Subarachnoid Hemorrhage, Aneurysmal Clinical Trial
Official title:
Multimodality Monitoring Directed Management of Aneurysmal Subarachnoid Haemorrhage
Aneurysmal subarachnoid haemorrhage (aSAH) affects up to 10,000 individuals per year in the
UK. It accounts for ~5% of strokes, but is responsible for about 25% quality-adjusted life
years (QALYs) lost due to stroke. Although early repair of ruptured aneurysms and aggressive
postoperative management has improved overall outcomes, it remains a devastating disease
with mortality approaching 50%. Survivors are left with neurological injuries that range
from subtle cognitive deficit to disabling cerebral infarctions, less than 60% them
returning to functional independence.
SAH triggers a series of pathological processes resulting in neuronal damage and consequent
neurological deficit termed early brain injury (EBI). Many of the patients who survive the
initial bleed, deteriorate days later from delayed ischaemic neurological deficit (DIND),
which causes poor outcome or death in up to 30% of patients with SAH. Both of these
pathological processes are still poorly understood which limits the number of treatment
options.
DIND is treated with blood pressure augmentation to ensure adequate blood flow in the brain.
In awake patients, response can be easily and accurately assessed by performing a thorough
neurological examination. In patients whose clinical condition demands sedation, intubation
and ventilation, assessing response to treatment using the neurological examination is
virtually impossible. Multimodality monitoring (MM), primarily microdialysis and brain
tissue oxygen tension with catheters inserted into the relevant parts of the brain offer
direct assessment of both delivery and utilisation of metabolic substrates at the cellular
level. These can be used for early detection of DIND as well as monitoring during blood
pressure augmentation. The aim of this study is to establish and validate a clinical
protocol for MM derived management of SAH patients, to determine optimal therapies for
correcting abnormalities in brain metabolism and explore the relationship between MD and
other monitoring modalities.
This is a prospective observational study of patients with poor grade subarachnoid
haemorrhage (SAH) caused by a ruptured brain artery aneurysm. The investigators aim to
include 100 patients over a 5-year period.
SAH is diagnosed using computer tomography imaging of the brain and the presence of a
ruptured aneurysm by means of computer tomography angiogram of the vessels of the head.
These two investigations are part of the standard clinical practice for every patient with
suspected SAH. Term ''poor grade'' is used for cases of SAH where the patient is unconscious
i.e. in a coma as a consequence of this disease and whose clinical condition requires
intubation and ventilation (with or without sedation) and thus admission to an intensive
care unit. All patients with poor grade SAH admitted to the neurosciences critical care unit
will be screened for participation in this study. All poor grade SAH patients are
unconscious and thus unable to give informed consent. Therefore, the next-of-kin of all
eligible patients will be approached to discuss and consider patient's involvement in the
study. If there is no next-of-kin, the treating clinician will be approached as a
professional consultee.
Once consent is obtained from next-of-kin, the participants will have the following
monitoring instituted:
1. An intracranial access device will be inserted under general anaesthesia with an
intracranial pressure (ICP), a Licox partial tension of tissue oxygen (PbtO2) probe and
a microdialysis (MD) catheter. Neuromonitors will be inserted into the part of the
brain that is supplied by the affected artery. This procedure will be performed on the
neurocritical care unit or in theatre if patients are undergoing other operative
procedures at the same time. Continuous neuromonitoring will commence. Hourly MD
samples will be processed and the leftover samples stored in -80oC for cytokine
analysis at a later date. Neuromonitoring will continue for as long as clinically
needed and up to 21 days from ictus.
2. All participants will be fitted with a near-infrared spectroscopy monitor (NIRS) . This
non-invasive monitor is used to measure tissue haemoglobin concentration and oxygen
content continuously and at the bedside.
3. Daily transcranial Doppler (TCD) examinations will be performed at the bedside to
assess the caliber of large cerebral arteries. This procedure is used in regular
clinical practice to diagnose large vessel spasm which is one of the pathological
substrates for delayed cerebral ischaemia (DCI) All participants will have a CT brain
perfusion scan between day 3 and day 5 from the initial haemorrhage (ictus) or when
clinically needed to assess brain perfusion and possibility of DCI which is part of
standard clinical practice. These scans are reviewed and reported by consultant
neuroradiologists. If they identify an area (or areas) of reversible ischaemia,
researchers will review the position of invasive brain monitors - if these are outside
of the area of DCI, additional monitors will be inserted into the identified area of
reversible ishaemia. Researchers will then use invasive brain monitors (MD and LiCox)
and non-invasive monitoring (NIRS and TCD) to assess the response to standard treatment
of cerebral reversible ischaemia which is hypertensive therapy i.e. mean arterial
pressure (MAP) augmentation with vasoactive medications.
Repeat CT brain perfusion scan will be performed between days 7 and 10 from the initial
haemorrhage or earlier if clinically indicated to assess response to treatment.
Following a 6 month period, researchers will see the patients in outpatient clinic to assess
functional outcome. This is part of the patient's standard clinical care as all our patients
are offered clinical follow up in this way.
Researchers will collect any biological samples that are available as part of the standard
clinical care of the participant and will not subject the participants to any additional
procedures. This would consist of:
- left over microdialysate samples that are not used for the standard clinical care of
the participant
- daily blood samples if the participant has an arterial line or central venous catheter
- samples of cerebrospinal fluid (CSF) if the participant has an external ventricular
drain
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