Nicotine Dependence Clinical Trial
Official title:
State and Trait Mediated Response to TMS in Substance Use Disorder
OBJECTIVES: The current protocol seeks to develop brain-based intermediate phenotypes of
response to transcranial magnetic stimulation (TMS) in chronic substance use disorder (SUD).
To date the field has relied on subjective reports, behavioral performance, and long-term
clinical outcomes as primary measures of TMS efficacy. While certainly ecologically valid,
these observable behaviors lack the sensitivity necessary to fully quantify the effects (or
lack thereof) across both individual participants and TMS intervention protocols.
This proposed within-subjects design seeks to leverage differences in metaplasticity that is,
the context in which stimulation occurs-by studying the response to stimulation in both sated
and abstinent states. It is predicted these state manipulations will potentiate response to
TMS. When a disruptive allostatic load like chronic nicotine exposure or acute abstinence is
placed on the brain, the underlying network becomes less stable and thus more susceptible to
TMS intervention. For SUD in general and tobacco use disorder (TUD) in particular, this state
dependence of TMS response is a potentially valuable tool to improve a given intervention s
clinical efficacy.
STUDY POPULATION: Physically and psychiatrically healthy smokers will be recruited. A
comparison group of non-smokers will be concurrently enrolled. We estimate we will require
n=51/group of completers to have sufficient power to develop the intermediate phenotypes of
TMS.
DESIGN: The protocol is a two group, between/within subject, fully counterbalanced design.
The between-subjects factor is GROUP (smoker/non-smoker) and the within-subjects factor for
each GROUP is TMS CONDITION (active/sham). Additionally, and for the smoker group, nicotine
STATE (sated/abstinent) is a nested within-subjects factor. Each group will receive single
sessions of active and sham intermittent theta burst stimulation to left dorsal lateral
prefrontal cortex, followed immediately by an MRI scan to characterize the acute
neurobiological response to stimulation. Smokers will repeat these procedures both during
smoking satiety and following an ~48-hour period nicotine abstinence.
OUTCOMES PARAMETERS: In addition to subjective and behavioral task performance changes
associated with TMS intervention, changes in MRI BOLD signal will be used to characterize the
neurobiological response to TMS intervention across groups and states. Taken together, the
development of brain-based markers of TMS response may thus improve both our mechanistic
understanding of the causal dysfunctions of TUD as well as the potential efficacy of these
interventions longer term to address the relevant clinical characteristics of the disease and
ultimately improve treatment outcomes.
OBJECTIVES: The current protocol seeks to develop brain-based intermediate phenotypes of
response to transcranial magnetic stimulation (TMS) in chronic substance use disorder (SUD).
To date the field has relied on subjective reports, behavioral performance, and long-term
clinical outcomes as primary measures of TMS efficacy. While certainly ecologically valid,
these observable behaviors lack the sensitivity necessary to fully quantify the effects (or
lack thereof) across both individual participants and TMS intervention protocols.
This proposed within-subjects design seeks to leverage differences in metaplasticity that is,
the context in which stimulation occurs-by studying the response to stimulation in both sated
and abstinent states. It is predicted these state manipulations will potentiate response to
TMS. When a disruptive allostatic load like chronic nicotine exposure or acute abstinence is
placed on the brain, the underlying network becomes less stable and thus more susceptible to
TMS intervention. For SUD in general and tobacco use disorder (TUD) in particular, this state
dependence of TMS response is a potentially valuable tool to improve a given intervention s
clinical efficacy.
STUDY POPULATION: Physically and psychiatrically healthy smokers will be recruited. A
comparison group of non-smokers will be concurrently enrolled. We estimate we will require
n=51/group of completers to have sufficient power to develop the intermediate phenotypes of
TMS.
DESIGN: The protocol is a two group, between/within subject, fully counterbalanced design.
The between-subjects factor is GROUP (smoker/non-smoker) and the within-subjects factor for
each GROUP is TMS CONDITION (active/sham). Additionally, and for the smoker group, nicotine
STATE (sated/abstinent) is a nested within-subjects factor. Each group will receive single
sessions of active and sham intermittent theta burst stimulation to left dorsal lateral
prefrontal cortex, followed immediately by an MRI scan to characterize the acute
neurobiological response to stimulation. Smokers will repeat these procedures both during
smoking satiety and following an ~48-hour period nicotine abstinence.
OUTCOMES PARAMETERS: In addition to subjective and behavioral task performance changes
associated with TMS intervention, changes in MRI BOLD signal will be used to characterize the
neurobiological response to TMS intervention across groups and states. Taken together, the
development of brain-based markers of TMS response may thus improve both our mechanistic
understanding of the causal dysfunctions of TUD as well as the potential efficacy of these
interventions longer term to address the relevant clinical characteristics of the disease and
ultimately improve treatment outcomes.
;
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Recruiting |
NCT05176418 -
IV Pulsed-Nicotine as a Model of Smoking: The Effects of Dose and Delivery Rate
|
Early Phase 1 | |
| Completed |
NCT04084210 -
Impact of Alternative Nicotine-Delivery Products on Combustible Cigarette Use
|
Phase 2 | |
| Completed |
NCT04043728 -
Addressing Psychological Risk Factors Underlying Smoking Persistence in COPD Patients: The Fresh Start Study
|
N/A | |
| Recruiting |
NCT03999099 -
Targeting Orexin to Treat Nicotine Dependence
|
Phase 1 | |
| Completed |
NCT03847155 -
Prevention of Nicotine Abstinence in Critically Ill Patients After Major Surgery
|
N/A | |
| Completed |
NCT02840435 -
Study on Sit to Quit Phone Intervention
|
N/A | |
| Completed |
NCT02139930 -
Project 2: Strategies for Reducing Nicotine Content in Cigarettes
|
N/A | |
| Completed |
NCT01982110 -
A Mindfulness Based Application for Smoking Cessation
|
N/A | |
| Completed |
NCT01926626 -
Evaluation of Moclobemide, a Reversible MAO-A Inhibitor, as an Adjunct to Nicotine Replacement Therapy in Female Smokers
|
Phase 2 | |
| Completed |
NCT01569490 -
Striving to Quit: First Breath
|
N/A | |
| Completed |
NCT01685996 -
Zonisamide Augmentation of Varenicline Treatment for Smoking Cessation
|
Phase 1/Phase 2 | |
| Withdrawn |
NCT01569477 -
Striving to Quit-Wisconsin Tobacco Quit Line
|
N/A | |
| Completed |
NCT01632189 -
The Effect of Varenicline on D2/D3 Receptor Binding in Smokers
|
N/A | |
| Active, not recruiting |
NCT01182766 -
New Treatment for Alcohol and Nicotine Dependence
|
Phase 2/Phase 3 | |
| Completed |
NCT01061528 -
Coping Skills Treatment for Smoking Cessation
|
N/A | |
| Completed |
NCT00996034 -
Nicotine Vaccination and Nicotinic Receptor Occupancy
|
Phase 2 | |
| Suspended |
NCT01636336 -
Effects of Progesterone on Smoked Nicotine Induced Changes in Hormones and Subjective Ratings of Stimulant Drug Effects
|
N/A | |
| Withdrawn |
NCT01589081 -
Effects of Progesterone on IV Nicotine-Induced Changes in Hormones and Subjective Ratings of Stimulant Drug Effect
|
N/A | |
| Completed |
NCT01943994 -
Psilocybin-facilitated Smoking Cessation Treatment: A Pilot Study
|
N/A | |
| Withdrawn |
NCT00571805 -
Study of Varencline Effects on Cigarette Smoking Reward and Craving During a Model of Brief Quit Attempt
|
Phase 1/Phase 2 |