Overview
The Impact of Caffeine on Cognition in Schizophrenia
Status:
Unknown status
Unknown status
Trial end date:
2019-06-01
2019-06-01
Target enrollment:
0
0
Participant gender:
All
All
Summary
Caffeine is the most used psychoactive drug in Canada, with regular consumption by 88% of the adult population, While rates of caffeine consumption are considered to be high in the general population, there is some evidence that they may be even higher within schizophrenia patients; in a 2006 U.S. study, daily consumption rates of caffeine were nearly double those observed in a healthy control population (471.6 mg/day vs. 254.2 mg/day). Furthermore, 13% of the schizophrenia population studied ingested more than 1000 mg/day of caffeine, well above the 400 mg daily maximum recommended by Health Canada. High doses of caffeine are particularly concerning for individuals with schizophrenia; caffeine alters dopaminergic activity at post-synaptic neurons through its actions at adenosine A2A receptors, which may exacerbate positive symptoms, such as delusions and hallucination. This significant rate of consumption is likely due in part to caffeine's actions on the human brain, resulting in increased arousal, elevated mood and beneficial effects on a wide-range of cognitive processes including verbal working memory, sustained attention, and executive function. These areas of caffeine-induced cognitive improvement notably overlap with the cognitive domains that are reported to be diminished in schizophrenia. Despite this overlap and the rates of caffeine consumption observed within schizophrenia, research reports examining the effects of caffeine on cognition and brain activity are all but non-existent in this population. The primary objective of this proposal is to compare the effects of caffeine and placebo on brain function during cognitive tasks in participants with schizophrenia. While the investigators have specific hypotheses for each task, overall the investigators hypothesize that caffeine will improve cognitive function (as evidenced by larger ERP amplitudes and/or reduced ERP latencies) compared to placebo in schizophrenia patients, with similar effects (albeit reduced in magnitude) observed in non-patient healthy controls.Phase:
N/AAccepts Healthy Volunteers?
Accepts Healthy VolunteersDetails
Lead Sponsor:
Nova Scotia Health AuthorityCollaborators:
Dalhousie University
Mount Saint Vincent UniversityTreatments:
Caffeine
Criteria
Inclusion Criteria:- Patient participants: Patients will have a primary diagnosis of schizophrenia and will
be judged as clinically stable, as indicated by the patient's primary physician and
including no changes in symptoms or antipsychotic medications for the last 2 months,
and each participant's primary medication (if any) will be limited to one of the
atypical anti-psychotics, excluding clozapine due to the noted interactions.
Participants will be required to understand spoken and written English and will be
right-handed (assessed by the Edinburgh Handedness Inventory [EHI]) to facilitate
source localization techniques. Participants will be required to have normal (or
corrected) vision.
- Healthy controls: Self-report of negative psychiatric, medical, neurological and
alcohol/drug abuse histories, and current non-use of medications (with the exception
of oral contraceptives). Participants will be required to understand spoken and
written English and will be right-handed (assessed by the Edinburgh Handedness
Inventory [EHI]) to facilitate source localization techniques. Participants will be
required to have normal (or corrected) vision.
Exclusion Criteria:
- Patients: Patient participants will be excluded if they meet any of the following
criteria: co-morbid DSM-IV TR Axis I disorder; current treatment with clozapine; total
PANSS score >65, reflecting an acute psychotic episode; current history of drug abuse
or dependence; history of head injury resulting in loss of consciousness; diagnosis of
epilepsy or any other neurologic disorder; electro-convulsive therapy (ECT) treatment
within the previous year; significant cardiac illness; or extrapyramidal symptoms
(EPS) resulting in movement disorders which could affect ERP recordings. Additionally,
as is common in caffeine research, participants will be excluded if they work night
shifts or do not report normal (i.e. nocturnal) sleep patterns during screening
- Healthy Controls: As is common in caffeine research, participants will be excluded if
they work night shifts or do not report normal (i.e. nocturnal) sleep patterns during
screening.