Traumatic brain injury (TBI) is one of the leading causes of death and disability within Canada and globally, with more than 50 million people per year suffering a TBI worldwide, incurring costs of nearly $540 billion CAD annually across the globe.^{Reference Maas, Menon and Adelson1} Overall, there has been little change in mortality and morbidity associated with TBI in the past four decades of TBI care. This morbidity and mortality are associated with both primary and secondary injury, with primary injury representing the structural damage to the brain at the time of the incident and secondary injury referring to the cascade of systemic and local cellular events that lead to tissue damage within the brain. Little can be done about primary injury, aside from public awareness, policy, and educational campaigns directed at the reduction in head injury incidence. However, the mechanisms involved in secondary brain injury after TBI are amenable to therapeutic intervention, which might lead to improvements in morbidity and mortality.

Over the past twenty years, the acute care for critically ill TBI patients has seen various advances, with the goal of secondary injury reduction. Implementation of guideline-based approaches to the intensive care unit (ICU) has aimed to homogenize TBI care globally^{Reference Carney, Totten and O’Reilly2} and provide a framework on which to add more advanced monitoring and individualized interventions according to patient-centered physiology and pathophysiology.^{Reference Le Roux, Menon and Citerio3} Such advances include the application of various multimodal monitoring (MMM) devices, which allow continuous real-time bedside assessments of cerebral physiology.^{Reference Le Roux, Menon and Citerio3} With the addition and integration of high-frequency signal processing techniques and strategies, one can derive additional continuous cerebral physiologic metrics at the bedside.

Such derived metrics have sparked a new age of monitoring and care for the critically ill TBI patient, ushering in an era where personalized medicine approaches are on the horizon.^{Reference Zeiler, Thelin and Donnelly4} Individualized physiologic targets in TBI care, including optimal cerebral perfusion pressure (CPPopt)^{Reference Needham, McFadyen, Newcombe, Synnot, Czosnyka and Menon5,Reference Kramer, Couillard, Zygun, Aries and Gallagher6} or individualized intracranial pressure (iICP) thresholds,^{Reference Zeiler, Ercole and Cabeleira7} are emerging in the literature as viable options at the forefront of personalized medicine in the ICU care of TBI but require more extensive external validation. Similarly, continuous bedside metrics for cerebrovascular reactivity/autoregulation,^{Reference Zeiler, Donnelly, Calviello, Smielewski, Menon and Czosnyka8} compensatory reserve,^{Reference Zeiler, Kim, Cabeleira, Calviello, Smielewski and Czosnyka9} autonomics,^{Reference Hasen, Almojuela and Zeiler10} brain tissue oxygenation (PbtO₂),^{Reference Okonkwo, Shutter and Moore11} and the cumulative ischemic burden can be employed.^{Reference Güiza, Depreitere and Piper12–Reference Helbok, Meyfroidt and Beer14} These additional measures are of great importance in TBI care, as many have shown to be independent predictors of global outcome in TBI, including cerebrovascular reactivity, CPPopt, and PbtO₂.^{Reference Okonkwo, Shutter and Moore11,Reference Zeiler, Ercole and Cabeleira15,Reference Oddo, Levine and Mackenzie16} Furthermore, derangement in metrics such as cerebrovascular reactivity or PbtO₂ are believed to contribute to the relatively unchanged mortality rates in severe TBI over the last 20–30 years, since the paradigm of care and focus of the past guidelines was on the relatively crude surrogate of cerebral blood flow: absolute ICP measure.^{Reference Donnelly, Czosnyka and Adams17,Reference Chesnut, Temkin and Carney18}

Future integration of MMM of cerebral physiology and high-frequency signal processing techniques, with advanced neuroimaging, proteomic, and genomic analysis, provides an opportunity to explore the molecular pathways involved in various aspects of cerebral physiologic dysfunction in vivo. Such work will aim to provide insight into the drivers of impaired cerebral physiology and develop therapeutics aimed at prevention and treatment, with the goal of morbidity and mortality reduction.

Though elegant in concept, the main issue with early and rapid discovery in this field of personalized medicine is the expertise and complexity of data involved. The MMM high-frequency digital physiology requires biomedical engineering expertise for acquisition, storage, and processing. Figure 1 provides an example of such hardware and software integration required for high-frequency signal capture and the need for other advanced capabilities such as integrated neuroimaging. Similarly, coordinating the capture of such valuable physiology with comprehensive information regarding patient-specific demographics and treatment strategies, neuroimaging, and biosamples for future proteomic/genomic analyses requires extensive coordination and collaboration between centers with both interest and expertise in the area. In addition, in order to generate sufficient sample size, such data collection initiates require ongoing prospective collection. Such approaches will also benefit from adaption of artificial intelligence and machine learning techniques.

Figure 1: 3 T IMRIS Suite, ICU Bedside Physiologic Recording and Extended Cerebral Physiologic Indices. 3 T = 3 Tesla, ABP = arterial blood pressure, AMP = pulse amplitude of ICP (derived through Fourier transformed ICP waveform), a.u. = arbitrary units, CPP = cerebral perfusion pressure, ICP = intracranial pressure, IMRIS = intraoperative magnetic resonance suite, MAP = mean arterial pressure, PRx = pressure reactivity index (autoregulation index), RAP = cerebral compensatory reserve index. (A) 3 T intraoperative MRI suite located next to intensive care unit. (B) Bedside setup for recording high-frequency digital waveforms of physiologic signals employing intensive care monitoring “plus” (ICM+) data acquisition software (Cambridge Enterprise Ltd, Cambridge, UK, http://icmplus.neurosurg.cam.ac.uk). (C) Left – Recorded digital waveforms of ABP and ICP (100 Hz), grey arrow displays zoomed window of the full waveforms; Right – processed signals from left window. Signals have been processed to display MAP, AMP, mean ICP, cerebral autoregulation (PRx), and cerebral compensatory reserve (RAP).

This brief communication highlights the CAnadian High-Resolution Traumatic Brain Injury (CAHR-TBI) Research Collaborative (Figure 2 – CAHR-TBI logo), which has been formed from centers with specific expertise in the area of high-frequency physiologic monitoring/processing, consisting of the University of Calgary (AK and CG), University of British Columbia (MS and DG), University of Montreal (FB), and University of Manitoba (FAZ – Location of the Winnipeg Acute TBI Research Program and Winnipeg Acute TBI Biobank (CTRN BRC-00446)). The mandate of this group is to facilitate collaborative high-resolution (HR) ICU research for TBI in Canada and become global leaders in this area, with the main goal of understanding drivers of cerebral physiologic dysfunction.

Figure 2: CAnadian High-Resolution Traumatic Brain Injury (CAHR-TBI) Research Collaborative Logo.

The CAHR-TBI collaborative has the following main objectives:

Facilitate creation of a unique high quality prospectively maintained HR database collaborative within Canada among centers with specialty expertise. Such database elements will include high-frequency digital cerebral physiology from MMM in the ICU, patient characteristics (demographics, injury, treatment, laboratory, imaging, outcomes), and biobank elements (at selected centers).

Enable open data sharing between involved centers to facilitate individual program research interests and provide multidisciplinary support for member-led initiatives.

To engage in Canadian-led collaborative initiatives in MMM for TBI and facilitate multicenter prospective studies into advanced MMM, signal processing, advanced prognostic modeling, big data strategies, and molecular pathways involved in physiologic dysfunction in TBI. Such approaches will also be expanded to other neurologic illnesses, such as aneurysmal subarachnoid hemorrhage and hypoxic ischemic brain injury.

To facilitate training of highly qualified personnel (HQP) in Canada within the field of advanced MMM, physiologic signal processing, and investigation into pathogenesis of secondary injury in TBI, creating the next generation of leaders in the field.

To engage, where appropriate, in national and international initiatives for HR data in TBI, including (but not limited to): Canadian Traumatic Brain Injury Research Consortium,^{Reference Hutchison, Emery and Gagnon19} Collaborative European NeuroTrauma Effectiveness Research in Traumatic Brain Injury (CENTER-TBI) study,^{Reference Maas, Menon and Steyerberg20} Genetic Associations In Neurotrauma initiative, in the International Initiative for Traumatic Brian Injury Research (InTBIR), and other regional initiatives (such as those with collaborators in Sweden and Finland).

The collaborative will have a variety of medium- and long-term initiatives, based on individual member interests. We currently house over 300 patients worth of archived high-frequency MMM physiologic data in moderate/severe TBI and expect ongoing prospective yearly collection of ~150 data sets, some of which will have bio banked blood/cerebrospinal fluid (CSF)/micodialysate samples for future proteomic/genetic analyses (depending on individual site capabilities). Currently, our areas of focus in high-resolution ICU (HR ICU) data for TBI will include:

1. A. Validation Studies for Advanced MMM in TBI: Such work will focus on providing multicenter validation to previous single-center retrospective studies in the field. These studies are crucial for such advanced monitoring concepts to be adopted clinically and to facilitate clinical trials on various metrics. Fields of validation include (but are not limited to): cerebrovascular reactivity, CPPopt, compensatory reserve, low-resolution monitoring metrics, newer monitoring indices, individual ICP thresholds, advanced invasive monitoring metrics (such as parenchymal brain tissue oxygen, cerebral blood flow, and microdialysis), and noninvasive cerebral physiology monitoring.

2. B. MMM Characterization of Cerebral Physiology: Despite a growing literature on MMM-based cerebral physiology, the complex interrelationship is not well understood. Studies on MMM relationships between raw and derived cerebral physiologic metrics will occur to improve our understanding.

3. C. Development of Noninvasive Modalities for Cerebral Physiologic Monitoring: Such work will focus on developing noninvasive techniques for physiology monitoring, such as cerebrovascular reactivity. This initiative will break ground in development, implementation, and validation of such advanced monitoring during subacute and long-term outcome phases after TBI.

4. D. Advanced Prognostic Models: Utilizing HR data sets, development of more complex and comprehensive prognostic models will occur. Such initiatives will be facilitated using machine learning and big data strategies. Further, we will integrate regional and provincial community health database infrastructure to link acute HR ICU data sets with socioeconomic outcome variables, so as to better characterize the relationship between acute phase physiologic phenotype and long-term sequelae of moderate/severe TBI.

5. E. Physiologic “State” Modeling: Knowledge and characterization of MMM cerebral physiologic “state” using time-series and Bayesian state-space techniques may provide the ability to characterize a patientʼs individual physiologic state and predict state transitions. Such work will involve engaging machine learning and artificial intelligence to aid with dynamic modeling.

6. F. Tissue Consequences of Impaired Physiology: Combined HR ICU physiologic data sets with computed tomography (CT) and magnetic resonance imaging (MRI)-based neuroimaging during the acute, subacute, and long-term phases post-TBI will facilitate our understanding of the impact of various physiologic derangements on imaging-based lesion development/progression and tissue fate. Such work will require integration of quantitative imaging analysis (via manual or semi-automated lesion segmentation techniques).

7. G. Uncover Molecular Pathways of Cerebral Physiologic Dysfunction in TBI: Combining HR ICU data sets with biobank whole blood, serum, and cerebrospinal fluid/microdialysate specimens will enable integration of proteomics and genomics with high-frequency physiology. Such unique data sets are positioned to shed light on molecular pathways involved in cerebral physiologic dysfunction and provide novel targets for prevention and treatment.

8. H. Chronic Sequelae of TBI: Such initiatives will focus on subacute and long-term characterization of TBI and its impact on cerebral physiology, neuroimaging-based tissue consequences (CT/MRI/positron emission tomography), and clinical phenotype. Works will integrate high-frequency continuous cerebral physiology, neuroimaging techniques, genomics, and serum/CSF proteomics.

Funding

Currently, funding for the ongoing prospective collection of patient information and high-frequency digital physiologic cerebral signals is provided by various local, regional, and federal partners, depending on the specific core site. Funding is provided by each siteʼs university through research grants, charitable foundations, existing trauma research funding, and federal grants (such as the National Institutes of Health (NIH) and the Canadian Foundation for Innovation (CFI)). Core members plan for group applications to federal funding opportunities to support ongoing infrastructure and specific prospective studies.

Knowledge Translation

Knowledge translation will occur through the various initiatives from the collaborative. We will generate projects that will be presented locally/nationally/internationally at meetings and publish in peer-reviewed venues regularly. Furthermore, the interests and initiatives will enable sustained training opportunities for HQPs in Canada, attract world-class talent for training, and ensure future growth and productivity for the CAHR-TBI Research Collaborative. All of these aspects will guarantee knowledge translation to various stakeholder parties, including academics, clinicians, and patients, facilitating improvements in patient care for those with TBI in Canada and globally.