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| Name | Class |
|---|---|
| Defence Research and Development Canada | INDUSTRY |
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The prevention of secondary brain injury is a primary goal in treating patients with severe traumatic brain injury (TBI). Secondary brain injury results from tissue ischemia induced by increased vascular resistance in the at-risk brain tissue due to compression by traumatic hematomas, and development of cytotoxic and vasogenic tissue edema. While traumatic hematomas may be managed surgically, cytotoxic and vasogenic edema with resulting perfusion impairment perpetuates brain ischemia and injury. Animal models suggest that remote ischemic conditioning (RIC) can reverse these effects and improve perfusion. Based on these findings it is hypothesized that RIC will exert beneficial effects on TBI in man, thereby representing a new therapeutic strategy for severe TBI.
Patients presenting to our institution suffering from severe TBI will be considered for enrollment. Eligible patients will have sustained a blunt, severe TBI (defined by Glasgow Coma Scale <8) with associated intra-cranial hematoma(s) not requiring immediate surgical decompression, with admission to an intensive care unit and insertion of an intra-cranial pressure monitor. Patients will be randomized to RIC versus sham-RIC intervention cohorts. RIC interventions will be performed using an automated device on the upper extremity delivering 20 cumulative minutes of limb ischemia in a single treatment session. The planned enrollment is a cohort of 40 patients.
Outcomes of this study will include multiple domains. Our primary outcome will include serial assessments of validated serum biomarkers of neuronal injury and systemic inflammation. Secondary outcomes will include descriptions of the clinical course of each patient, radiologic assessment of brain perfusion, and neurocognitive and psychological assessment post-discharge.
If clinical outcomes are improved using RIC, this study would support RIC as a novel treatment for TBI. Its advantages include safety and simplicity and, requiring no specialized equipment, its ability to be used in any environment including pre-hospital settings or in austere theatres. The investigators anticipate that TBI patients treated with RIC will have improved clinical, biochemical, and neuropsychological outcomes compared to standard treatment protocols.
Traumatic brain injury is a leading cause of morbidity and mortality in victims of blunt trauma, leading to a tremendous economic cost, chronic neuropsychological sequelae and productive years of life lost. Treatment of inoperable primary brain injury consists largely of supportive care to support natural healing and prevention or reduction of secondary insults (1).
Many of the phenomena of secondary injury are related to ischemic sequelae of injury progression. Brain parenchymal edema increases both regional and global intra-cranial pressures, decreasing perfusion pressure, resulting in impaired perfusion, an oxygen debt, and ischemic injury (2). Local compression from traumatic hematomas may act in concert with edema to further impair perfusion. One strategy that has been successfully employed in the treatment of other ischemic insults is an intervention known as "remote ischemic conditioning" (RIC). RIC is felt to induce systemic responses which promote physiologic adaptations to moderate ischemia and minimize the impact of subsequent ischemic insults. Because these effects are systemic, extremity ischemic conditioning may impact brain injury. In the setting of TBI, where all patients carry a risk of ischemic secondary injury, early intervention with RIC may minimize the harm of secondary ischemic insults and improve outcomes.
The systemic effects of RIC have been demonstrated in a variety of organ systems and mechanisms of ischemia. Application of RIC has demonstrable benefits in preventing ischemia-induced organ dysfunction in insults to the heart (3-6), kidneys (7,8), and ocular organ systems (9). Our recent work has demonstrated its benefit in preventing organ injury following hemorrhagic shock (10). The technique has also demonstrated promise in reducing brain injury secondary to stroke or neurosurgical trauma (11-13).
Ischemic conditioning of brain injuries has proven benefits in animal models. Limb preconditioning reduces toxic oxygen free radicals, reduces neuronal apoptosis, reduces intra-cranial inflammation, improves integrity of the blood-brain barrier, and reduces brain parenchymal edema (14,15). RIC also improves microvascular perfusion to ischemic tissues which, in the brain, may reduce secondary injury by promoting perfusion to the at-risk injured brain (16). Even when performed after the intra-cranial trauma in a "post-conditioning" model, limb ischemic conditioning is associated with decreased apoptosis, decreased edema, and decreased brain infarction volumes (17,18). A single recent trial of RIC in human TBI patients showed a decrease in serum biomarkers of central nervous system (CNS) injury in the conditioned cohort (19).
Given the promising findings of the remote ischemic conditioning technique in reducing biomarkers of intra-cranial inflammation, an assessment of the clinical effectiveness of post-traumatic remote ischemic conditioning in modifying the outcomes of patients with isolated severe traumatic brain injuries is warranted.
Outcomes of this proposed prospective, randomized controlled trial will fall into the following validated categories:
The known physiologic effects of RIC are theoretically beneficial to patients suffering severe TBI who are at risk of clinical deterioration due to secondary injury. By mitigating the effects of inflammation and edema and improving microvascular perfusion, at-risk brain tissue may be salvaged and thus patient outcomes improved. This theory is supported by the existing evidence and a well-planned selection of outcome measures including biochemical, clinical, and radiographic outcomes may demonstrate the benefits of RIC in this patient population.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Control Arm | Sham Comparator | Control-arm patients will be treated with standard "Best Practice" management of traumatic brain injury, with the addition of sham-RIC. The sham intervention will use a purpose-built device which will visually and audibly mimic a functional RIC device, with the key distinction being non-inflation of the arm cuff with resultant non-occlusion and no induced ischemia. To mask patient enrollment, all patients in both study arms will have the arm and RIC device draped in an opaque sheet so that the extremity distal to the RIC device are not visible to medical staff during the period of intervention. |
|
| RIC Arm | Experimental | The RIC treatment will be applied with a purpose-built commercial RIC device which will aid in standardizing dose and delivery. Therapeutic RIC will be provided by the CellAegis Technologies autoRIC device on an upper extremity. As with the control cohort, this cohort will undergo complete extremity draping. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| CellAegis Technologies autoRIC device | Device | The autoRIC device from CellAegis technologies will be applied as per the manufacturer's instructions on an upper extremity. The device will automatically inflate and deflate a blood pressure cuff to supra-systolic blood pressures, maintaining an occlusive pressure for a period of five minutes, followed by five minutes of re-perfusion with cuff deflation, completing a ten minute cycle. This cycle will repeat four times for a cumulative total of twenty minutes of occlusive conditioning over forty minutes of intervention time. |
| Measure | Description | Time Frame |
|---|---|---|
| Neuron Specific Enolase (NSE) - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| S100A12 - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Calcium Binding Protein Beta (S100B) - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Glial Fibrillary Acidic Protein (GFAP) - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Monocyte Chemoattractant Protein (MCP1) - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Epinephrine - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Measure | Description | Time Frame |
|---|---|---|
| Cerebral vascular perfusion, acute | Patients will undergo Arterial Spin Loading Functional Magnetic Resonance Imaging (fMRI) at 72 hours post-RIC to quantify blood flow to the acutely ischemic brain parenchyma. | 24 hours |
| Intracranial Pressure (ICP) measurement, first 24 hours |
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Inclusion Criteria:
Exclusion Criteria:
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| Name | Affiliation | Role |
|---|---|---|
| Ori D Rotstein, MD | Unity Health Toronto - St. Michael's hospital | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| St Michaels Hospital | Toronto | Ontario | M5B 1W8 | Canada |
| PubMed Identifier | Type | Citation | Retractions |
|---|---|---|---|
| Background | ACS TQIP Best Practices in the Management of Traumatic Brain Injury. 2015. | ||
| 1919689 | Background | Bouma GJ, Muizelaar JP, Choi SC, Newlon PG, Young HF. Cerebral circulation and metabolism after severe traumatic brain injury: the elusive role of ischemia. J Neurosurg. 1991 Nov;75(5):685-93. doi: 10.3171/jns.1991.75.5.0685. | |
| 20189026 |
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| ID | Term |
|---|---|
| D000070642 | Brain Injuries, Traumatic |
| D020196 | Trauma, Nervous System |
| D015427 | Reperfusion Injury |
| D002545 | Brain Ischemia |
| D001930 | Brain Injuries |
| D014947 | Wounds and Injuries |
| ID | Term |
|---|---|
| D001927 | Brain Diseases |
| D002493 | Central Nervous System Diseases |
| D009422 | Nervous System Diseases |
| D006259 | Craniocerebral Trauma |
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This trial is a prospective double-blind parallel cohort study of patients undergoing either standard of care plus placebo (sham-RIC) or standard treatment plus a single session of upper extremity remote ischemic conditioning.
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While it is not technically possible to mask participants to the application of RIC versus sham therapies, all participants in this trial by design will be intubated in an intensive care unit with severe traumatic brain injury; it is improbable that our inability to mask the patients will compromise outcomes or induce bias as patients are unlikely to have consciousness or memory of the therapy.
|
|
| Best Practice Management of Traumatic Brain Injury | Other | Standard treatment of TBI in a dedicated trauma-neuro intensive care unit will include a tiered management strategy corresponding to many published treatment algorithms, including the American College of Surgeons Trauma Quality Improvement Program (ACS TQIP) guidelines for the management of intra-cranial hypertension. Standard practice without limitations will be applied to both cohorts of patients in this study. |
|
| Norepinephrine - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Interleukin 10 (IL10) - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Interleukin 1 Beta (IL1B) - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Tumor Necrosis Factor Alpha (TNF Alpha) - biomarker | Plasma concentration measured by measured by enzyme-linked immunosorbent ELISA and multiplex platform at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| International Normalized Ratio (INR) - standard lab test. | Standard coagulation parameter, to be measured at all time points specified below. | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Prothrombin Time (PTT) - standard lab test. | Standard coagulation parameter, to be measured at all time points specified below | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
| Rotational Thromboelastometry (ROTEM), standard lab test. | ROTEM coagulation assessment using the commercial ROTEM device traditionally used for the assessment of trauma-induced coagulopathy, to be measured at all time points specified below | Admission (0 hours), 6 hours, 24 hours, 48 hours, and 72 hours |
The number of episodes of ICP >20 mmHg, measured in 15 minute increments, over the first 24 hours. |
| 24 hours |
| Intracranial Pressure (ICP) measurement, 24-96 hours | The number of episodes of ICP >20 mmHg, measured in 15 minute increments, over 24-96 hours. | 24 hours, 96 hours |
| Escalation along an established care algorithm | Patient care interventions will be plotted against the Tier 1, Tier 2, and Tier 3 categories of interventions described by the American College of Surgeons Trauma Quality Improvement Program (ACS TQIP) guidelines for the management of traumatic intracranial hypertension. | 12 months |
| Mortality beyond 12 hours post-admission | Patient deaths occurring in the first 12 hours will result in patient-exclusion as it is unlikely that these patients would have had different outcomes regardless of treatment strategies. | 12 months |
| Incidence of surgical decompression beyond 12 hours post-admission | Patient progression to need for definitive surgery occurring in the first 12 hours will result in patient-exclusion as it is unlikely that these patients would have had different outcomes regardless of treatment strategies. | 12 months |
| Hospital length of stay, number of days | Number of continuous calendar days or partial calendar days admitted to an acute-care hospital. | 12 months |
| Intensive Care Unit length of stay, number of days | Number of continuous calendar days or partial calendar days admitted to an intensive-care unit. | 2 months |
| Total duration of mechanical ventilation, number of days | Number of calendar days or partial calendar days including treatment with invasive ventilation. | 2 months |
| Destination of discharge | Home (functionally independent), rehabilitation facility, or chronic care facility | 12 months |
| Glasgow Outcomes Scale, Extended (GOSE) - neurocognitive test | The GOSE scale assessing neurocognitive function will be assessed on hospital, discharge, at three months post-discharge, and at 6 and 12 months post-discharge. | discharge, 3 months, 6 months, and 12 months |
| Disability Rating Scale (DRS) - neurocognitive function rating | The DRS scale assessing neurocognitive function will be assessed on hospital discharge, at three months post-discharge, and at 6 and 12 months post-discharge. | discharge, 3 months, 6 months, and 12 months |
| Patient Health Questionnaire 9th edition (PHQ-9) - neurological - self assessment | The PHQ-9 screen for mental health disorders will be assessed on hospital discharge, at three months post-discharge, and at 6 and 12 months post-discharge. | discharge, 3, 6, and 12 months |
| Posttraumatic Stress Disorder Checklist for the Diagnostic and Statistical Manual of Mental Disorders 5th edition (PCL-5) - neurological - self assessment | The PCL-5 screen for Post-Traumatic Stress Disorder will be assessed on hospital discharge, at three months post-discharge, and at 6 and 12 months post-discharge. | discharge, 3 months, 6 months, and 12 months |
| Background |
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| D014652 | Vascular Diseases |
| D002318 | Cardiovascular Diseases |
| D011183 | Postoperative Complications |
| D010335 | Pathologic Processes |
| D013568 | Pathological Conditions, Signs and Symptoms |
| D002561 | Cerebrovascular Disorders |