Influence of Fampridine on Working Memory in Healthy Subjects
- Registration Number
- NCT04516603
- Lead Sponsor
- Prof. Dominique de Quervain, MD
- Brief Summary
Proof-of-concept study on the effects of 10 mg fampridine (oral administration) on working memory in healthy participants.
The hypotheses is that fampridine improves working memory performance.
- Detailed Description
Not available
Recruitment & Eligibility
- Status
- WITHDRAWN
- Sex
- All
- Target Recruitment
- Not specified
- male or female
- generally healthy
- normotensive (BP between 90/60 mmHg and 140/90 mmHg)
- BMI between 19 and 29,9 kg/m2
- aged between 18 and 30 years
- fluent German-speaking
- Informed consent as documented by signature
- contraindications to the class of drugs under study, e.g. known hypersensitivity or allergy to 4-aminopyridine
- use of potassium channel blockers within the last 3 months
- concomitant treatment with OCT 2 inhibitors (e.g. cimetidine, propranolol)
- acute or chronic psychiatric disorder (e.g. major depression, psychoses, somatoform disorder, suicidal tendency)
- acute cerebrovascular condition
- history of seizures
- risk of lowered seizure threshold (due to e.g. sleep deprivation, withdrawal of alcohol after alcohol abuse)
- renal impairment
- history of malignant cancers
- walking problems (e.g. due to dizziness)
- other clinically significant concomitant disease states (e.g. hepatic dysfunction, cardiovascular disease, diabetes, asthma)
- clinically significant laboratory or ECG abnormality that could be a safety issue in the study
- known or suspected non-compliance
- drug or alcohol abuse
- inability to follow the procedures of the study, e.g. due to language or psychological problems of the participant
- participation in another study with an investigational drug within the 30 days preceding and during the present study
- prior participation (less than two years ago) in a study investigating working memory (notably the n-back task)
- enrolment of the investigator, his/her family members, employees and other dependent persons
- smoking (>3 cigarettes per day)
- intake of psychoactive drugs (e.g. benzodiazepines, antidepressants, neuroleptics)
- pregnancy or breast feeding
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- CROSSOVER
- Arm && Interventions
Group Intervention Description Fampridine SR Fampridine SR Single oral administration of a tablet fampridine (10 mg) formulated for oral administration taken once in the morning without food. Tablets must be administered whole. The single intake is followed by a washout period of at least 7 days equalling over 40 half-lives of the active substance fampridine (t½ = 3.61 h) between experimental and control intervention. Placebo Placebo Identically looking placebo tablets consisting of the identical additives formulated for oral administration.
- Primary Outcome Measures
Name Time Method Medium-load working memory performance test day 1 and 2, each 4 hours after intake of study medication to assess differences between the Verum and Placebo condition Accuracy as assessed by a letter n-back task (Papassotiropoulos, Henke et al. 2011) with the levels 0-back and 2-back.
This test includes a 2-back task assessing working memory and a 0-back task ('x-target' task) measuring concentration. The 2-back task requires participants to respond to a letter repeat with one intervening letter (for example, S-m-s-g...). The 'x-target' task requires participants to respond to the occurrence of the letter 'x' in a sequence of letters (for example, N-l-X-g...). Accuracy (i.e. correct 2-back responses minus correct 0-back responses) will be calculated.
- Secondary Outcome Measures
Name Time Method Bochumer Matrizentest (BOMAT - advanced -short) test day 1 and 2 each 4 hours after intake of study medication to assess differences between the Verum and Placebo condition Bochumer Matrizentest (BOMAT - advanced -short; Hossiep/Turck/Hasella, 2001, 1st edition), matrix reasoning. The BOMAT will be administered to measure fluid intelligence (Gf) consisting of 29 items. A time-limited version will be used according to Jaeggi (Jaeggi 2010). The total score is calculated by summing the correct solutions, ranging between 0 to 29. A parallel version will be used for the second test day.
N-back with a 3-back condition test day 1 and 2 each 4 hours after intake of study medication to assess differences between the Verum and Placebo condition N-back with a 3-back condition, which is more demanding than the 2-back condition. Accuracy (3-back minus 0-back) will be calculated.
Symbol Digit Modalities Test, SDMT test day 1 and 2 each 4 hours after intake of study medication to assess differences between the Verum and Placebo condition Symbol Digit Modalities Test, SDMT (Smith 2013, 13th edition), a processing speed test. The test consists of the presentation of a series of 9 symbols, each of them is paired with a single digit, labeled 1-9, in a key at the top of a sheet. The remainder of the page has a pseudorandomized sequence of the symbols and the participant must respond with the digit associated with each of these as quickly as possible. The score is the number of correct answers in 90 seconds. The administration of SDMT will be preceded by a learning sequence at both timepoints. A parallel version will be used for the second test day.
Digit Span Task test day 1 and 2 each 4 hours after intake of study medication to assess differences between the Verum and Placebo condition Digit span task, a subtest of the "Wechsler Intelligenztest für Erwachsene" (WIE;von Aster 2006). Total scores for digit span forward and backward will be calculated as described in the manual of the WIE. A parallel version will be used for the second test day.
Reaction time test day 1 and 2 each 4 hours after intake of study medication to assess differences between the Verum and Placebo condition Reaction time for correct 2-back responses minus correct 0-back responses.
Trial Locations
- Locations (1)
University of Basel, Transfaculty Research Platform
🇨🇭Basel, BS, Switzerland