Attention Deficit Disorder With Hyperactivity Clinical Trial
Official title:
A Single-blind, Randomised, Sham Controlled, Phase IIa Exploratory Clinical Trial, to Examine the Safety and Efficacy of BGX-3006 (tPCS) on Paediatric ADHD Participants.
Children with ADHD display a certain brainwave profile which might be different to that of a
child who does not have ADHD. Treatment with tPCS (transcranial pulsed current stimulation)
has shown that this brainwave profile could possibly be altered to more closely resemble a
brainwave profile of a child who does not have ADHD. Researchers believe that by changing
this brainwave profile it might lessen symptoms of ADHD.
tPCS is a name used to describe the type of current this device produces. It involves
randomly (in no specific pattern) produced pulses of current at different times that the
brain picks up. These pulses of low current stimulate the brain in a certain way and affect
the brainwave activity.
Treatment is given by applying a low frequency current using small electrodes clipped to the
earlobes. The current comes from an external battery source. The pulses of current generated
by this device stimulate certain parts of the brain which result in a possible increased
control of attention and behaviour. This treatment has already been proven to be safe and
will not hurt your child.
Due to these specific parts of the brain being stimulated, and the positive results of
previous research, it seems possible to control certain functions in children suffering from
inattention and hyperactivity.
The idea of using tPCS stimulation as a possible way for helping children with confirmed
ADHD opens a new window to future research. The final goal of this device and research is to
offer a safe, non-invasive (conservative treatment that does not require piercing into the
body or the removal of tissue) treatment that can be used on a long-term basis and shows a
clear improvement of ADHD symptoms for children and even adults with ADHD.
- Inspection of Records: Investigators and institutions involved in the trial will permit
trial-related monitoring, audits, Independent Ethics Committee (IEC) review, and regulatory
inspection(s) by providing direct access to all trial records. In the event of an audit, the
investigator agrees to allow the sponsor, representatives of the sponsor and applicable
regulatory authorities access to all trial records. The confidentiality of records that can
identify participants will be protected, respecting the privacy and confidentiality rules in
accordance with regulatory requirements.
The investigator must promptly notify the sponsor of any audits scheduled by any regulatory
authorities and promptly forward copies of any audit reports received to the sponsor.
In order to ensure data accuracy, data for individual participant visits must be completed
as soon as possible/ during/ immediately following the visit. All completed data will be
reviewed, signed, and dated by the investigator in a timely manner.
- Database Management and Quality Control: Data management, including the development and
management of a database, will be performed in accordance with regulatory requirements. The
designated data management vendor will review the CRF data for completeness and accuracy. A
formal querying process will be followed whereby the data management group will request the
site personnel to clarify any apparent erroneous entries or inconsistencies and will request
additional information from the site as required.
Medical history/current medical conditions and adverse events will be coded using the
Medical dictionary for regulatory activities (MedDRA) terminology.
- Sample Size: As this research is exploratory in nature a sample size was calculated based
on some assumptions as there is no current data to compare in pediatrics, tPCS, and ADHD.
Since no preliminary data is available a clinically relevant improvement is regarded as a
15% shift on the total range of the two ADHD sub-scales (Inattention and
Hyperactivity/Impulsivity), with 9 items in each, i.e. 4.05 (=0.15 x 27 where items score 0
to 3 Likert scale). The standard deviation is estimated as range/6 = 27/6 = 4.5, i.e. the
total range of a Gaussian distribution was 6 standard deviation. A sampling ratio of 2:1 is
used. A sample size of 48 children (32:16) will have 80% power to detect a difference of
4.05 points between the groups when testing two-sided using Students t-test at the 0.05
level of significance.
Continuous data will be summarised using descriptive statistics. Categorical data will be
presented using N and % (using the number of participants without missing data in the
calculation). 95% confidence intervals will be determined for all data, where applicable. No
imputation of missing values will be performed in the calculation of summary statistics.
- Safety Data Analysis: The safety analyses will be performed for the safety population
only. All safety parameters (adverse events, physical examination findings, vital signs,
physical measurements and qEEG findings) will be summarised descriptively by treatment
group. The descriptive statistics will include the number of observations, mean, standard
deviation, median, minimum and maximum for continuous variables and number of observations
and their percentages for categorical variables. Changes from baseline as well as shift
tables will be provided for the safety laboratory parameters (within, below or above normal
range).
The analysis of adverse events will include all treatment emergent adverse events. Adverse
events will be coded using MedDRA and will be presented by system organ class and preferred
term for each treatment group.
- Efficacy Data
1. Primary Efficacy analysis:
The mean change in both the Inattention and Hyperactivity-Impulsive subscales of the
SNAP-IV-C rating scale as well as the Conners'3 Parent rating scale from baseline to
Day 42 will be calculated for each group. Mean changes from baseline at the other trial
time points (Days 0, 14, 28, and 42) will also be calculated.
The statistical analysis methods will consist of paired t-tests within groups and
analysis of Co-variance (ANCOVA) between groups for the change in assessments over
time. The paired t-tests will compare the change variable from before tPCS
administration to after tPCS within groups (active and sham condition). A one-way
ANCOVA, with factor groups (active or sham) and co-variance baseline value, will be
employed to compare groups with respect to change from baseline for estimated outcomes,
e.g. change in complete scores from baseline to 6-weeks for inattentive and
hyperactivity-impulsivity on SNAP-IV-C and Conners'3 Parent rating scales. Groups will
also be compared over time (Days 0, 14, 28 and 42) using a linear mixed model analysis
and of particular interest will be the interaction between group and time.
2. Secondary Efficacy analysis:
The mean change in the psychometric test-battery from baseline to Day 42 will be calculated
for each group. Mean changes from baseline at the other trial time points (Days 0, 14, 28,
and 42) will also be calculated.
The statistical analysis methods will consist of paired t-tests within groups and analysis
of Co-variance (ANCOVA) between groups for the change in assessments over time. The paired
t-tests will compare the change variable from before tPCS administration to after tPCS
within groups (active and sham condition). A one-way ANCOVA, with factor groups (active or
sham) and co-variance baseline value, will be employed to compare groups with respect to
change from baseline for estimated outcomes, e.g. change in complete scores from baseline to
6-weeks for the psychometric test-battery. Groups will also be compared over time (Days 0,
14, 28 and 42) using a linear mixed model analysis for repeated measures and of particular
interest will be the interaction between group and time.
EEG analysis Power spectra will be determined for each epoch of data for the
frequency-domain analysis. Mean and median power frequencies will be calculated within each
of the 4 EEG frequency bands (intraband) and over the entire EEG range (interband). Also,
the band power fractions or relative amount of power within an EEG band with respect to the
total amount of spectrum power will be determined. The coherence analysis will be completed
using two bands (alpha and theta) and four sub-bands (low-alpha (8-10 Hz), high-alpha (10-12
Hz), low-beta (12-20 Hz), and high-beta (20-30 Hz)). We will use the Welch's averaged
modified periodogram method to find the estimated coherence of signal x and y, representing
each electrode site. It is a function of the power spectral densities of x and y and their
cross power spectral density. Groups will also be compared over time (Days 0, 42 and 84)
using a linear mixed model analysis for repeated measures and of particular interest will be
the interaction between group and time.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Subject), Primary Purpose: Treatment
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