Stroke Clinical Trial
Official title:
The Brain Heart Interaction in Acute Stroke
Many studies have shown that acute cerebral dysfunction can impair cardiac function and autonomic control of blood pressure, heart rate and vascular tone, however, the size of the stroke is rarely reported. Involvement of the insular cortex seems to predispose to cardiac damage and autonomic dysfunction. However, it is not clear whether cardiac dysfunction is merely a marker of large strokes or location of the stroke is critical.
Background
On one hand structural cardiac anomalies and arrhythmias such as atrial fibrillation can
give rise to thrombi that are dislodged as emboli to the brain and cause stroke. On the
other hand acute emotional stress or cerebral events can cause acute cardiac dysfunction
with left ventricular failure in the absence of cardiac causes. The extreme variant of
stress cardiomyopathy is known as Takotsubo cardiomyopathy. Patients are presenting with
chest pain, electrocardiographic changes similar to acute myocardial infarction with
ST-segment elevation, T-wave inversion, or QT prolongation, and elevated cardiac biomarkers
such as CK and troponin. When coronary angiography is performed coronary arteries are
normal, but the left ventricle shows mostly apical and midventricular dyskinesia and apical
ballooning or rarely basal akinesia and apical hyperkinesia. The exact pathogenesis is
unknown. Presumably high catecholamine levels resulting from the extreme emotional stress or
acute cerebral events cause severe peripheral vasospasms resulting in myocardial
dysfunction.
It has been known for many decades that myocardial damage such as small patchy necroses and
subendocardial hemorrhages and cardiac arrhythmias can occur after subarachnoid or
intracerebral haemorrhage. Greenhout and Reichenbach and Weidler observed abnormally
increased autonomic activity or an imbalance between parasympathetic and sympathetic input
to the heart. Systematic analyses of heart and brain interactions were first performed by JW
Norris and coworkers in Toronto. They examined cardiac enzymes in 230 acute stroke patients
and found raised CK-MB in 25 (11%). They also found that catecholamine concentrations in
stroke patients were higher than in controls, that patients with higher CK levels had higher
norepinephrine levels, more often arrhythmias and such elevated CK and norepinephrine levels
were more common in hemispheric compared to brain stem strokes. DiAngelantonio et al
assessed cardiac troponin I levels on admission of 330 stroke patients. When troponin I
levels were elevated the odds for in-hospital death or non-fatal cardiac events were
increased. These results were corroborated in a systematic review of 15 similar studies.
According to this review troponin was elevated in 18.1% of 2901 stroke patients. Patients
with elevated troponin levels had an odds ratio of 3.0 (95% CI 1.5-6.2) for showing
electrocardiographic changes and an odds ratio for death of 2.9 (95% CI 1.7-4.8). Hakan Ay
and coworkers addressed the question whether stroke in specific brain areas are more prone
to cardiac damage. In a case control study they analysed diffusion weighted MR images of
patients with elevated troponin T levels (cTnT) and patients with normal levels to identify
voxels with diffusion restriction that are associated with troponin elevation. Brain regions
that were a priori associated with cTnT elevation included the right posterior, superior,
and medial insula and the right inferior parietal lobule. Among patients with right middle
cerebral artery infarction, the insular cluster was involved in 88% of patients with and 33%
without cTnT elevation (odds ratio: 15.00; 95% CI: 2.65 to 84.79). Their findings indicate
that the right insula is associated with elevated serum cardiac troponin T level indicative
of myocardial injury. In an additional MR study using diffusion and perfusion imaging the
same group of researchers found that infarctions encompassing the insula is associated with
increased conversion of ischemic but potentially viable penumbral tissues into infarction.
Unlike Ay et al Laowattana and coworkers found left insular stroke associated with an
increased risk of adverse cardiac outcome and decreased cardiac wall motion compared to
stroke in other locations and TIA. According to their findings left insular lesions show
decreased parasympathetic tone and right insular lesions increased sympathetic drive. This
results in abnormal fluctuations in blood pressure, abnormal circadian blood pressure
patterns, higher norepinephrine levels and elevated blood pressure in acute stroke.
Furthermore, baroreflex sensitivity has been found to be reduced after stroke, i.e.
autonomic adjustment of heart rate and vascular tone to sudden blood pressure changes was
compromised. Sykora et al demonstrated that baroreflex impairment in acute stroke is not
associated with carotid atherosclerosis but with insular involvement. In their study both
insulae seemed to participate in processing the baroreceptor information with the left
insula being more dominant. Other authors found that there might be a hemispheric dominance
of autonomic control and that impairment of cardiovascular autonomic control increases with
higher NIHSS scores. The reason for the neuroanatomic correlation of insular strokes and
myocardial injury and that middle cerebral artery stroke involving the insula are more prone
to growth as found by Ay et al is not known. A hypothesis focuses on the tight connections
of the insular cortex to the limbic system. Phylogenetically the limbic system belongs to
the oldest parts of the brain. It encompasses a group of gyri and nuclei and
interconnections in the center of the brain such as amygdala, hippocampus, gyrus cinguli,
fornix, anterioventral thalamic nuclei, and hypothalamus. The main functions of the limbic
system is controlling the endocrine and autonomic nervous system, emotional life and
behavior, olfaction, pleasure, and short and long term memory and learning. Dysautonomia
after stroke is independent whether stroke is ischemic or hemorrhagic. Similarly, excitation
of the cortex in epilepsy can result in cardiac dysfunction. Epilepsy can cause ictal
tachycardia and bradycardia and ECG changes, even if brain imaging does not show any
structural abnormality. In addition, more than a third of epilepsy patients show ictal
bradycardia that would merit insertion of a permanent pacemaker. Sudden unexpected death is
increased five fold in epilepsy, and especially patients with treatment refractory
generalised tonic clonic seizures are at risk. One of the main reasons might be brain heart
interactions with asystole. To summarize, many studies have shown that acute cerebral
dysfunction can impair cardiac function and autonomic control of blood pressure, heart rate
and vascular tone, however, the size of the stroke is rarely reported. Involvement of the
insular cortex seems to predispose to cardiac damage and autonomic dysfunction. However, it
is not clear whether cardiac dysfunction is merely a marker of large strokes or location of
the stroke is critical.
Objective
The aim of the proposed research is to answer the question whether both size of stroke and
location are independent predictors of impairment of cardiac function in acute stroke.
Methods
This is a retrospective analysis of patients of the Bernese Stroke Data Base who all had a
full MRI examination at admission. All acute stroke patients will be screened for Troponin
elevations, abnormal electrocardiograms or both. Patients with primary cardiac causes or
other reasons for troponin elevations or ECG changes will be handled separately. The study
patients will be compared to at least 200 control stroke patients without troponin
elevations and without ECG changes. Infarct location, vessel occlusions and volumes of
diffusion restriction and perfusion deficit will be assessed on MR images. In a
multivariable analysis, the investigators will find out whether Troponin elevations and ECG
abnormalities are associated with infarct location or infarct size or both. In addition, the
investigators will perform a voxel based analysis for correlation of infarct location and
troponin elevations and ECG abnormalities.
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Observational Model: Cohort, Time Perspective: Retrospective
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