Ischemic Stroke Clinical Trial
Official title:
Neuroactive Steroids in Acute Ischemic Stroke: Association With Cognitive, Functional and Neurological Outcomes.
Despite several scientific and technological advances, there is no single neuroprotective
treatment that can reverse the brain damage after acute ischemic stroke (AIS). Neuroactive
steroids are cholesterol-derived hormones that have the ability to modulate the normal and
pathologic nervous system employing genomic and non genomic mechanisms.
In this work, we first investigated if AIS affects the plasma concentration of five
neuroactive steroids (cortisol, estradiol, progesterone, testosterone and 3-alpha
androstenediol glucuronide). Second, we studied if levels of circulating steroids associate
with neurological, cognitive and functional outcome in a cohort of 60 to 90 year-old male
and female patients with AIS.
For this purpose, we recruited patients who were hospitalized at the Emergency Room of the
Central Military Hospital within the first 24 hours after stroke onset. We designed two
experimental groups, each one composed of 30 control subjects and 30 AIS patients, both
males and females. The assessment of neurological deficit was performed with the NIHSS and
the tests used for the functional and cognitive status were: (1) modified Rankin Scale; (2)
Photo test and (3) abbreviated Pfeiffer's mental status questionnaire.
Introduction Acute ischemic stroke (AIS) represents a severe challenge to public health and
a heavy economic burden to countries with a growing senior population. This illness
represented the second cause of death and the third cause of world disability in 2010. In
Latin America there are a few epidemiological population-based studies and this information
comes from hospital records. In 2011 AIS caused 1 of every 20 deaths in the United States.
On average, every 40 seconds someone in the United States suffers a stroke and eventually
dies every 4 minutes from this disease. It has been shown that the incidence and mortality
of AIS is different between sexes. Despite advances in the pathophysiology and risk factors
of ischemic stroke, there is no effective treatment to cure cerebral ischemic damage. Among
the plethora of available drugs employed for CNS diseases, neuroactive steroids are
endogenous molecules derived from cholesterol or synthetic compounds that have the ability
to cross the blood-brain barrier and modulate brain function in health and disease. The
concentrations in plasma and cerebrospinal fluid of these molecules are altered in various
neurological diseases, although the clinical significance of these alterations remains to be
ascertained. In this work we evaluated whether AIS affects the plasma concentrations of
estradiol, progesterone, cortisol, testosterone and 3-alpha androstenediol glucuronide. As a
corollary of these measurements, we also evaluated if changes in circulating steroids bear a
relationship with the neurological outcome, cognitive status and functional dependence of
the AIS patients.
Material and Methods Participants We recruited patients with AIS from July 2014 to December
2014 who were hospitalized at the Emergency Room of the Central Military Hospital within the
first 24 hours after stroke onset. Stroke was defined according to the World Health
Organization's criteria, and a diagnosis of AIS was confirmed in all patients based on the
evidence of neuroimaging including computed tomography and magnetic resonance imaging,
following the Recommendations on Stroke Prevention, Diagnosis and Therapy Report. Sixty-90
year-old subjects were randomly selected and distributed in two experimental groups: 1) a
control group, involving subjects without physical or psychiatric illness, and 2) an AIS
group, consisting of: patients with diagnosis of AIS within the 24 hours of their
neurovascular event. Subjects were distributed between groups so that each group contained
30 patients (15 women and 15 men). The Ethics Committee of the Central Military Hospital H
Grl 601 ¨Cir My Dr. Cosme Argerich¨ approved the study (Act N ° 308, February 26, 2014), and
the patients or their next-of-kin provided informed consent for participation. Tables 1 and
2 shows the criteria employed for inclusion or exclusion of the studied subjects.
Procedures Patients were diagnosed for AIS by a certified neurologist at the Emergency Room
of the Central Military Hospital. Neurological, cognitive and functional status were
determined by NIHSS score, Photo test, Pfeiffer mental status score and by modified Rankin
score respectively. A sample of venous blood was withdrawn in the early morning (07 to 09
AM) after assessment of neurological and cognitive status. According to the Trial of Org
10172 in Acute Stroke Treatment (TOAST) criteria, stroke subtypes were classified as
large-artery atherothrombotic (LAA), cardioembolic (CE), small-artery occlusion (SAO), other
causes, and undetermined. Stroke risk factors included a medical history of hypertension,
defined as self-reported history of hypertension or using antihypertensive drugs, diabetes
mellitus (DM) defined as history of DM or using hypoglycemic medications at discharge,
dyslipidemias, defined as self-reported history of all types of dyslipidemia or oral
antidyslipidemia drugs or using antidyslipidemia drugs at discharge, atrial fibrillation
(AF), defined as history of AF, confirmed by at least one electrocardiogram or the presence
of arrhythmia during hospitalization, and modifiable lifestyle factors, including current
smoking, alcohol consumption, and obesity (body mass index >30 kg/m2).
Measures Quantitation of neuroactive steroids in plasma The measurement of estradiol
(Estradiol EII) and progesterone (Progesterone II) was performed by electrochemiluminescence
immunoassay (ECLIA) employing a Cobas e601, Roche Diagnostics, Mannheim, Deutschland. The
functional sensitivity of the method of estradiol was 12 pg/ml and the analytical
sensitivity was 5.0 pg/ml, while for progesterone the functional sensitivity of the method
was 0.15 ng/ml and the analytical sensitivity was 0.03 ng/ml according to the manufacturer.
In the case of cortisol and testosterone, they were determined by an immunoassay
chemiluminescent microparticle (CMIA) procedure, using a Team Architect i1000, Abbott
Laboratories, Middletown, USA. The cortisol functional sensitivity was 1μg/dL, and the
analytical sensitivity was 0.2 ng/ml, whereas for testosterone the functional sensitivity
was 1μg/dl and the analytical sensitivity was 0.05 ng/ml according to the manufacturer.
While alpha-3-androstenediolglucoronide was determined by radioimmunoassay (RIA) using a DSL
9200, Beckman Coulter, Texas USA . The functional sensitivity was 0.34 ng/ml according to
the manufacturer.
Neurological impairment during AIS The assessment of neurologic status during the AIS was
carried out with the National Institute of health stroke scale at the time of
hospitalization (NIHSS, available at
(http://www.ninds.nih.gov/doctors/NIH_Stroke_Scale.pdf).
Cognitive testing At the time of the cognitive assessment, patients with AIS were vigil on 9
or more points on the Glasgow Coma Scale. The cognitive tests used were: (1) Test photos and
(2) the abbreviated questionnaire of Pfeiffer. These tests were performed within 24 hours of
the AIS and prior to the extraction of blood for steroid analysis. The reasons for the
choice of these tests were: A) Test photos evaluated memory, object recognition and verbal
fluency. This test is not influenced by the level of education of the patient, it is simple
and brief in duration (4 minutes). B) The Pfeiffer Test studied orientation, calculation,
recent and remote memory, and information about daily events. It is important that the score
of this test depends of the total errors. It is also applicable to people with low
educational level, visual or auditory sensory deficit and advanced age.
Functional dependence for daily activities The functional status of patients with AIS was
measured with the modified Rankin Scale at the time of discharge. Data was collected through
an interview designed for the purpose of reducing the variability between evaluators.
;
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