Traumatic Brain Injury Clinical Trial
Official title:
Multimodal Monitoring of Cerebral Autoregulation After Pediatric Brain Injury
Various methods have been studied to evaluate autoregulation. However, there is currently no universally accepted technique to assess integrity of the cerebral autoregulation neurovascular system. In the last decade, significant progress has been achieved in developing methods to assess cerebral autoregulation by quantifying cross-correlation between spontaneous oscillations in CBF or oxygenation and similar oscillations in arterial blood pressure. In this study the investigators will analyze the relationship between spontaneous fluctuations in mean arterial blood pressure and cerebral blood flow velocity or cerebral regional oxygenation to investigate two novel methods for measuring cerebral autoregulation, Transfer Function Analysis and Wavelet Coherence after acute pediatric brain injury.
Status | Recruiting |
Enrollment | 30 |
Est. completion date | January 2025 |
Est. primary completion date | January 2025 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 28 Days to 18 Years |
Eligibility | Inclusion Criteria: - Ages 28 days-18 years admitted to the PICU at Children's Medical Center Dallas - Acute presentation (< 24 hour) onset of neurologic injury - Acute neurologic injury can be due to any of the following mechanisms: - Severe accidental or abusive traumatic brain injury - Severe encephalopathy secondary to cardiac arrest - Spontaneous intracranial hemorrhage - Status epilepticus - Stroke - Presence of or pending placement of invasive indwelling arterial line for stand medical care - Any patient with an ICP monitor placed as standard of care Exclusion Criteria: - Patients without an arterial line placed as standard of care - Patients unable to cooperate with wearing a TCD headpiece device - Expected death within 24-48 hours - Inability to place NIRS probes or insonate TCD signal due to massive facial or cranial injury - Receiving an inhalational anesthetic agent - Hemoglobinopathy, myoglobinemia or and hyperbilirubinemia (due to inaccurate NIRS readings) |
Country | Name | City | State |
---|---|---|---|
United States | Children's Medical Center | Dallas | Texas |
Lead Sponsor | Collaborator |
---|---|
University of Texas Southwestern Medical Center | Southern Methodist University, The University of Texas at Arlington |
United States,
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* Note: There are 22 references in all — Click here to view all references
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Transfer Function Analysis | The transfer function has three components:
I. Gain: This measures the magnitude of transmission of MAP oscillations to CBFv. Effectively, a functional dCA system dampens the strength of transmitted oscillations resulting in a lower gain value. A higher gain value is therefore suggestive of impaired autoregulation. II. Phase is a "time delay" in degrees measured between the two waveforms. Absence of autoregulation would result in both MAP and CBFV changing at the same time. This would be measured as a 0°phase shift. Hence, a non-zero phase shift indicates intact autoregulation and counter-regulation of CBFV in response to changes in MAP. III. Coherence:This provides a measure of association between the two waves at difference frequencies. Coherence varies between 0 and 1, similar to a correlation coefficient it expresses the fraction of MAP linearly associated with CBFv. Gain, phase, and coherence will be aggregated to get the transfer function analysis. |
Day 1 post injury | |
Primary | Transfer Function Analysis | The transfer function has three components:
I. Gain: This measures the magnitude of transmission of MAP oscillations to CBFv. Effectively, a functional dCA system dampens the strength of transmitted oscillations resulting in a lower gain value. A higher gain value is therefore suggestive of impaired autoregulation. II. Phase is a "time delay" in degrees measured between the two waveforms. Absence of autoregulation would result in both MAP and CBFV changing at the same time. This would be measured as a 0°phase shift. Hence, a non-zero phase shift indicates intact autoregulation and counter-regulation of CBFV in response to changes in MAP. III. Coherence:This provides a measure of association between the two waves at difference frequencies. Coherence varies between 0 and 1, similar to a correlation coefficient it expresses the fraction of MAP linearly associated with CBFv. Gain, phase, and coherence will be aggregated to get the transfer function analysis. |
Day 3 post injury | |
Primary | Transfer Function Analysis | The transfer function has three components:
I. Gain: This measures the magnitude of transmission of MAP oscillations to CBFv. Effectively, a functional dCA system dampens the strength of transmitted oscillations resulting in a lower gain value. A higher gain value is therefore suggestive of impaired autoregulation. II. Phase is a "time delay" in degrees measured between the two waveforms. Absence of autoregulation would result in both MAP and CBFV changing at the same time. This would be measured as a 0°phase shift. Hence, a non-zero phase shift indicates intact autoregulation and counter-regulation of CBFV in response to changes in MAP. III. Coherence:This provides a measure of association between the two waves at difference frequencies. Coherence varies between 0 and 1, similar to a correlation coefficient it expresses the fraction of MAP linearly associated with CBFv. Gain, phase, and coherence will be aggregated to get the transfer function analysis. |
Day 5 post injury | |
Primary | Transfer Function Analysis | The transfer function has three components:
I. Gain: This measures the magnitude of transmission of MAP oscillations to CBFv. Effectively, a functional dCA system dampens the strength of transmitted oscillations resulting in a lower gain value. A higher gain value is therefore suggestive of impaired autoregulation. II. Phase is a "time delay" in degrees measured between the two waveforms. Absence of autoregulation would result in both MAP and CBFV changing at the same time. This would be measured as a 0°phase shift. Hence, a non-zero phase shift indicates intact autoregulation and counter-regulation of CBFV in response to changes in MAP. III. Coherence:This provides a measure of association between the two waves at difference frequencies. Coherence varies between 0 and 1, similar to a correlation coefficient it expresses the fraction of MAP linearly associated with CBFv. Gain, phase, and coherence will be aggregated to get the transfer function analysis. |
Day 7 post injury | |
Primary | Transfer Function Analysis | The transfer function has three components:
I. Gain: This measures the magnitude of transmission of MAP oscillations to CBFv. Effectively, a functional dCA system dampens the strength of transmitted oscillations resulting in a lower gain value. A higher gain value is therefore suggestive of impaired autoregulation. II. Phase is a "time delay" in degrees measured between the two waveforms. Absence of autoregulation would result in both MAP and CBFV changing at the same time. This would be measured as a 0°phase shift. Hence, a non-zero phase shift indicates intact autoregulation and counter-regulation of CBFV in response to changes in MAP. III. Coherence:This provides a measure of association between the two waves at difference frequencies. Coherence varies between 0 and 1, similar to a correlation coefficient it expresses the fraction of MAP linearly associated with CBFv. Gain, phase, and coherence will be aggregated to get the transfer function analysis. |
Day 10 post injury | |
Primary | Wavelet Coherence Analysis | Wavelet coherence uses phase, gain and coherence to determine a relationship between the two waveforms values MAP/CPP and SctO2. | Day 10 post injury | |
Primary | Change in Glasgow Outcome Scale Extended-Pediatrics (GOSEP) score | The 8-point Glasgow Outcome Scale Extended-Pediatrics (GOSEP) will be used to assess change in neurologic function from baseline. The GOSEP is composed of 3 parts: eye opening, best motor response, and best verbal response. Eye opening is measure 1-4, the higher the category, the better outcome. Best motor response is measured as 1-6, the higher the score, the better outcome. Best verbal response is measured as 1-5, the higher the score, the better outcome. All 3 categories are summed together to equal a total GOSEP score. The higher the overall score, the better potential outcome. | 6 months post discharge. | |
Primary | Change in Pediatric Evaluation of Disability Inventory Computer Adaptive Test (PEDI-CAT) score | Pediatric Evaluation of Disability Inventory Computer Adaptive Test (PEDI-CAT) a validated tool to measure domains of daily activities, mobility, social/cognitive function and responsibility from birth through 18 years. It will be used to assess change from baseline. | 6 months post discharge. |
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