Hematoma, Subdural, Chronic Clinical Trial
Official title:
Role of Dexamethasone in the Conservative Treatment of Chronic Subdural Hematoma: a Double-blind Randomized Controlled Pilot Study
Current opinion regarding the use of steroids in the treatment of chronic subdural hematomas
are mostly based on observational studies. Here we present data from a prospective
randomized pilot study of twenty chronic subdural hematoma (CSDH) patients treated with
dexamethasone or placebo for 30 days.
Twenty patients with computed tomography (CT)- or magnetic resonance imaging (MRI)-confirmed
CSDH were recruited from a single center and randomized in order to receive dexamethasone or
placebo as a conservative treatment. Patients affected to the treatment group received oral
dexamethasone 12mg/day for three weeks followed by tapering. These patients were followed
for 6 months and the rate of success of conservative treatment versus placebo was measured.
Parameters such as hematoma thickness and global impression of change were also compared
before and after treatment with chi-square tests. Adverse events and complications were
documented.
Patients Recruitment for this single-center double-blind randomized placebo-controlled study
was performed between January 2007 and May 2009. Patients were enrolled based on the
following inclusion criteria: 18 years and older with evidence of subacute or chronic
supratentorial subdural hematoma by CT (computerized tomography) scan or MRI (magnetic
resonance imaging) and classified between 0 and 2 using the Markwalder grading scale (17)
(Grade 0 for normal neurological status, grade 1 for no neurological deficits but mild
symptoms, grade 2 for focal or variable neurological deficits, grade 3 for several focal
neurological signs, and grade 4 for comatose). Exclusion criteria included contraindications
or intolerance to corticosteroid therapy or patients already undergoing steroid treatment
for any other indication, previous neurological surgery up to one year prior to being
considered for the study, concomitant cerebral pathology of neoplastic or presumed
infectious origin, anticoagulant therapy that could not be stopped for 6 months and refusal
to participate in the study. If at any time, patients developed a sudden increase in
hematoma volume, a midline displacement of greater than 1cm or a deterioration of their
level of consciousness, they were removed from the conservative study protocol in order to
undergo surgery.
This study was approved by the research ethics board at Centre Hospitalier Universitaire
(CHU) de Quebec. Written and fully informed consent was obtained from each participant.
Randomization Allocation to each group was done in a 1:1 ratio with block sizes ranging from
4 to 6, to one of the two arms ; a treatment arm in which participants received
dexamethasone according to the protocol, and a control group in which they received placebo.
Randomization was performed via a web-based service by a pharmacist, which was not involved
in any other part of the study. Both investigators and participants were blind to treatment
allocation.
Treatment Participants allocated to the treatment group received a daily dosage of 12mg (4mg
three times a day) of dexamethasone for three weeks. Corticosteroid treatment was then
tapered off over the next week (8mg for 48 hrs, 4mg for 48 hrs, 2mg for 48 hrs and 1mg for
24 hrs). Identical oral capsules filled with lactose were administered to the control
(placebo) group for 28 days. Participants were returned at home with blister packs
containing their medication for each day of the trial and were asked to return empty packs
to ensure compliance with the assigned treatment. The treatment (placebo or dexamethasone)
was discontinued if a patient required surgical drainage of its hematoma or suffered from
significant side effects.
Evaluation and follow-up The primary outcome of this pilot study was to determine the
efficacy of dexamethasone as compared with placebo in reducing the rate of surgical
intervention for CSDH graded 0 to 2 on the Markwalder grading scale (Grade 0 for normal
neurological status, grade 1 for no neurological deficits but mild symptoms, grade 2 for
focal or variable neurological deficits, grade 3 for several focal neurological signs, and
grade 4 for comatose).
Eligible patients who consented for the study underwent the routine standard of care. This
included 1) a complete medical history review and neurological physical exam ; 2) head
computerized tomography (CT) or MRI with measurement of maximal hematoma thickness (in mm),
midline shift ; 3) and a check of blood and vital parameters. In addition, patients were
asked to complete detailed questionnaires measuring symptoms typically associated with
subdural hematomas.
Follow-up appointments were scheduled 2 weeks, 1, 2 and 6 months after initiation of
treatment. At each visit, the three components of the clinical evaluation described above
were repeated. Moreover, a seven point categorical scale was used to evaluate patient's
global impression of change relative to the initial state (unchanged , very much improved,
much improved, minimally improved, minimally worse, much worse, very much worse).
Treatment-related side effects were also inquired about and collected.
The rate of success of conservative management was defined as the percentage of patients not
requiring surgery in each treatment group during the 6 months following enrollment.
Radiological progression of the hematoma in terms of thickness and magnitude of midline
shift, hematoma-related symptoms and medication-related side effects were carefully
collected.
Statistical analyses Demographical characteristics, baseline neurological status and
hematoma size and location were compared for both groups using a Mann-Whitney test for
continuous variable and a χ2 test for categorical variables.
To compare the rate of success, a categorical frequency comparison with the Fisher's exact
test was used. For the other outcome measures we used Mann-Whitney U test and Student's
t-test for normally distributed variables and χ2 or Fisher's exact test for categorical
frequencies. All statistical tests were done with the Statistical package for Social
Sciences software version 16.0 and the significance threshold was set at p<0.05.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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