Ignite Creation Date:
2024-07-17 @ 12:07 PM
Last Modification Date:
2024-10-26 @ 3:34 PM
Study NCT ID:
NCT06493071
Status:
NOT_YET_RECRUITING
Last Update Posted:
2024-07-09
First Post:
2024-06-17
Brief Title:
Transcutaneous Auricular Vagus Nerve Stimulation taVNS for Inflammation and Depression Following SCI
Sponsor:
Lawson Health Research Institute
Organization:
Lawson Health Research Institute
Study Overview
Official Title:
Transcutaneous Auricular Vagus Nerve Stimulation taVNS as an Anti-inflammatory Strategy for the Treatment of Depression Following Spinal Cord Injury
Status:
NOT_YET_RECRUITING
Status Verified Date:
2024-07
Last Known Status:
None
Delayed Posting:
No
If Stopped, Why?:
Not Stopped
Has Expanded Access:
False
If Expanded Access, NCT#:
N/A
Has Expanded Access, NCT# Status:
N/A
Acronym:
None
Brief Summary:
Spinal cord injury SCI has been shown to be associated with impairment to the autonomic nervous system in the form of reduced activity of a key nerve known as the vagus nerve As the vagus nerve has an important role in regulating inflammation and is associated with depression it may represent a key mechanism which contributes to chronic inflammation and depression following SCI
A technique known as transcutaneous auricular vagus nerve stimulation taVNS can stimulate the vagus nerve non-invasively through an electrode applied on the skin of the ear This technique has been shown to effectively reduce inflammation and improve symptoms of depression in other populations without any serious adverse events However it has not been assessed in individuals with SCI
The primary objective of this study is to assess the efficacy of taVNS therapy for the treatment of inflammation and depression Autonomic function as assessed by measures of heart rate variability HRV will also be assessed to quantify changes in vagal tone The study will be conducted over a 2-year period with 44 individuals with SCI and depression participating Participants will be randomly assigned to receive either active taVNS or a placebo sham treatment over a 30-day period
The researchers will assess changes in depression symptoms autonomic function heart rate variability and biomarkers related to inflammation at baseline and 30-days Safety and adherence will also be evaluated to confirm the feasibility for long-term use
This study aims to explore a novel and non-invasive treatment strategy for depression in individuals with spinal cord injury If taVNS is found to be safe effective and feasible for SCI patients it could offer a simple cost-effective way to address chronic inflammation and depression in this population
A technique known as transcutaneous auricular vagus nerve stimulation taVNS can stimulate the vagus nerve non-invasively through an electrode applied on the skin of the ear This technique has been shown to effectively reduce inflammation and improve symptoms of depression in other populations without any serious adverse events However it has not been assessed in individuals with SCI
The primary objective of this study is to assess the efficacy of taVNS therapy for the treatment of inflammation and depression Autonomic function as assessed by measures of heart rate variability HRV will also be assessed to quantify changes in vagal tone The study will be conducted over a 2-year period with 44 individuals with SCI and depression participating Participants will be randomly assigned to receive either active taVNS or a placebo sham treatment over a 30-day period
The researchers will assess changes in depression symptoms autonomic function heart rate variability and biomarkers related to inflammation at baseline and 30-days Safety and adherence will also be evaluated to confirm the feasibility for long-term use
This study aims to explore a novel and non-invasive treatment strategy for depression in individuals with spinal cord injury If taVNS is found to be safe effective and feasible for SCI patients it could offer a simple cost-effective way to address chronic inflammation and depression in this population
Detailed Description:
Depression and chronic inflammation are highly prevalent following SCI Inflammation plays an increasingly appreciated role in the pathology of depression One key mechanism is the ability to dysregulate a key metabolic pathway the Kynurenine pathway resulting in serotonin deficits and increased production of neurotoxic metabolites Prior research from our lab has demonstrated the efficacy of diet and exercise to affect this pathway and improve clinical symptoms However we have shown that the burdensome nature of such interventions limits long-term adherence in SCI Stimulating the vagus nerve has been shown to induce anti-inflammatory effects in populations with chronic inflammation eg rheumatoid arthritis Crohns disease and lower scores of depression
However the potential benefits of a chronic vagus nerve stimulation intervention has not been assessed in individuals with SCI Transcutaneous auricular vagus nerve stimulation taVNS is a simple to administer and non-invasive neurostimulatory technique which can stimulate the vagus nerve via the skin of the ear Given that SCI is associated with chronic inflammation high rates of depression and reductions in vagal tone they may represent a population that would be particularly susceptible to the benefits of this low-burden low-cost treatment strategy
The overall objective of this study is to demonstrate that transcutaneous auricular vagus nerve stimulation taVNS therapy is a safe and feasible treatment which effectively activates the vagus nerve in individuals with SCI The study will also provide preliminary efficacy data related to the impact on symptoms of depression and inflammatory biomarkers
Participants will be randomized to receive either active taVNS therapy treatment group or sham taVNS therapy placebo group The intervention will be performed over a 30-day period and will follow the recommended daily stimulation of 4-hours per day with at least 1-hour carried out continuously for a total of 30 sessions
All participants will have an in-person baseline visit to determine optimal taVNS stimulation parameters and be trained on instructions for use For the active stimulation group stimulation will target the auricular branch of the vagus nerve by applying stimulation to the cymba conchae region of the left ear using the tVNS R device taVNS Technologies Erlangen Germany For the sham group stimulation will target the earlobe which will allow the participant to feel the stimulation while avoiding stimulation of the auricular branch of the vagus nerve To achieve adequate stimulation while avoiding unpleasant or painful sensations the stimulation intensity will be gradually increased in increments of 01mA until the subjective pain threshold is reached and then reduced to a stimulus intensity just below the individuals pain threshold expected range based on prior studies 1 - 32mA Pulse width will be set at 100μs and frequency will be set at 25Hz as performed in our previous protocol in spinal cord injured patients approved by Health Canada 364351 and shown to safely and effectively increase vagal tone The stimulation parameters determined during this in-person baseline visit will be locked for the duration of the 30-day intervention
Upon establishing appropriate stimulation parameters each participant will be trained on instructions for use As the tVNS R device is designed to be carried out independently by the patient instructions for use are simple and user friendly The participant will be instructed to 1 clean the ear using provided alcohol swabs 2 place the electrode in the ear in the appropriate orientation depending on group allocation 3 turn the device on by pressing the ON button and 4 begin stimulation by pressing the STARTSTOP button once Participants may then place the device in their pocket and go about their daily activities as normal The device will display percent completion of the daily 4-hour stimulation period so that participants are aware of there daily progress and when the session is complete
At the initial study visit as well as the 30-day post study visit participants will also undergo an assessment of heart rate variability HRV depression and inflammatory biomarkers
HRV will be assessed via electrocardiogram ECG to assess changes in autonomic function related to vagal tone For the collection of ECG signals participants will be instructed to avoid caffeine alcohol and strenuous exercise for at least 24 hours prior to assessment Participants will be instructed to remain relaxed focus on breathing and avoid speaking throughout the protocol ECG recording will be collected using the Polar H10 heart monitor Continuous heart rate will be recorded for a period of 5-minutes to obtain a baseline measure This process will be repeated following the 30-day intervention period at the post testing session ECG data will be imported to Kubios software for analysis of root mean square of successive differences RMSSD as well as high frequency HF power RMSSD is a time domain measure of heart rate variability corresponding to the variability in the intervals between successive heartbeats and is a measure of vagal tone HF power is a frequency domain measure of heart rate variability corresponding to heart rate fluctuations occurring in the frequency range of 015 to 04Hz and also reflects vagal tone RMSSD which is less influenced by breathing rate will be the primary assessment of vagal tone and HF power will be assessed to ensure consistency in measures Measures of vagal tone will be assessed at baseline and post-intervention to assess whether the intervention successfully targets the vagus nerve and increases vagal tone
Depression will be assessed via the Patient Health Questionnaire PHQ-9 at baseline and 30-days post-intervention The PHQ-9 has been shown to be a valid assessment for major depressive disorder in individuals with SCI The PHQ-9 is a 9-item questionnaire with items pertaining to feelings over the previous 2-weeks Each item is scored on a scale from 0 not at all to 3 nearly every day with total scores allowing for assessment of depression severity A score ranging from 0-4 suggests none-minimal depression severity 5-9 suggests mild depression severity 10-14 suggests moderate depression severity 15-19 suggests moderately severe depression severity and 20-27 suggests severe depression severity The instrument also includes a functional health assessment which asks participants how emotional difficulties or problems impact work life at home or relationships with other people with responses ranging from not difficult at all to extremely difficult A PHQ-9 score 10 has a sensitivity of 88 and a specificity of 88 for major depression The PHQ-9 will be assessed at baseline post-intervention and weekly throughout the intervention
Biomarkers will be assessed via blood samples 20 ml collected by a certified phlebotomist for the quantification of plasma biomarkers Blood draws will be performed at baseline and post-intervention Plasma concentrations of the pro-inflammatory cytokines tumour necrosis factor-alpha TNF-α C-reactive protein CRP interleukin-6 IL-6 interleukin-1 beta IL-1β and interferon-gamma IFN-y will be quantified using 32x4 simple plex multianalyte cartridge for the Ella automated immunoassay system ProteinSimple San Jose California Each of the cytokines TNF-α IL-1β IL-6 and IFN-y have been shown to dysregulate the KYN pathway while CRP is a ubiquitous measure of inflammation Plasma concentrations of metabolites of the kynurenine pathway including tryptophan TRP kynurenine KYN kynurenic acid KYNA and quinolinic acid QUIN will be quantified in triplicate via enzyme-linked immunosorbent assay ImmuSmol Pessac France
In addition safety and adherence will be monitored throughout the intervention period via twice weekly phone calls Any incidence of treatment-emergent adverse events during the intervention will be recorded each week and compared between the taVNS and control groups A description of the adverse event number of events and total number of participants affected will be recorded Adherence will be assessed each week by the number of days whereby participants completed the full 4-hour session These phone calls will include completion of the PHQ-9 to monitor for any signs of worsening depression
However the potential benefits of a chronic vagus nerve stimulation intervention has not been assessed in individuals with SCI Transcutaneous auricular vagus nerve stimulation taVNS is a simple to administer and non-invasive neurostimulatory technique which can stimulate the vagus nerve via the skin of the ear Given that SCI is associated with chronic inflammation high rates of depression and reductions in vagal tone they may represent a population that would be particularly susceptible to the benefits of this low-burden low-cost treatment strategy
The overall objective of this study is to demonstrate that transcutaneous auricular vagus nerve stimulation taVNS therapy is a safe and feasible treatment which effectively activates the vagus nerve in individuals with SCI The study will also provide preliminary efficacy data related to the impact on symptoms of depression and inflammatory biomarkers
Participants will be randomized to receive either active taVNS therapy treatment group or sham taVNS therapy placebo group The intervention will be performed over a 30-day period and will follow the recommended daily stimulation of 4-hours per day with at least 1-hour carried out continuously for a total of 30 sessions
All participants will have an in-person baseline visit to determine optimal taVNS stimulation parameters and be trained on instructions for use For the active stimulation group stimulation will target the auricular branch of the vagus nerve by applying stimulation to the cymba conchae region of the left ear using the tVNS R device taVNS Technologies Erlangen Germany For the sham group stimulation will target the earlobe which will allow the participant to feel the stimulation while avoiding stimulation of the auricular branch of the vagus nerve To achieve adequate stimulation while avoiding unpleasant or painful sensations the stimulation intensity will be gradually increased in increments of 01mA until the subjective pain threshold is reached and then reduced to a stimulus intensity just below the individuals pain threshold expected range based on prior studies 1 - 32mA Pulse width will be set at 100μs and frequency will be set at 25Hz as performed in our previous protocol in spinal cord injured patients approved by Health Canada 364351 and shown to safely and effectively increase vagal tone The stimulation parameters determined during this in-person baseline visit will be locked for the duration of the 30-day intervention
Upon establishing appropriate stimulation parameters each participant will be trained on instructions for use As the tVNS R device is designed to be carried out independently by the patient instructions for use are simple and user friendly The participant will be instructed to 1 clean the ear using provided alcohol swabs 2 place the electrode in the ear in the appropriate orientation depending on group allocation 3 turn the device on by pressing the ON button and 4 begin stimulation by pressing the STARTSTOP button once Participants may then place the device in their pocket and go about their daily activities as normal The device will display percent completion of the daily 4-hour stimulation period so that participants are aware of there daily progress and when the session is complete
At the initial study visit as well as the 30-day post study visit participants will also undergo an assessment of heart rate variability HRV depression and inflammatory biomarkers
HRV will be assessed via electrocardiogram ECG to assess changes in autonomic function related to vagal tone For the collection of ECG signals participants will be instructed to avoid caffeine alcohol and strenuous exercise for at least 24 hours prior to assessment Participants will be instructed to remain relaxed focus on breathing and avoid speaking throughout the protocol ECG recording will be collected using the Polar H10 heart monitor Continuous heart rate will be recorded for a period of 5-minutes to obtain a baseline measure This process will be repeated following the 30-day intervention period at the post testing session ECG data will be imported to Kubios software for analysis of root mean square of successive differences RMSSD as well as high frequency HF power RMSSD is a time domain measure of heart rate variability corresponding to the variability in the intervals between successive heartbeats and is a measure of vagal tone HF power is a frequency domain measure of heart rate variability corresponding to heart rate fluctuations occurring in the frequency range of 015 to 04Hz and also reflects vagal tone RMSSD which is less influenced by breathing rate will be the primary assessment of vagal tone and HF power will be assessed to ensure consistency in measures Measures of vagal tone will be assessed at baseline and post-intervention to assess whether the intervention successfully targets the vagus nerve and increases vagal tone
Depression will be assessed via the Patient Health Questionnaire PHQ-9 at baseline and 30-days post-intervention The PHQ-9 has been shown to be a valid assessment for major depressive disorder in individuals with SCI The PHQ-9 is a 9-item questionnaire with items pertaining to feelings over the previous 2-weeks Each item is scored on a scale from 0 not at all to 3 nearly every day with total scores allowing for assessment of depression severity A score ranging from 0-4 suggests none-minimal depression severity 5-9 suggests mild depression severity 10-14 suggests moderate depression severity 15-19 suggests moderately severe depression severity and 20-27 suggests severe depression severity The instrument also includes a functional health assessment which asks participants how emotional difficulties or problems impact work life at home or relationships with other people with responses ranging from not difficult at all to extremely difficult A PHQ-9 score 10 has a sensitivity of 88 and a specificity of 88 for major depression The PHQ-9 will be assessed at baseline post-intervention and weekly throughout the intervention
Biomarkers will be assessed via blood samples 20 ml collected by a certified phlebotomist for the quantification of plasma biomarkers Blood draws will be performed at baseline and post-intervention Plasma concentrations of the pro-inflammatory cytokines tumour necrosis factor-alpha TNF-α C-reactive protein CRP interleukin-6 IL-6 interleukin-1 beta IL-1β and interferon-gamma IFN-y will be quantified using 32x4 simple plex multianalyte cartridge for the Ella automated immunoassay system ProteinSimple San Jose California Each of the cytokines TNF-α IL-1β IL-6 and IFN-y have been shown to dysregulate the KYN pathway while CRP is a ubiquitous measure of inflammation Plasma concentrations of metabolites of the kynurenine pathway including tryptophan TRP kynurenine KYN kynurenic acid KYNA and quinolinic acid QUIN will be quantified in triplicate via enzyme-linked immunosorbent assay ImmuSmol Pessac France
In addition safety and adherence will be monitored throughout the intervention period via twice weekly phone calls Any incidence of treatment-emergent adverse events during the intervention will be recorded each week and compared between the taVNS and control groups A description of the adverse event number of events and total number of participants affected will be recorded Adherence will be assessed each week by the number of days whereby participants completed the full 4-hour session These phone calls will include completion of the PHQ-9 to monitor for any signs of worsening depression
Study Oversight
Has Oversight DMC:
None
Is a FDA Regulated Drug?:
False
Is a FDA Regulated Device?:
False
Is an Unapproved Device?:
None
Is a PPSD?:
None
Is a US Export?:
False
Is an FDA AA801 Violation?:
None