Stroke Hemorrhagic Clinical Trial
Official title:
Randomized, Double-blind, Placebo-controlled Trial to Investigate the Effectiveness of Early Intravenous Tranexamic Acid in Limiting Hematoma Expansion in Patients With Spontaneous Intracerebral Hemorrhage
This study aims to explore the effectiveness of tranexamic acid (also known as trans amine or
TXA) in reducing hematoma expansion in patients with hemorrhagic stroke when given in the
acute phase.
METHODOLOGY
This will be a Phase III, parallel-group double-blind randomised placebo control trial.
Patients allocated to the control group will receive standard care for hemorrhagic stroke
according to the 2015 American Heart Association guidelines. Patients allocated to the
intervention group will receive, in addition to standard care, a loading dose of intravenous
TXA 1gm within 3 hours of symptom onset followed by a 1gm maintenance dose over 8 hours.
Timing and dosing are in accordance to previous established study protocols. Patients in the
intervention group will only receive a single treatment course of TXA.
Study subjects will be identified by either the on-duty clinicians from the Department of
Neurosurgery of this institution or by the study investigators. Should the patient meet study
eligibility criteria consent will be obtained either from the patient or from his/her next of
kin. 1:1 block randomization will be performed by a remote internet randomization service by
accessing a website. Patients allocated to the intervention arm will have 1gm of TXA added to
100ml of normal saline (0.9%) infused over 10 minutes as a loading dose. This is then
followed by a maintenance dose of 1gm of TXA in 500ml of intravenous isotonic solution
infused at 120mg/hour (60ml/hour) for 8 hours. Patient's allocated to the control arm will
have an equal volume of normal saline (0.9%) infused as a placebo. The patient and the
outcome assessor will be blinded to study group allocation.
The primary endpoint of this study will be to assess the percentage change in brain blood
clot volume by computed tomography brain scans on admission, 6 hours later, at 24 hours and
at 1 week.
INTRODUCTION
There are very few treatment options for patients with spontaneous intracerebral hemorrhage,
a type of hemorrhagic stroke especially prevalent among Chinese, during the acute phase.
Blood clot expansion in the brain (hematoma expansion; HE) is one of the most significant
predictors for poor outcome in such patients.
Tranexamic acid (TXA) is a commonly used medication available in all acute Hospital Authority
hospitals prescribed for a variety of conditions when bleeding occurs, for example epistaxis
and menorrhagia. Intravenous administration of TXA has been proven to benefit severe trauma
patients by reducing mortality and also preventing the recurrent rupture of brain aneurysms
in another type of hemorrhagic stroke. The medication is safe and has been proven to improve
outcomes in these patients.
A previously performed pilot study exploring the safety and feasibility of administrating
intravenous TXA to patients with hemorrhagic stroke was recently performed and concluded the
medication's safety. There was also a trend to significance for reducing the percentage
change of hematoma volume in patients who received TXA.
This study aims to explore the effectiveness of TXA in reducing hematoma expansion in
patients with hemorrhagic stroke when given in the acute phase.
METHODOLOGY
This will be a Phase III, parallel-group double-blind randomised placebo control trial.
Patients allocated to the control group will receive standard care for hemorrhagic stroke
according to the 2015 American Heart Association guidelines. Patients allocated to the
intervention group will receive, in addition to standard care, a loading dose of intravenous
TXA 1gm within 3 hours of symptom onset followed by a 1gm maintenance dose over 8 hours.
Timing and dosing are in accordance to previous established study protocols. Patients in the
intervention group will only receive a single treatment course of TXA.
Study subjects will be identified by either the on-duty clinicians from the Department of
Neurosurgery of this institution or by the study investigators. Should the patient meet study
eligibility criteria consent will be obtained either from the patient or from his/her next of
kin. 1:1 block randomization will be performed by a remote internet randomization service by
accessing a website. Patients allocated to the intervention arm will have 1gm of TXA added to
100ml of normal saline (0.9%) infused over 10 minutes as a loading dose. This is then
followed by a maintenance dose of 1gm of TXA in 500ml of intravenous isotonic solution
infused at 120mh/hour (60ml/hour) for 8 hours. Patient's allocated to the control arm will
have an equal volume of isotonic solution infused as a placebo. The patient and the outcome
assessor will be blinded to study group allocation.
The primary endpoint of this study will be to assess the percentage change in brain blood
clot volume by computed tomography brain scans on admission, 6 hours later, at 24 hours and
at 1 week. Volumetric analysis of the brain scans will be performed by two radiologists
blinded to the patient's study group allocation..
Secondary endpoints will be assessed by a research assistant blinded to the patient's study
group allocation. One such endpoint is functional outcome in terms of the Glasgow Outcome
Scale and modified Rankin scale at 3 months and 6 months after stroke. Another secondary
endpoint is quality of life at 3 months and 6 months by adopting the Stroke-specific Quality
of Life Scale. Other secondary endpoints include death within 30 days of admission, vascular
occlusive events (myocardial infarction, pulmonary embolism, deep vein thrombosis), ischemic
stroke, seizures and other TXA-associated adverse effects.
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