A Study to Evaluate the Efficacy and Safety of Piracetam on Aphasia After Acute Ischemic Cerebral Artery Stroke
- Conditions
- Acute Ischaemic Middle Cerebral Artery Stroke
- Interventions
- Other: Placebo
- Registration Number
- NCT01883011
- Lead Sponsor
- UCB S.A. - Pharma Sector
- Brief Summary
The aim of this study was to confirm the efficacy of piracetam after 12 weeks of treatment on the aphasic status of subjects suffering from aphasia after acute ischemic middle cerebral artery stroke and having received their medication within 7 h post-stroke onset.
- Detailed Description
An interim analysis was performed, as planned in the protocol, on the primary efficacy measure (Day 84 FAST Score) for aphasic subjects. This interim analysis indicated that there was less than a 20 % chance of showing a 15 % difference between placebo and piracetam at the end of the trial, under the assumption that there was indeed a 15 % difference. Thus, it was the decision of UCB to stop further recruitment into this study.
Recruitment & Eligibility
- Status
- TERMINATED
- Sex
- All
- Target Recruitment
- 571
- Male or female adults โฅ 50 years
- Considered as reliable and mentally capable of adhering to the protocol
- Signed informed consent (by the subject or the next of kin) or inclusion of the subject as per Ethics Committee approved procedures
- Clinical diagnosis of a middle cerebral artery ischemic stroke
- A disabling motor deficit at the moment of inclusion, defined as having a total Middle Cerebral Artery (MCA) score between 15 and 65
- Treated before 7 h (6 h and 59 minutes) after the estimated stroke onset
- If the subject had a stroke during the night, the onset of stroke is assumed to be the last time the subject was seen awake and normal, or last time the subject remembered he/she was awake and normal
- Being aphasic, defined as having an Aphasia Severity Rating (ASR) score of < 3
- Stupor or coma: < 10 on the item consciousness of the Middle Cerebral Artery (MCA) scale
- A previous stroke with clinical sequel or a previous stroke with aphasia (even in case of complete recovery from aphasia)
- A medical or neurological disease interfering with the assessments and causing a clear deficit:
-
- in functional ability or autonomy
-
- in motor function
-
- in cognitive capacities
-
- in language
- A systemic disease with neurological symptoms
- A life threatening disease with life expectancy of less than 1 year
- Renal insufficiency (creatinine > 2 mg/100 ml or > 180 ยตmol/l; creatinine had to be determined as soon as possible but not before inclusion)
- Any concomitant treatments that could not be stopped at the moment of inclusion or that had been started after the onset of the stroke and before inclusion (as long as not considered by the advisory board as effective drug), such as:
-
- Cerebro-vascular active products: bufenine, buflomedil, cinnarizine, codergocrinemesilate, citicholine, cyclandelate, cyprodemanol, deanolacetamidobenzoate, flunarizine, ginkgo-biloba extr., inositolnicotinate, isoxsuprine, meclofenoxate, naftidrofuryloxalate, nicergoline, nicotinic acid (smoking is allowed), nimodipine, pentifylline, papaverine, pentoxifylline, piracetam, pyrisuccideanoldimaleate, pyritinol, raubasine, vincamine, viquidil, xantinolnicotinate. A list of these drugs with generic and brand name, adapted to each of the participating countries accompanied the Case Report Form (CRF)
-
- Thrombolytics: recombinant tissue-type plasminogen activator (alteplase) (rt- PA), streptokinase, urokinase, ancrod
-
- Hemodilution
-
- Glucose infusion >5 %
- Subjects known to not being able to be followed for 12 weeks
- Known alcohol or drug addiction or abuse
- Subjects previously enrolled in this trial
- Known allergy/intolerance to piracetam/excipients
- Lactation, pregnancy, or pregnancy potential, unless using an effective means of contraception
- Illiterate subjects (subjects not able to read prior to stroke)
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- PARALLEL
- Arm && Interventions
Group Intervention Description Placebo Placebo IV infusion 12 g placebo in 60 ml IV Ampoules 3 g placebo in 15 ml Oral solution 33% placebo (bottle of 125 ml) Oral tablets 1200 mg placebo (blisters of 10 tablets) All IV forms were identical in presentation, size and color to allow a double blind design. All oral forms were identical in shape, size, color and taste to allow a double blind design. Piracetam Piracetam IV infusion 12 g piracetam in 60 ml IV Ampoules 3 g piracetam in 15 ml Oral solution 33 % piracetam (bottle of 125 ml) Oral tablets 1200 mg piracetam (blisters of 10 tablets)
- Primary Outcome Measures
Name Time Method The percentage of subjects recovering from aphasia as per the Frenchay Aphasia Screening Test (FAST) score at Day 84 Day 84 FAST describes the presence, absence or severity of aphasia, but does not differentiate types of aphasia.
Comprehension, expression and reading were main score targets tested by picture card with attached reading card. The FAST score covered a range from 0-20. Subjects with FAST score โค13 where considered as aphasic and subjects with FAST score \> 13 were considered as non-aphasic.
There were 2 tests of comprehension and 2 tests of expression and 1 of reading, however the reading test was not included in the primary efficacy variable.
- Secondary Outcome Measures
Name Time Method Middle Cerebral Artery infarction scale (MCA) score at Day 84 Day 84 The MCA was developed for clinical trial evaluation of middle cerebral artery stroke. The scale evaluates 10 items: consciousness, verbal communication, elevation of the arm, finger and thumb movements, arm tone, deviation of head and eyes, facial movements, elevation of the leg, dorsiflexion of the foot and leg tone. Weighted scores for each item provide a maximum score of 100.
Total Barthel Index (BI) score at Day 84 Day 84 This scale evaluates 10 items: eating, moving from (wheel) chair to bed and back, personal hygiene, using the lavatory, bathing, walking/wheelchair, stairs, getting dressed/undressed, controlling bowel motion, controlling bladder.
Weighted scores for each item vary between 0 and 15 to provide a maximum score of 100. Subjects who can perform all specified activities without help receive a score of 100. Even though they are independent in daily activities, they could remain handicapped by neurologic impairments.Mini Mental State Examination (MMSE) score at Day 84 Day 84 The MMSE is divided into two sections, the first of which requires vocal responses only and covers orientation, memory and attention: the maximum score is 21.
The second part tests ability to name, follow verbal and written commands, write a sentence spontaneously and copy a complex polygon: the maximum score is 9. Maximum score of the two parts is 30. The test is not timed. A score โค 23 indicates that the subject is demented.
Trial Locations
- Locations (44)
103
๐ง๐ชAntwerpen, Belgium
252
๐ฌ๐ทAthens, Greece
003
๐ฆ๐นLinz, Austria
750
๐ณ๐ดBergen, Norway
455
๐ต๐ฑBialystok, Poland
452
๐ต๐ฑWarszawa, Poland
303
๐ฌ๐ทBudapest, Greece
305
๐ฌ๐ทBudapest, Greece
250
๐ฌ๐ทThessaloniki, Greece
450
๐ต๐ฑWarsaw, Poland
304
๐ญ๐บDebrecen, Hungary
454
๐ต๐ฑKrakow, Poland
451
๐ต๐ฑPoznan, Poland
601
๐ธ๐ฌSingapore, Singapore
300
๐ญ๐บBudapest, Hungary
004
๐ฆ๐นInssbruck, Austria
152
๐ซ๐ทNice cedex 1, France
201
๐ฉ๐ชMagdeburg, Germany
001
๐ฆ๐นLinz, Austria
102
๐ง๐ชAntwerpen, Belgium
200
๐ฉ๐ชMinden, Germany
302
๐ฌ๐ทBudapest, Greece
550
๐ธ๐ชStockholm, Sweden
203
๐ฉ๐ชNidda-bad-Salzhausen, Germany
500
๐ช๐ธTerrassa, Spain
104
๐ง๐ชBrussels, Belgium
150
๐ซ๐ทCharleville-Mezieres, France
202
๐ฉ๐ชSaarbrucken, Germany
502
๐ช๐ธMadrid, Spain
350
๐ฎ๐นPerugia, Italy
456
๐ต๐ฑLodz, Poland
654
๐น๐ทEdirne, Turkey
600
๐ธ๐ฌSingapore, Singapore
653
๐น๐ทIstanbul, Turkey
501
๐ช๐ธMadrid, Spain
503
๐ช๐ธMalaga, Spain
700
๐จ๐ณTaipei, Taiwan
050
๐ฆ๐ทBuenos Aires, Argentina
051
๐ฆ๐ทBuenos Aires, Argentina
107
๐ง๐ชGenk, Belgium
251
๐ฌ๐ทAthens, Greece
301
๐ญ๐บMiskolc, Hungary
652
๐น๐ทIstanbul, Turkey
650
๐น๐ทEskisehir, Turkey