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Serotonergic Modulation of Motor Function in Subacute and Chronic SCI

Primary Purpose

Spinal Cord Injury

Status
Unknown status
Phase
Phase 1
Locations
United States
Study Type
Interventional
Intervention
Lexapro
Placebo
Sponsored by
Shirley Ryan AbilityLab
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Spinal Cord Injury focused on measuring Gait training, Lexapro, Tizanidine

Eligibility Criteria

18 Years - 65 Years (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  • age of subjects between 18 and 65 years of age, due to the effects of greater age on functional recovery of ambulation (Penrod et al. 1990);
  • medically stable with medical clearance from the subject's primary internist or physiatrist to participate;
  • level of the lesion between C5-T10 spinal cord level due to non-progressive etiology;
  • <6 months or >1 yr since initial injury. Range of motion requirements include: ankle dorsiflexion ankle to 10 degrees and plantarflexion to 30 degrees, knee flexion from 0 to 120 degrees, hip flexion to 90 degrees, and hip extension to 10 degrees.

Exclusion Criteria:

  • presence of concurrent severe medical illness, including unhealed decubiti, existing infection, cardiovascular disease, significant osteoporosis (as indicated by history of fractures following injury)
  • active heterotrophic ossification in the lower extremities
  • known history of peripheral nerve injury in lower legs
  • history of known traumatic head injury
  • a history of cardiovascular or pulmonary complications, including significant obstructive and/or restrictive lung diseases
  • inability to tolerate 30 minutes of standing without orthostasis (decrease in blood pressure by 20 mmHg systolic and 10 mmHg diastolic)
  • individuals who are undergoing concurrent physical therapy will be excluded to eliminate confounding effects
  • women of childbearing potential will not be excluded, although women who are pregnant will be excluded due to the lack of proven safety of pharmacological agents in pregnant women
  • cranial stimulation exclusions: history of epilepsy or a seizure event, metal implants in the head or face, unexplained and recurring headaches, skull abnormalities or fractures, implanted cardiac pacemaker or suffered a concussion within the last 6 months
  • interactions with other medications or previous sensitivity to SSRIs, 5-HT antagonists or anti-histamines
  • patients prescribed medications for alleviation of spastic motor behaviors, anti-depressant medications, or other medications with known interactions to SSRIs will be excluded from participation unless both attending physician and patient agree to cease all such medications during the evaluation and training period. A 14-day minimum washout period for all such medications will be utilized
  • patients with known liver, renal, or other metabolic disease that may interfere with drug action and/or clearance will be excluded from the proposed study. The low daily dosage of the agent to be used (10 mg Lexapro and 16 mg Cypro) has shown very little side effects with patients with hepatic or renal disease
  • patients who are diagnosed or previously diagnosed with depression will be excluded. A preliminary screening tool (Center for Epidemiological Studies - Depression Scale) will be administered to all patients. Scores > 16 indicate symptoms of depression. For those patients, a physician will be required to evaluate the subject to determine eligibility.

Sites / Locations

  • Rehabilitation Institute of Chicago

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Active Comparator

Arm Label

Gait Training with Lexapro

Gait Training with Placebo

Arm Description

Gait training 2 weeks, gait training 4 weeks (3 X week) with Lexapro (10mg SSRI), wash out period of 1 week, gait training, for 4 weeks with placebo (10 mg). Patients will also be provided prescribed TIZ by their physician to help control of spastic motor behaviors.

Gait training 2 weeks, gait training for 4 weeks (3X week) with Placebo (10 mg), wash out period of 1 week, gait training for 4 weeks with Lexapro(10 mg). Patients will also be provided prescribed TIZ by their physician to help control of spastic motor behaviors.

Outcomes

Primary Outcome Measures

Walking Index for Spinal Cord Injury (WISCI II)
Evaluation of bracing, assistive device, and assistance required for ambulation

Secondary Outcome Measures

Volitional Strength
Ankle, knee, hip flexors/extensors strength (Nm) tested bilaterally (Biodex®)
Gait kinematics
Kinematic excursions of hip/knee/ankle (Motion Analysis®)
Fastest possible walking velocity over ground (FV; m/s)
Subject walks a distance of 10m with the middle 6m being timed. Instructions to walk normal comfortable pace.
Six minute walking distance (m)
Subject asked to walk normal comfortable pace for 6 minutes. Total distance is recorded. Subject can take rest breaks as needed but are encouraged to continue walking throughout the 6 minutes.
Lower Extremity Motor Scores (LEMS)
Measure of lower extremity muscle strength on 0-5 point scale
Modified Ashworth of knee extensors/flexors (ModAsh)
Measure of spasticity of knee flexors and extensors during passive range of motion
Spinal Cord Assessment Tool for Spasticity (SCATS)
Measure of spasticity tested in supine
Peak Treadmill Velocity
Peak treadmill speed during graded treadmill testing

Full Information

First Posted
February 7, 2013
Last Updated
April 18, 2019
Sponsor
Shirley Ryan AbilityLab
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1. Study Identification

Unique Protocol Identification Number
NCT01788969
Brief Title
Serotonergic Modulation of Motor Function in Subacute and Chronic SCI
Official Title
Serotonergic Modulation of Motor Function in Subacute and Chronic SCI
Study Type
Interventional

2. Study Status

Record Verification Date
April 2019
Overall Recruitment Status
Unknown status
Study Start Date
June 2005 (undefined)
Primary Completion Date
December 2016 (Actual)
Study Completion Date
December 2019 (Anticipated)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Principal Investigator
Name of the Sponsor
Shirley Ryan AbilityLab

4. Oversight

Data Monitoring Committee
No

5. Study Description

Brief Summary
The manifestation of weakness and involuntary reflexes following motor incomplete spinal cord injury (SCI) may be partly a result of damage to descending pathways to the spinal cord that release serotonin. In models of SCI, for example, application of agents that simulate serotonin has been shown to modulate voluntary motor behaviors, including augmentation of walking recovery. In humans following neurological injury, the effects of 5HT agents are unclear. Few previous reports indicate improved motor function following administration of agents which enhance the available serotonin in the brain, although some data suggests that decreased serotonin may be beneficial. In this application, the investigators propose to study the effects of clinically used agents that increase or decrease intrinsic serotonin activity in the brain on strength and walking ability following human motor incomplete SCI. Using detailed electrophysiological recordings, and biomechanical and behavioral measures, the investigators will determine the effects of acute or chronic doses of these drugs on voluntary and involuntary motor behaviors during static and dynamic conditions. The novelty of this proposed research is the expectation that agents that enhance serotonin activity may increase abnormal reflexes in SCI, but simultaneously facilitate motor and walking recovery. Despite potential improvements in voluntary function, the use of pharmacological agents that may enhance spastic motor behaviors following SCI is in marked contrast to the way in which drugs are typically used in the clinical setting.
Detailed Description
The proposed study will consist of a double-blinded, randomized controlled trial using a crossover design to assess the effects of SSRIs (escitalopram oxalate, Lexapro®, Forest Pharmaceuticals, Inc) and 5HT-antagonists (cyproheptadine [CYPRO], Periactin ®, Merck, Inc) on volitional and spastic motor behaviors in subjects with motor incomplete SCI following both acute and chronic medication delivery. Voluntary and reflexive motor behaviors in 120 subjects with SCI will be assessed. These interventions will be applied to individuals with acute (< 6 months post injury) chronic (> 1 year post injury) motor incomplete SCI to determine both the rate and extent of changes in volitional motor performance and involuntary spastic behaviors. For the training portion of the study (referred to as subproject 2 below), a portion of the acute and chronic subjects will be evaluated every 2 weeks for up to16 weeks and participate in locomotor training, to investigate and better understand changes in motor function and recovery in individuals with spinal cord injuries. Following 2-4 weeks of this training, individuals will be given either the study drug, or placebo and continue evaluation and training. Following an additional 4 weeks, subjects will be given either the placebo or study drug (whichever they did not receive during the prior 4 weeks). The order will be randomized.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Spinal Cord Injury
Keywords
Gait training, Lexapro, Tizanidine

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 1
Interventional Study Model
Crossover Assignment
Masking
ParticipantCare ProviderInvestigatorOutcomes Assessor
Allocation
Randomized
Enrollment
42 (Actual)

8. Arms, Groups, and Interventions

Arm Title
Gait Training with Lexapro
Arm Type
Experimental
Arm Description
Gait training 2 weeks, gait training 4 weeks (3 X week) with Lexapro (10mg SSRI), wash out period of 1 week, gait training, for 4 weeks with placebo (10 mg). Patients will also be provided prescribed TIZ by their physician to help control of spastic motor behaviors.
Arm Title
Gait Training with Placebo
Arm Type
Active Comparator
Arm Description
Gait training 2 weeks, gait training for 4 weeks (3X week) with Placebo (10 mg), wash out period of 1 week, gait training for 4 weeks with Lexapro(10 mg). Patients will also be provided prescribed TIZ by their physician to help control of spastic motor behaviors.
Intervention Type
Drug
Intervention Name(s)
Lexapro
Other Intervention Name(s)
escitalopram
Intervention Description
Agent + training vs Placebo + training
Intervention Type
Drug
Intervention Name(s)
Placebo
Other Intervention Name(s)
microcrystalline dextrose
Intervention Description
Agent + training vs Placebo + training
Primary Outcome Measure Information:
Title
Walking Index for Spinal Cord Injury (WISCI II)
Description
Evaluation of bracing, assistive device, and assistance required for ambulation
Time Frame
Compare changes in WISCI II pre to post training with placebo to pre to post training with Lexapro during a 10-12 week time period.
Secondary Outcome Measure Information:
Title
Volitional Strength
Description
Ankle, knee, hip flexors/extensors strength (Nm) tested bilaterally (Biodex®)
Time Frame
Pre Training (Day 1), Pre Drug B (approx end of week 5), Post Final (approx end of week 10)
Title
Gait kinematics
Description
Kinematic excursions of hip/knee/ankle (Motion Analysis®)
Time Frame
Pre Training (Day 1), Pre Drug A (approx end of week 2), Post Drug A (approx end of week 4), Pre Drug B (approx end of week 5), Post Drug B (approx end of week 9), Post-Final (approx end of week 10)
Title
Fastest possible walking velocity over ground (FV; m/s)
Description
Subject walks a distance of 10m with the middle 6m being timed. Instructions to walk normal comfortable pace.
Time Frame
Pre Training (Day 1), Pre Drug A (approx end of week 2), Post Drug A (approx end of week 4), Pre Drug B (approx end of week 5), Post Drug B (approx end of week 9), Post-Final (approx end of week 10)
Title
Six minute walking distance (m)
Description
Subject asked to walk normal comfortable pace for 6 minutes. Total distance is recorded. Subject can take rest breaks as needed but are encouraged to continue walking throughout the 6 minutes.
Time Frame
Pre Training (Day 1), Pre Drug A (approx end of week 2), Post Drug A (approx end of week 4), Pre Drug B (approx end of week 5), Post Drug B (approx end of week 9), Post-Final (approx end of week 10)
Title
Lower Extremity Motor Scores (LEMS)
Description
Measure of lower extremity muscle strength on 0-5 point scale
Time Frame
Pre Training (Day 1), Pre Drug A (approx end of week 2), Post Drug A (approx end of week 4), Pre Drug B (approx end of week 5), Post Drug B (approx end of week 9), Post-Final (approx end of week 10)
Title
Modified Ashworth of knee extensors/flexors (ModAsh)
Description
Measure of spasticity of knee flexors and extensors during passive range of motion
Time Frame
Pre Training (Day 1), Pre Drug A (approx end of week 2), Post Drug A (approx end of week 4), Pre Drug B (approx end of week 5), Post Drug B (approx end of week 9), Post-Final (approx end of week 10)
Title
Spinal Cord Assessment Tool for Spasticity (SCATS)
Description
Measure of spasticity tested in supine
Time Frame
Pre Training (Day 1), Pre Drug A (approx end of week 2), Post Drug A (approx end of week 4), Pre Drug B (approx end of week 5), Post Drug B (approx end of week 9), Post-Final (approx end of week 10)
Title
Peak Treadmill Velocity
Description
Peak treadmill speed during graded treadmill testing
Time Frame
Compare changes in peak treadmill velocity pre to post training with placebo to pre to post training with Lexapro during a 10-12 week time period.

10. Eligibility

Sex
All
Minimum Age & Unit of Time
18 Years
Maximum Age & Unit of Time
65 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: age of subjects between 18 and 65 years of age, due to the effects of greater age on functional recovery of ambulation (Penrod et al. 1990); medically stable with medical clearance from the subject's primary internist or physiatrist to participate; level of the lesion between C5-T10 spinal cord level due to non-progressive etiology; <6 months or >1 yr since initial injury. Range of motion requirements include: ankle dorsiflexion ankle to 10 degrees and plantarflexion to 30 degrees, knee flexion from 0 to 120 degrees, hip flexion to 90 degrees, and hip extension to 10 degrees. Exclusion Criteria: presence of concurrent severe medical illness, including unhealed decubiti, existing infection, cardiovascular disease, significant osteoporosis (as indicated by history of fractures following injury) active heterotrophic ossification in the lower extremities known history of peripheral nerve injury in lower legs history of known traumatic head injury a history of cardiovascular or pulmonary complications, including significant obstructive and/or restrictive lung diseases inability to tolerate 30 minutes of standing without orthostasis (decrease in blood pressure by 20 mmHg systolic and 10 mmHg diastolic) individuals who are undergoing concurrent physical therapy will be excluded to eliminate confounding effects women of childbearing potential will not be excluded, although women who are pregnant will be excluded due to the lack of proven safety of pharmacological agents in pregnant women cranial stimulation exclusions: history of epilepsy or a seizure event, metal implants in the head or face, unexplained and recurring headaches, skull abnormalities or fractures, implanted cardiac pacemaker or suffered a concussion within the last 6 months interactions with other medications or previous sensitivity to SSRIs, 5-HT antagonists or anti-histamines patients prescribed medications for alleviation of spastic motor behaviors, anti-depressant medications, or other medications with known interactions to SSRIs will be excluded from participation unless both attending physician and patient agree to cease all such medications during the evaluation and training period. A 14-day minimum washout period for all such medications will be utilized patients with known liver, renal, or other metabolic disease that may interfere with drug action and/or clearance will be excluded from the proposed study. The low daily dosage of the agent to be used (10 mg Lexapro and 16 mg Cypro) has shown very little side effects with patients with hepatic or renal disease patients who are diagnosed or previously diagnosed with depression will be excluded. A preliminary screening tool (Center for Epidemiological Studies - Depression Scale) will be administered to all patients. Scores > 16 indicate symptoms of depression. For those patients, a physician will be required to evaluate the subject to determine eligibility.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Thomas G Hornby, PhD, PT
Organizational Affiliation
Rehabiltiation Institute of Chicago/UIC
Official's Role
Principal Investigator
Facility Information:
Facility Name
Rehabilitation Institute of Chicago
City
Chicago
State/Province
Illinois
ZIP/Postal Code
60611
Country
United States

12. IPD Sharing Statement

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Serotonergic Modulation of Motor Function in Subacute and Chronic SCI

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