Modulation of Episodic Memory Using Theta Burst Stimulation (TBS)
| Status: | Withdrawn |
|---|---|
| Conditions: | Healthy Studies |
| Therapuetic Areas: | Other |
| Healthy: | No |
| Age Range: | 60 - 80 |
| Updated: | 9/8/2018 |
| Start Date: | December 15, 2018 |
| End Date: | December 30, 2019 |
The goal of this study is to evaluate the effect of white matter guided theta burst
stimulation on episodic memory task performance in healthy older adults. The investigators
aim to propagate the effect of theta burst stimulation from a superficial locus of
stimulation (angular gyrus) to hippocampus and parahippocampal regions using white matter
tract connection between these regions. Study activities and population group - for the study
plans to recruit 20 healthy older adults who already have white matter scans acquired as part
of another study performed by the Cabeza Lab at Duke University.
Using tractography the exact site of stimulation on the cortical surface will be localized.
An initial motor evoked potential (MEP) assessment will differentiate responders to theta
burst stimulation from non responders. Responders will receive 1200 pulses of intermittent
theta burst stimulation (iTBS) or sham stimulation to the angular gyrus while they perform
the encoding portion of an episodic memory task. There after, they will perform retrieval
piece of the task and data analysis will compare these performances.
stimulation on episodic memory task performance in healthy older adults. The investigators
aim to propagate the effect of theta burst stimulation from a superficial locus of
stimulation (angular gyrus) to hippocampus and parahippocampal regions using white matter
tract connection between these regions. Study activities and population group - for the study
plans to recruit 20 healthy older adults who already have white matter scans acquired as part
of another study performed by the Cabeza Lab at Duke University.
Using tractography the exact site of stimulation on the cortical surface will be localized.
An initial motor evoked potential (MEP) assessment will differentiate responders to theta
burst stimulation from non responders. Responders will receive 1200 pulses of intermittent
theta burst stimulation (iTBS) or sham stimulation to the angular gyrus while they perform
the encoding portion of an episodic memory task. There after, they will perform retrieval
piece of the task and data analysis will compare these performances.
Aims and Hypotheses The purpose of the study is to evaluate the effect of theta burst
stimulation (TBS) which is a relatively new paradigm of transcranial magnetic stimulation
(TMS) on episodic memory (EM) in healthy older adults (hOA).
Aim1: Evaluate the effect of theta burst stimulation (TBS) on episodic memory (EM) in healthy
older adults. Hypothesis 1 - There will be significant improvement in EM compared to baseline
with one session of TBS.
Aim 2: Correlate white matter integrity to improvement in task retrieval with TBS. Hypothesis
2- Stronger white matter (WM) tract connections correlate to greater improvement in retrieval
performance.
BACKGROUND Alzheimer's disease (AD) affects 5 million Americans, at a cost of over 200
billion dollars. The first and most debilitating symptom of AD is a severe deficit in the
ability to remembering personal past events, or episodic memory (EM), which eventually
renders patients isolated from family and friends and unable to live independently. This EM
deficit reflects primarily the deterioration of medial temporal lobe regions, particularly
the hippocampus (HC). AD treatments must start very early in the disease progression, when
brain damage is still small, and the earliest stage when AD can be diagnosed is known as mild
cognitive impairment due to AD (MCI-AD).
Recently, different forms of noninvasive brain stimulation techniques have been applied to
healthy older adults, AD and MCI-AD to improve memory impairment. Most of these trials used
high-frequency repetitive transcranial magnetic stimulation (rTMS) applied to the left
dorsolateral prefrontal cortex (DLPFC). Although a small number of these studies have shown
beneficial effects, considerable questions remain as to whether TMS has clinically relevant
effects in elderly populations, as well as to what neuroscience-based mechanisms account for
these effects. An obstacle for using TMS to enhance EM is that the brain region most critical
for EM and most affected by early AD, the hippocampus (HC), is situated deep inside the
brain, beyond TMS direct effects (~1" below the skull). One study attempted to target
hippocampus and peri-hippocampal regions for stimulation via TMS. They stimulated the lateral
parietal cortex and utilized functional connectivity between this region and
hippocampus/peri-hippocampal regions (mainly entorhinal cortex) to enhance performance on an
associative memory task. The inferior longitudinal fasciculus connects angular gyrus to
hippocampus and para-hippocampal regions, and could propagate stimulation effects from
cortical to subcortical structures, although studies on effect on TMS on white matter
neuronal populations are limited as detailed below. The effect of TMS on neuronal populations
in the white matter tracts was recently modeled using tractography and e-field calculations,
and increasingly, these approaches need to account for what percentage of variance in motor
threshold (MT) would be accounted for by white matter tracts.
TBS is a potent paradigm of TMS. As detailed in a seminal paper by Huang et al, there are 2
patterns for the paradigm: - continuous theta burst stimulation (cTBS) and intermittent theta
burst stimulation (iTBS). The former produces suppression of MEP and the latter produces
increase in MEP. iTBS delivers 50 Hz stimuli in packets of 10 lasting 2 seconds. Each
stimulus burst delivered at 50 Hz is given every 200 milliseconds making the overall
frequency of stimulus delivery 5 Hz. Hence the stimulation encompasses nested 50 Hz bursts
(gamma frequency) given at 5 Hz (theta frequency). Most investigational studies which did not
have treatment outcome measures have used either 40 second of cTBS or 190 seconds of iTBS.
Both these paradigms have been shown to cause changes in MEP for 60 minutes. Variations in
pattern of stimulation have also been effective, although there are limited studies to
warrant its use. The investigators therefore propose to use stimulate the function of the
hippocampal formation in healthy older adults (hOA) by targeting a cortical region directly
connected to the hippocampal formation: the angular gyrus. To increase indirect effects on
hippocampal formation, the investigators will use the most powerful TMS technique available,
intermittent Theta Burst Stimulation (iTBS).
METHODOLOGY The study is designed to be a pilot one evaluating the effect of TBS on EM in
healthy older adults (hOA). The investigators plan to screen 30 participants to select 20
subjects.
Screening Potential participants will be in the age group of 60-80 years and encompasses
subjects who have been recruited to previous studies at Cabeza Lab (Pro00005021), hence
having brain imaging data already collected.
Study procedure On day 1 of the study, subjects will have the National Institute of Health
(NIH) Toolbox administered to them. The NIH toolbox is a comprehensive set of
neuro-behavioral measurements that quickly assesses cognitive functions from the convenience
of an iPad. Total time allotted for NIH toolbox administration is 45 minutes. Following this,
subjects will have motor evoked potential (MEP) performed after which they will be
administered intermittent theta burst stimulation (iTBS) to motor cortex. This will be
followed by measurement of motor evoked potential (MEP) again. Subjects who do not show a 10
% increase in motor evoked potential (MEP) with iTBS will be excluded from further parts of
the study.
Our study uses a specific kind of TMS, known as intermittent theta burst stimulation (iTBS).
On day 1 of the study, subjects will be administered either left-sided iTBS to the motor
cortex. The subject will be seated in a chair. Electromyogram (EMG) electrodes will be
applied to the right hand for motor evoked potential (MEP) recording. For iTBS the active
motor threshold would be 80 % as used in most theta burst studies detailed in this review.
Subjects would receive iTBS comprising 50 Hz bursts given at 3 to 5 Hz for close to 3 minutes
which comprises 19 trains and 600 pulses. The subject will be monitored until MEPs return to
baseline. A side effects checklist will be completed at the beginning and at the end of the
experimental session. All sessions will be performed by one of the protocol investigators, or
by a trained and accredited research assistant supervised by the protocol investigators.
If a 10 % increase is seen in the MEP, then subjects will receive a second session of iTBS or
sham stimulation to the left angular gyrus one hour after the screening session. If they
receive iTBS, this will comprise 6 minutes of stimulation equivalent to 1200 pulses and 38
trains of the stimulus. The subject will be monitored until MEPs return to baseline. A side
effects checklist will be completed at the beginning and at the end of the experimental
session. Sham stimulation will use superficial electrodes to mimic the experience of
receiving actual stimulation. All sessions will be performed by one of the protocol
investigators, or by a trained and accredited research assistant supervised by the protocol
investigators. Subjects will perform encoding trials of episodic memory task with stimulation
and retrieval piece of the task after the stimulation.
stimulation (TBS) which is a relatively new paradigm of transcranial magnetic stimulation
(TMS) on episodic memory (EM) in healthy older adults (hOA).
Aim1: Evaluate the effect of theta burst stimulation (TBS) on episodic memory (EM) in healthy
older adults. Hypothesis 1 - There will be significant improvement in EM compared to baseline
with one session of TBS.
Aim 2: Correlate white matter integrity to improvement in task retrieval with TBS. Hypothesis
2- Stronger white matter (WM) tract connections correlate to greater improvement in retrieval
performance.
BACKGROUND Alzheimer's disease (AD) affects 5 million Americans, at a cost of over 200
billion dollars. The first and most debilitating symptom of AD is a severe deficit in the
ability to remembering personal past events, or episodic memory (EM), which eventually
renders patients isolated from family and friends and unable to live independently. This EM
deficit reflects primarily the deterioration of medial temporal lobe regions, particularly
the hippocampus (HC). AD treatments must start very early in the disease progression, when
brain damage is still small, and the earliest stage when AD can be diagnosed is known as mild
cognitive impairment due to AD (MCI-AD).
Recently, different forms of noninvasive brain stimulation techniques have been applied to
healthy older adults, AD and MCI-AD to improve memory impairment. Most of these trials used
high-frequency repetitive transcranial magnetic stimulation (rTMS) applied to the left
dorsolateral prefrontal cortex (DLPFC). Although a small number of these studies have shown
beneficial effects, considerable questions remain as to whether TMS has clinically relevant
effects in elderly populations, as well as to what neuroscience-based mechanisms account for
these effects. An obstacle for using TMS to enhance EM is that the brain region most critical
for EM and most affected by early AD, the hippocampus (HC), is situated deep inside the
brain, beyond TMS direct effects (~1" below the skull). One study attempted to target
hippocampus and peri-hippocampal regions for stimulation via TMS. They stimulated the lateral
parietal cortex and utilized functional connectivity between this region and
hippocampus/peri-hippocampal regions (mainly entorhinal cortex) to enhance performance on an
associative memory task. The inferior longitudinal fasciculus connects angular gyrus to
hippocampus and para-hippocampal regions, and could propagate stimulation effects from
cortical to subcortical structures, although studies on effect on TMS on white matter
neuronal populations are limited as detailed below. The effect of TMS on neuronal populations
in the white matter tracts was recently modeled using tractography and e-field calculations,
and increasingly, these approaches need to account for what percentage of variance in motor
threshold (MT) would be accounted for by white matter tracts.
TBS is a potent paradigm of TMS. As detailed in a seminal paper by Huang et al, there are 2
patterns for the paradigm: - continuous theta burst stimulation (cTBS) and intermittent theta
burst stimulation (iTBS). The former produces suppression of MEP and the latter produces
increase in MEP. iTBS delivers 50 Hz stimuli in packets of 10 lasting 2 seconds. Each
stimulus burst delivered at 50 Hz is given every 200 milliseconds making the overall
frequency of stimulus delivery 5 Hz. Hence the stimulation encompasses nested 50 Hz bursts
(gamma frequency) given at 5 Hz (theta frequency). Most investigational studies which did not
have treatment outcome measures have used either 40 second of cTBS or 190 seconds of iTBS.
Both these paradigms have been shown to cause changes in MEP for 60 minutes. Variations in
pattern of stimulation have also been effective, although there are limited studies to
warrant its use. The investigators therefore propose to use stimulate the function of the
hippocampal formation in healthy older adults (hOA) by targeting a cortical region directly
connected to the hippocampal formation: the angular gyrus. To increase indirect effects on
hippocampal formation, the investigators will use the most powerful TMS technique available,
intermittent Theta Burst Stimulation (iTBS).
METHODOLOGY The study is designed to be a pilot one evaluating the effect of TBS on EM in
healthy older adults (hOA). The investigators plan to screen 30 participants to select 20
subjects.
Screening Potential participants will be in the age group of 60-80 years and encompasses
subjects who have been recruited to previous studies at Cabeza Lab (Pro00005021), hence
having brain imaging data already collected.
Study procedure On day 1 of the study, subjects will have the National Institute of Health
(NIH) Toolbox administered to them. The NIH toolbox is a comprehensive set of
neuro-behavioral measurements that quickly assesses cognitive functions from the convenience
of an iPad. Total time allotted for NIH toolbox administration is 45 minutes. Following this,
subjects will have motor evoked potential (MEP) performed after which they will be
administered intermittent theta burst stimulation (iTBS) to motor cortex. This will be
followed by measurement of motor evoked potential (MEP) again. Subjects who do not show a 10
% increase in motor evoked potential (MEP) with iTBS will be excluded from further parts of
the study.
Our study uses a specific kind of TMS, known as intermittent theta burst stimulation (iTBS).
On day 1 of the study, subjects will be administered either left-sided iTBS to the motor
cortex. The subject will be seated in a chair. Electromyogram (EMG) electrodes will be
applied to the right hand for motor evoked potential (MEP) recording. For iTBS the active
motor threshold would be 80 % as used in most theta burst studies detailed in this review.
Subjects would receive iTBS comprising 50 Hz bursts given at 3 to 5 Hz for close to 3 minutes
which comprises 19 trains and 600 pulses. The subject will be monitored until MEPs return to
baseline. A side effects checklist will be completed at the beginning and at the end of the
experimental session. All sessions will be performed by one of the protocol investigators, or
by a trained and accredited research assistant supervised by the protocol investigators.
If a 10 % increase is seen in the MEP, then subjects will receive a second session of iTBS or
sham stimulation to the left angular gyrus one hour after the screening session. If they
receive iTBS, this will comprise 6 minutes of stimulation equivalent to 1200 pulses and 38
trains of the stimulus. The subject will be monitored until MEPs return to baseline. A side
effects checklist will be completed at the beginning and at the end of the experimental
session. Sham stimulation will use superficial electrodes to mimic the experience of
receiving actual stimulation. All sessions will be performed by one of the protocol
investigators, or by a trained and accredited research assistant supervised by the protocol
investigators. Subjects will perform encoding trials of episodic memory task with stimulation
and retrieval piece of the task after the stimulation.
Inclusion Criteria:
- Healthy controls in the age group 60-80 years old
- No other Diagnostic and Statistical Manual of Mental Disorders (DSM) 5 axis 1
diagnoses
- Willing to provide informed consent
- Structural magnetic resonance imaging (MRI) and diffusion tensor imaging (DTI) data
available
Exclusion Criteria:
- Subjects are unable or unwilling to give informed consent
- Presence of any organic brain illness
- Presence or history of stroke, traumatic brain injury or head injury with loss of
consciousness, transient ischemic attack (TIA), any diagnosed neurological disorder
including but not limited to multiple sclerosis, Huntington's disease, Parkinson's
disease, dementia or major neurocognitive disorder.
- Presence of cranial metal implants, structural brain lesion including but not limited
to cerebral aneurysms.
- Presence of devices that may be affected by repetitive transcranial magnetic
stimulation (rTMS) (pacemaker, medication pump, cochlear implant, implanted brain
stimulator)
- Current or recent (within the past 6 months) substance abuse or dependence, excluding
nicotine and caffeine.
- Current serious medical illness
- History of seizure except those therapeutically induced by electroconvulsive therapy
(ECT) (childhood febrile seizures are acceptable and these subjects may be included in
the study), history of epilepsy in self or first degree relatives
- For subjects age > 59 years, a total scaled score < 8 on the Dementia Rating Scale-2.
We found this trial at
1
site
2301 Erwin Rd
Durham, North Carolina 27710
Durham, North Carolina 27710
919-684-8111
Principal Investigator: Roberto Cabeza, PhD
Phone: 919-970-7847
Duke Univ Med Ctr As a world-class academic and health care system, Duke Medicine strives...
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