Tourette Syndrome Clinical Trial
Official title:
Developing New Treatments for Tourette Syndrome: Therapeutic Trials With Modulators of Glutamatergic Neurotransmission
Verified date | January 2018 |
Source | Johns Hopkins University |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
A joint NIH -Tourette Syndrome Association Conference has emphasized the critical need for
the testing and development of new pharmacotherapy for tic suppression in Tourette syndrome
(TS). This submission is a safety, tolerability and efficacy pilot study using two
medications that modulate glutamate neurotransmission, riluzole, a glutamate antagonist, and
D-serine, a glutamate agonist. Glutamate is the primary excitatory neurotransmitter in the
central nervous system, an essential component of pathways implicated in TS and an extensive
modulator of dopamine, the major neurotransmitter associated with tics.
This is a single site, short-term, proof of concept study of riluzole and D-serine for the
treatment of tics. Each medication will be evaluated and compared to placebo as part of a
double-blind, randomized, parallel, flexible dose, three-arm, 8-week, treatment protocol
(D-serine, riluzole, or placebo). A total of sixty patients (age 8-17 years) with TS and
moderate to moderately-severe tics will receive study medication according to a 2:1 (dopamine
modulating drug: placebo), randomized schedule, i.e., riluzole (n=24), D-serine (n=24),
placebo (n=12). The primary outcome measure is tic suppression as determined by changes in
the Total Tic Subscore of the Yale Global Tic Severity Scale (YGTSS). Secondary tic outcome
measures include changes in the YGTSS Total Score and two Global Impression Scales. Further,
since both riluzole and D-serine have been proposed as treatments for obsessive-compulsive
behaviors, a TS co-morbidity, these symptoms will be followed. Safety measures include serial
physical examinations, vital signs, laboratory studies (comprehensive metabolic panel,
complete blood count, plasma amino acids, and urine analyses), documentation of side effects
and adverse events, and measurement of changes in ADHD, depression and anxiety.
This pilot investigation will provide important proof-of-concept data on glutamate therapies
for TS and, in turn, evidence for large-scale, multi-center clinical trials.
Status | Completed |
Enrollment | 39 |
Est. completion date | September 2013 |
Est. primary completion date | September 2013 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 8 Years to 17 Years |
Eligibility |
Inclusion Criteria: - Tourette syndrome (criteria based on the TS Classification Study Group), which includes onset before 18 years, multiple involuntary motor tics, one or more vocal tics, a waxing and waning course, the gradual replacement of old symptoms with new ones, the presence of tics for more than one year, the absence of other medical explanations (effects of a substance (e.g., stimulants) or a general medical condition for tics, and observation of tics by a reliable examiner) or Chronic Motor Tic disorder (criteria similar to Tourette syndrome except for the absence of vocal tics) - Age 8-17 years, either gender - Observable tics, achieving a minimum score of > 22 on the Total Tic score of Yale Global Tic Severity Scale (YGTSS) - Tic symptoms severe enough to warrant therapy (e.g., causing psycho-social or physical difficulty) - Written informed consent provided by the patient's parent (or legal guardian) and assent provided by the patient consistent with Institutional Review Board requirements - Ability and willingness to comply with study protocol requirements - Women of childbearing potential must be using a medically acceptable contraceptive method. Acceptable methods of birth control are limited to: Intra-Uterine Device (IUD), oral, implantable, injectable contraceptives and estrogen patch, double barrier method (spermicide+diaphragm), or abstinence - Baseline weight of at least 33 kilograms - Tic-suppressing drug naive, or currently not on treatment for TS (off medications for at least three weeks), or if, in the judgment of the PI, they are not adequately managed using current therapy (prescribed for greater than one month) and are willing to maintain a constant dose throughout the protocol. Exclusion Criteria: - Secondary tics - Significant medical illness (metabolic, endocrine, cardiac, hematological, gastrointestinal, pulmonary, epilepsy) - Current major depression - generalized anxiety disorder - separation anxiety disorder - psychotic symptoms (based on clinical evaluation and the results of the CY-BOCS, CDI-S, and MASC evaluations) - pervasive developmental disorder - autism - mental retardation (I.Q. less than 70) - anorexia/bulimia, or substance abuse - Any other conditions that in the opinion of the Investigators would interfere with the evaluation of the results or constitute a health hazard for the patient - Pregnancy - Hypersensitivity to D-serine or riluzole - Abnormal laboratory values on screening laboratory testing if clinically significant at the Principal Investigator's discretion. Subjects with co-morbid ADHD, obsessive compulsive disorder (OCD), and conduct disorder will not be excluded as long as these diagnoses are not the subject's primary problem |
Country | Name | City | State |
---|---|---|---|
United States | Johns Hopkins University | Baltimore | Maryland |
Lead Sponsor | Collaborator |
---|---|
Johns Hopkins University | National Institute of Mental Health (NIMH) |
United States,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | The Change From Baseline to 6-week Scores for The Total Tic Subscale (TTS) | The primary outcome measure is effective tic suppression as determined by the difference in the Total Tic subscale (TTS) scores of the Yale Global Tic Severity Scale (YGTSS) at baseline and 6 weeks. i) Yale Global Tic Severity Scale (YGTSS): The YGTSS is a semi-structured clinical interview designed to measure current tic severity. It is comprised of two parts, a tic score (0-50) and a total impairment score (0-50). The Total Tic Score (TTS: 0-50) has been selected as the primary outcome measure. The scale ranges from 0 (the best possible outcome) to 50 (the worst possible outcome). This scale is considered the best currently available scale to rate the severity of tics. The data provided below represents the mean change (baseline minus six week) for the D-serine group (n = 9), Riluzole (n = 10), and Placebo group (n = 5). For consistency, all values weather positive or negative represent baseline minus week 6. |
Baseline and 6-weeks | |
Secondary | The Change From Baseline to 6-week Scores for the Yale Global Tic Severity Scale (YGTSS) Total Score. | i) Yale Global Tic Severity Scale (YGTSS): The YGTSS is a semi-structured clinical interview designed to measure current tic severity. It is comprised of two parts, a tic score (0-50) and a total impairment score (0-50), total maximum score is 100. This scale has established validity, as assessed by Dr. Walkup and colleagues and is considered the best currently available scale to rate the severity of tics. This scale ranges from 0 (the best possible outcome) to 100 (the worst possible outcome). The data provided below represents the mean change (baseline minus six week) for the D-serine group (n = 9), Riluzole (n = 10), and Placebo group (n = 5). For consistency, all values weather positive or negative represent baseline minus week 6. Please note that summary data (mean and standard deviation per group) were intended to be reported, and not participant level data (i.e. each individual data point of every subject per group). |
Baseline and 6-weeks | |
Secondary | The Change From Baseline to 6-week Score for the Clinical Global Impression -Improvement (CGI-I). | Clinical Global Impression-Improvement (CGI-I): The CGI-I is used to compare current severity to baseline. A score of 1 corresponds to "very much improved"; 2 equals "much improved;" 3 denotes "minimal change"; and 4 represents "no change." Scores above 4 are used to indicate deterioration, i.e., 5 equals "minimally worse;" 6 is "much worse;" and 7 is "very much worse." The data provided below represents the mean change (baseline minus six week) for the D-serine group (n = 9), Riluzole (n = 10), and Placebo group (n = 5). For consistency, all values weather positive or negative represent baseline minus week 6. Please note that summary data (mean and standard deviation per group) were intended to be reported, and not participant level data (i.e. each individual data point of every subject per group). |
Baseline and 6-weeks | |
Secondary | The Change From Baseline to 6-week Score for the Patient Global Impression of Improvement (PGI-I). | Patient Global Impression of Improvement (PGI-I) is a single seven point scale in which the patient/parent is asked to assess the change in overall condition ranging from "very much" improved to "very much worse." A score of 1 corresponds to "very much better"; 2 equals "much better;" 3 denotes "a little better"; and 4 represents "no change." Scores above 4 are used to indicate deterioration, i.e., 5 equals "a little worse;" 6 is "much worse;" and 7 is "very much worse." The data provided below represents the mean change (baseline minus six week) for the D-serine group (n = 9), Riluzole (n = 10), and Placebo group (n = 5). For consistency, all values weather positive or negative represent baseline minus week 6. Please note that only summary data (mean and standard deviation per group) were intended to be reported, and not participant level data (i.e. each individual data point of every subject per group)--this applies to all outcome measures reported in the results. |
Baseline and 6 weeks | |
Secondary | Changes in the Children's Yale-Brown Obsessive-Compulsive Scale (CY-BOCS) From Baseline to 6-weeks. | Secondary outcome for obsessive-compulsive behaviors will be measured by changes in the Children's Yale-Brown Obsessive-Compulsive Scale (CY-BOCS) from baseline to 6-weeks. The severity of OCD was evaluated using either the Child Yale-Brown Obsessive Compulsive Scale (CY-BOCS) or Yale-Brown Obsessive Compulsive Scale (Y-BOCS). The (C)Y-BOCS is the most widely used instrument to assess the severity of obsessive-compulsive symptoms in research studies involving children. The (C)Y-BOCS has well established psychometric properties. The scale ranges from 0 (the best possible outcome) to 10 (the worst possible outcome). The data provided below represents the mean change (baseline minus six week) for the D-serine group (n = 9), Riluzole (n = 10), and Placebo group (n = 5). For consistency, all values weather positive or negative represent baseline minus week 6. |
Baseline and 6-weeks | |
Secondary | The Change From Baseline to 6-week in Plasma Amino Acid Levels | Blood testing was performed at baseline and at each clinic visit. Data shown below reflects baseline Glutamic Acid minus Week 6 Glutamic Acid, and baseline Serine minus Week 6 Serine levels; as acquired from the blood tests during these respective clinic visits. | Baseline and 6 weeks. | |
Secondary | The Change From Baseline to 6-week in Scores of the DuPaul Attention Deficit Hyperactivity Disorder Rating Scale. | DuPaul ADHD Rating Scale: The presence of ADHD symptoms will be assessed using the DSM-IV version of the ADHD rating scale developed by DuPaul. This scale has been normed in large clinical and community samples and has excellent psychometric properties including a test-retest reliability over a 2-week period of 0.93 and significant correlations with direct observations of classroom behavior. The scale has a maximum possible score of 72, and a minimum of 0. The scale ranges from 0 (the best possible outcome) to 70 (the worst possible outcome). The data provided below represents the mean change (baseline minus six week) for the D-serine group (n = 9), Riluzole (n = 10), and Placebo group (n = 5). For consistency, all values weather positive or negative represent baseline minus week 6. |
Baseline and 6 weeks | |
Secondary | The Change From Baseline to 6-week in Scores of the Child Depression Inventory - Short Version (CDI-S) Scale | Depression Inventory-Short Version (DI-S): Depression severity will be rated by using the Depression Inventory-Short Version (DI-S). This 10 item scale takes about 5 minutes to complete. It has excellent psychometric properties and is designed for repeated administrations over time. The maximum possible score of 20, and a minimum score of 0. Higher score on this scale indicates greater severity of depression in children. The data provided below represents the mean change (baseline minus six week) for the D-serine group (n = 9), Riluzole (n = 10), and Placebo group (n = 3). For consistency, all values weather positive or negative represent baseline minus week 6. |
Baseline and 6-weeks | |
Secondary | The Change From Baseline to 6-week in Scores of the Multi-Dimensional Anxiety Scale for Children (MASC) | Multidimensional Anxiety Scale (MAS): Anxiety will be followed using the Multidimensional Anxiety Scale for Children (MASC), which has been developed by Dr. John March at Duke University and is now considered the preferred instrument for rating anxiety. The MASC asks the patient how they have been thinking and acting recently. It has a maximum possible score of 117 and a minimum score of 0. Higher score on this scale indicates greater severity of anxiety in children. The data provided below represents the mean change (baseline minus six week) for the D-serine group (n = 9), Riluzole (n = 10), and Placebo group (n = 5). For consistency, all values weather positive or negative represent baseline minus week 6. |
Baseline and 6-weeks | |
Secondary | Expanded Pittsburgh Side Effect Scale Modified to Include Side Effects of Riluzole and D-serine. | The scale consists of 25 items with a score of 0 to 3 per item. 0- none, 1- mild, 2- moderate and 3- severe side effect. The total could be zero (no side effects) to 75 or higher.The scale also allows for the addition of other side effects not included in the original scale and the total score could potentially be higher than 75. If no other side effects outside of the original scale are recorded, the the maximum score remains at 75. | Baseline | |
Secondary | Expanded Pittsburgh Side Effect Scale Modified to Include Side Effects of Riluzole and D-serine. | The scale consists of 25 items with a score of 0 to 3 per item. 0- none, 1- mild, 2- moderate and 3- severe side effect. The total could be zero (no side effects) to 75 or higher.The scale also allows for the addition of other side effects not included in the original scale and the total score could potentially be higher than 75. If no other side effects outside of the original scale are recorded, the the maximum score remains at 75. | Week 2 | |
Secondary | Expanded Pittsburgh Side Effect Scale Modified to Include Side Effects of Riluzole and D-serine. | The scale consists of 25 items with a score of 0 to 3 per item. 0- none, 1- mild, 2- moderate and 3- severe side effect. The total could be zero (no side effects) to 75 or higher.The scale also allows for the addition of other side effects not included in the original scale and the total score could potentially be higher than 75. If no other side effects outside of the original scale are recorded, the the maximum score remains at 75. | Week 4 | |
Secondary | Expanded Pittsburgh Side Effect Scale Modified to Include Side Effects of Riluzole and D-serine. | The scale consists of 25 items with a score of 0 to 3 per item. 0- none, 1- mild, 2- moderate and 3- severe side effect. The total could be zero (no side effects) to 75 or higher.The scale also allows for the addition of other side effects not included in the original scale and the total score could potentially be higher than 75. If no other side effects outside of the original scale are recorded, the the maximum score remains at 75. | Week 6 | |
Secondary | Expanded Pittsburgh Side Effect Scale Modified to Include Side Effects of Riluzole and D-serine. | The scale consists of 25 items with a score of 0 to 3 per item. 0- none, 1- mild, 2- moderate and 3- severe side effect. The total could be zero (no side effects) to 75 or higher.The scale also allows for the addition of other side effects not included in the original scale and the total score could potentially be higher than 75. If no other side effects outside of the original scale are recorded, the the maximum score remains at 75. | Week 8 |
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