phenomena and relate them to measures of cerebral ischemia and malperfusion. MMNM combines invasive (e.g. electrocorticography, cerebral microdialysis, brain tissue oxygenation) and noninvasive (e.g. neuroimaging, continuous EEG) techniques. Additionally, cerebral microdialysis can measure the unbound extracellular drug concentrations of sedatives, which potentially inhibit CSD and seizures in various degrees, beyond the blood-brain barrier without further interventions. Hypotheses 1. Online multimodal neuromonitoring can accurately detect changes in neuronal metabolic demand and pathological neuronal bioelectrical changes in highly vulnerable brain tissue. 2. Online multimodal neuromonitoring can accurately detect the impact of pathological neuronal bioelectrical changes on metabolic demand in highly vulnerable brain tissue. 3. The occurrence and duration of pathological neuronal bioelectrical changes are dependent on sedatives and antiepileptic drug concentrations 4. The occurrence and duration of pathological neuronal bioelectrical changes have a negative impact on functional and neurological long-term patient outcome. 5. Simultaneous invasive and non-invasive multimodal neuromonitoring can identify a clear relationship of both methods regarding pathological neuronal bioelectrical changes and metabolic brain status. Methods Systematic analysis of MMNM measurements following standardized criteria and correlation of electrophysiological phenomena with cerebral metabolic changes in all included patients. In a second step neuroimaging, cerebral extracellular sedative drug concentrations and neurological functional outcome, will be correlated with both electrophysiologic and metabolic changes. Due to numerous high-resolution parameters, machine learning algorithms will be used to correlate comprehensive data on group and individual levels following a holistic approach. Level of originality Extensive, cutting edge diagnostic methods are used to get a better insight into the pathophysiology of electrophysiological and metabolic changes during the development of secondary brain damage. Due to the immense amount of high-resolution data, a computer-assisted evaluation will be applied to identify relationships in the development of secondary brain injury. For the first time systematic testing of several drug concentrations beyond the blood-brain barrier will be performed. With these combined methods, we will be able to develop new cerebroprotective treatment concepts on an individual basis.

Recruitment information / eligibility
Status Recruiting
Enrollment 100
Est. completion date December 1, 2025
Est. primary completion date December 1, 2025
Accepts healthy volunteers
Gender All
Age group 18 Years to 80 Years
Eligibility Inclusion Criteria: - Individuals between 18-80 years with poor grade aneurysmal SAH (World Federation Neurosurgical Societies >3), severe ICH (ICH Score >3) or severe TBI (Glasgow Coma Scale < 9). The diagnosis of SAH, ICH and TBI will be established by computed tomography (CT). - Individuals that are unlikely to regain consciousness within the following 48 hours. - Individuals that are expected to survive for the next 48 hours. Exclusion Criteria: - Individuals younger than 18 years old and older than 80 years. - Pregnant women (documented via positive ß-HCG test). - Patients, who do not want to participate in the study. As the patient is not able to consent prior to the study, information about the study details will be given to the patient in case of clinical improvement. The patient information sheet will be handed out. Thereafter, the patient has the possibility to withdraw permission of study-participation.

Study Design

Related Conditions & MeSH terms

Locations
Country Name City State
Austria Department of Neurosurgery, Medical University of Vienna Vienna

Sponsors (2)
Lead Sponsor Collaborator
Medical University of Vienna Karl Landsteiner Institute for Clinical Epilepsy Research

Country where clinical trial is conducted

Austria, 

Outcome
Type Measure Description Time frame Safety issue
Primary Count of SD during electrocorticography Count of cortical spreading depolarization (SD) during continuous electrocorticography up to 21 days
Primary Daily pattern duration of CSD during electrocorticography Duration of cortical spreading depression (CSD) per hour during continuous electrocorticography up to 21 days
Primary Daily pattern duration of NCSE during electrocorticography Duration of nonconvulsive status epilepticus (NCSE) per hour during continuous electrocorticography up to 21 days
Primary Daily pattern duration of RPPIIC during electrocorticography Duration of rhythmic or periodic EEG patterns on the ictal-interictal continuum (RPPIIC) per hour during continuous electrocorticography up to 21 days
Primary Daily duration of metabolic crisis Duration of metabolic crisis (defined as Lactate Pyruvate ratio [LPR] > 40 and lactate higher than 4 mmol/l) during continuous electrocorticography up to 21 days
Primary Daily duration of mitochondrial dysfunction Duration of mitochondrial dysfunction (defined as LPR > 40, Pyruvate > 70 µmol/l and partial brain tissue oxygenation [PbtO2] > 20 mmHg) during continuous electrocorticography up to 21 days
Primary Daily duration of ischemia Duration of ischemia (defined as PbtO2 < 15 mmHg and cerebral perfusion pressure [CPP] < 60 mmHg) during continuous electrocorticography up to 21 days
Primary Daily duration of elevated intracranial pressure (ICP) Duration of elevated intracranial pressure (defined as ICP > 22 mmHg) during continuous electrocorticography up to 21 days
Primary Neuropharmacology Cmax) Cmax of routinely used sedative drug concentrations in blood and brain (Esketamine, Midazolam and Propofol) up to 21 days
Primary Neuropharmacology (AUC) AUC of routinely used sedative drug concentrations in blood and brain (Esketamine, Midazolam and Propofol) up to 21 days
Primary Neuropharmacology (t1/2) t1/2 of routinely used sedative drug concentrations in blood and brain (Esketamine, Midazolam and Propofol) up to 21 days
Primary Neuroimaging Absence or presence of hypoperfusion or ischemic infarctions in neuroimaging up to 28 days
Primary Functional patient outcome modified Rankin Scale up to 6 months
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