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Stroke is the clinical term for acute loss of perfusion to vascular territory of
the brain, resulting in ischemia and a corresponding loss of neurologic
function.
Classified as either hemorrhagic or ischemic, strokes typically
manifest with the sudden onset of focal neurologic deficits, such as weakness,
sensory deficit, or difficulties with language.
Ischemic strokes have a heterogeneous group of causes, including thrombosis, em
bolism, and hypoperfusion, whereas hemorrhagic strokes can be either intraparenc
hymal or subarachnoid.
Only in recent years have advances allowed for significant improvement in the
outcome of this devastating disease. A new era in acute stroke care began in
1995, when the National Institute of Neurologic Disorders and Stroke (NINDS)
tissue plasminogen activator (t-PA) Stroke Study Group first presented data
indicating that early administration of t-PA benefited a carefully selected
patient group with acute ischemic stroke (AIS).1 While newer recanalization
approaches are being explored, all modalities are faced with the issue of time,
for "time is brain."2
Pathophysiology
The brain is the most metabolically active organ in the body. While representing
only 2% of the body's mass, it requires 15-20% of the total resting cardiac
output to provide the necessary glucose and oxygen for its metabolism. Ischemic
strokes result from events that limit or stop blood flow, such as embolism,
thrombosis in situ, or relative hypoperfusion. As blood flow decreases, neurons
cease functioning, and irreversible neuronal ischemia and injury begin at blood
flow rates of less than 18 mL/100 mg/min.
Ischemic cascade:
The processes involved in stroke injury at the cellular level are referred to as
the ischemic cascade. Many factors are thought to result in cell death and
dysfunction, and others are being discovered at a rapid rate. Within seconds to
minutes of the loss of glucose and oxygen delivery to neurons, the cellular
ischemic cascade begins. This is a complex process that begins with cessation of
the normal electrophysiologic function of the cells. The resultant neuronal and
glial injury produces edema in the ensuing hours to days after stroke, causing
further injury to the surrounding tissues.
Ischemic penumbra:
An acute vascular occlusion produces heterogeneous regions of ischemia in the
dependent vascular territory. The quantity of local blood flow is comprised of
any residual flow in the major arterial source and the collateral supply, if
any. Regions of the brain without significant flow are referred to collectively
as the core, and these cells are presumed to die within minutes of stroke onset.
Zones of decreased or marginal perfusion are collectively called the ischemic
penumbra. Tissue in the penumbra can remain viable for several hours because of
marginal tissue perfusion, and currently studied pharmacologic interventions for
preservation of neuronal tissue target this penumbra.
Recanalization strategies, including IV rt-PA and intra-arterial approaches
attempt to establish revascularization so that cells in the penumbra can be
rescued before irreversible injury occurs. Restoring blood flow can mitigate the
effects of ischemia only if performed quickly. Neuroprotective strategies are
intended to both preserve the penumbral tissues and extend the time window for
revascularization techniques. While no neuroprotective agent has demonstrated
benefit in definitive clinical trials, several studies are underway.
Mechanisms of Stroke
Embolic strokes
Emboli may either be of cardiac or arterial origin. Cardiac sources include
atrial fibrillation, recent myocardial infarction, prosthetic valves, native
valvular disease, endocarditis, mural thrombi, dilated cardiomyopathy, or patent
foramen ovale allowing passage of venous circulation emboli. Arterial sources
are atherothrombolic or cholesterol emboli that develop in the arch of the aorta
and in the extracranial arteries (ie, carotid and vertebral arteries). Embolic
strokes tend to have a sudden onset, and neuroimaging may demonstrate previous
infarcts in several vascular territories or calcific emboli.
Thrombotic strokes
Thrombotic strokes include large-vessel strokes and small-vessel or lacunar
strokes. They are due to in situ occlusions on atherosclerotic lesions in the
carotid, vertebrobasilar, and cerebral arteries, typically proximal to major
branches. Thrombogenic factors may include injury to and loss of endothelial
cells exposing the subendothelium and platelet activation by the subendothelium,
activation of the clotting cascade, inhibition of fibrinolysis, and blood
stasis. Thrombotic strokes are generally thought to originate on ruptured
atherosclerotic plaques. Intracranial atherosclerosis may be the cause in
patients with widespread atherosclerosis. In other patients, especially younger
patients, other causes should be considered, including hypercoagulable states
(eg, antiphospholipid antibodies, protein C deficiency, protein S deficiency),
sickle cell disease, fibromuscular dysplasia, arterial dissections, and
vasoconstriction associated with substance abuse.
Lacunar stroke
Lacunar strokes represent 20% of all ischemic strokes. They occur when the
penetrating branches of the middle cerebral artery (MCA), the lenticulostriate
arteries, or the penetrating branches of the circle of Willis, vertebral artery,
or basilar artery become occluded. Causes of lacunar infarcts include
microatheroma, lipohyalinosis, fibrinoid necrosis secondary to hypertension or
vasculitis, hyaline arteriosclerosis, and amyloid angiopathy. The great majority
are related to hypertension.
Watershed infarcts
These infarcts, also known as border zone infarcts, develop from relative
hypoperfusion in the most distal arterial territories and can produce bilateral
symptoms. Frequently, these occur perioperatively or in situations of prolonged
hypotension.
Frequency
Mortality/Morbidity
Stroke is the third leading cause of death in the United States (46.6 per
100,000 in 2005), following cardiac and cancer-related deaths. Worldwide in
1990, more than 4.3 million people died of cerebrovascular disorders.
Stroke is the leading cause of disability in the United States; 26% of stroke
survivors need assistance with daily living, 30% need some type of assistance
for walking, and 26% require admission to a long-term care facility.
Furthermore, at least one third of stroke survivors have depression as well as
many of their care providers.
The direct costs (ie, treatment) and indirect costs (ie, lost productivity) of
stroke in the United States are approximately $68.9 billion/year in 2009.
Race
In the United States, stroke has a higher incidence in the black population than
in the white population.3
Blacks have an age-adjusted risk of death from stroke that is 1.49 times that
of whites.
White males have a stroke incidence of 62.8 per 100,000, with death being the
final outcome in 26.3% of cases, compared with women who have a stroke
incidence of 59 per 100,000 and a death rate of 39.2%.
Hispanics have a lower overall incidence of stroke than whites and blacks but
more frequent lacunar strokes and stroke at an earlier age.
Sex
In patients younger than 60 years, the incidence of stroke is greater in males
(3:2 ratio).
Age
Stroke can occur in patients of all ages, including children.
Risk of stroke increases with age, especially in patients older than 64 years,
in whom 75% of all strokes occur.
The World Health Organization
estimates that 15 million people suffer a stroke worldwide each year, resulting
in 5 million deaths and 5 million people permanently disabled.
Clinical
History
The American Stroke Association advises the public to be aware of the symptoms
of stroke that are easily recognized and to call 911 immediately. These
symptoms include the following:
1. Sudden numbness or weakness of face, arm, or leg, especially on one side
of the body
2. Sudden confusion, difficulty in speaking or understanding
3. Sudden deterioration of vision of one or both eyes
4. Sudden difficulty in walking, dizziness, and loss of balance or coordinati
on
5. Sudden, severe headache with no known cause
A focused medical history aims to identify risk factors for atherosclerotic
and cardiac disease, including hypertension, diabetes mellitus, tobacco use,
high cholesterol, and a history of coronary artery disease, coronary artery
bypass, or atrial fibrillation. Consider stroke in any patient presenting with
acute neurological deficit or any alteration in level of consciousness.
Common signs of stroke include the following:
1. Acute hemiparesis or hemiplegia
2. Complete or partial hemianopia, monocular or binocular visual loss, or
diplopia
3. Dysarthria or aphasia
4. Ataxia, vertigo, or nystagmus
5. Sudden decrease in consciousness
- In younger patients, elicit a history of recent trauma, coagulopathies,
illicit drug use (especially cocaine), migraines, or use of oral
contraceptives.
- Family members, bystanders, and especially prehospital personnel can provide
invaluable information regarding the time and events surrounding the onset of
symptoms or when the patient was last seen normal.
- Establishing the time the patient was last normal is especially critical when
thrombolytic therapy is an option. If the patient awakens with the symptoms,
then the time of onset is defined as the time the patient was last seen
without symptoms. Family members, coworkers, or bystanders may be required to
help establish the exact time of onset, especially in right hemispheric
strokes accompanied by neglect or left hemispheric strokes with aphasia.
- If the patient is a candidate for thrombolytic therapy, a thorough review of
the inclusion and exclusion criteria must be performed. The exclusion criteria
largely focus on identifying risk of hemorrhagic complication associated with
thrombolytic use.
Physical
Physical examination is directed toward 5 major areas:
(1) assessing the airway, breathing, and circulation (ABCs)
(2) defining the severity of the patient's neurologic deficits
(3) identifying potential causes of the stroke
(4) identifying potential stroke mimics
(5) identifying comorbid conditions.
The physical examination must encompass all the major organ systems, starting
with the ABCs and the vital signs. Patients with stroke, especially
hemorrhagic, can clinically deteriorate quickly; therefore, constant
reassessment is critical. Ischemic strokes, unless large or involving the
brainstem, do not tend to cause immediate problems with airway patency,
breathing, or circulation compromise. On the other hand, patients with
intracerebral or subarachnoid hemorrhage frequently require intervention for
both airway protection and ventilation.
Vital signs, while nonspecific, can point to impending clinical
deterioration and may assist in narrowing the differential diagnosis. Many
patients with stroke are hypertensive at baseline, and their blood pressure
may become more elevated after stroke. While hypertension at presentation is
common, blood pressure decreases spontaneously over time in most patients.
Acutely lowering blood pressure has not proven to be beneficial in these
stroke patients in the absence of signs and symptoms of associated malignant
hypertension, AMI, congestive heart failure (CHF), or aortic dissection.
Head, ears, eyes, nose, and throat examination: A careful examination of the
head and neck is essential. Contusions, lacerations, and deformities may
suggest trauma as the etiology for the patient's symptoms. Auscultation of
the neck may elicit a bruit, suggesting carotid disease as the cause of the
stroke.
Cardiac: Cardiac arrhythmias, such as atrial fibrillation, are found
commonly in patients with stroke. Similarly, strokes may occur concurrently
with other acute cardiac conditions, such as AMI and acute CHF; thus,
auscultation for murmurs and gallops is recommended.
Extremities: Carotid or vertebrobasilar dissections, and less commonly,
thoracic aortic dissections, may cause ischemic stroke. Unequal pulses or
blood pressures in the extremities may reflect the presence of aortic
dissections.
The neurologic examination must be thorough, and yet this is perhaps the
weakest area of training for primary care and emergency providers. A directed
and focused examination can be performed in minutes and not only provides
great insight into the potential cause of the patient's deficits, but also
helps determine the intensity of treatment required.
A useful tool in quantifying neurological impairment is the National
Institutes of Health Stroke Scale (NIHSS). This scale easily used, is reliable
and valid, provides insight to the location of vascular lesions, and is
correlated with outcome in patients with ischemic stroke. It focuses on 6
major areas of the neurologic examination: (1) level of consciousness, (2)
visual function, (3) motor function, (4) sensation and neglect, (5) cerebellar
function, and (6) language. The NIHSS is used most by stroke teams. It enables
the consultant to rapidly determine the severity and possible location of the
stroke. A patient's score on the NIHSS is strongly associated with outcome,
and it can help identify those patients who are likely to benefit from
thrombolytic therapy and those who are at higher risk to develop hemorrhagic
complications of thrombolytic use.
Causes
Risk factors for ischemic stroke comprise both modifiable and nonmodifiable
etiologies. Identification of risk factors in each patient can uncover clues to
the cause of the stroke and the most appropriate treatment and secondary
prevention plan.
Nonmodifiable risk factors include age, race, sex, ethnicity, history of
migraine headaches, sickle cell disease, fibromuscular dysplasia, and
heredity.
Modifiable risk factors include the following:
Hypertension (the most important)
Diabetes mellitus
Cardiac disease - Atrial fibrillation, valvular disease, mitral stenosis,
and structural anomalies allowing right to left shunting, such as a patent
foramen ovale and atrial and ventricular enlargement
Hypercholesterolemia
Transient ischemic attacks (TIAs)
Carotid stenosis
Hyperhomocystinemia
Lifestyle issues - Excessive alcohol intake, tobacco use, illicit drug use,
obesity, physical inactivity
Oral contraceptive use
Differentials
Bell Palsy
Meningitis
Brain Abscess
Migraine Variants
Brain Metastasis
Seizures and Epilepsy, Overview and Classification
Cerebral Venous Thrombosis
Subdural Hematoma
Conversion Disorders
Transient Global Amnesia
Dizziness, Vertigo, and Imbalance
Viral Encephalitis
Epidural Hematoma
Hypoglycemia
Other Problems to be Considered
Hyperglycemia
Hypertensive urgency/emergency
Ingestions (eg, ethanol)
Spinal injury
Uremia
Workup
Lab Studies
Laboratory evaluation of the patient with ischemic stroke should be driven by
comorbid illnesses as well as the potential acute stroke.
Glucose and electrolyte tests: Hypoglycemia is the most common electrolyte
abnormality that produces strokelike symptoms. It is easily corrected, and
correction leads to rapid resolution of symptoms. Electrolyte disorders,
hyperglycemia, hypoglycemia, and uremia should be considered as the cause of
ongoing mental and physical deficits while pursuing the diagnosis of stroke.
Complete blood count: CBC provides key information regarding hemoglobin and
hematocrit, as well as platelet count, which is important in fibrinolytic
candidates. Additionally, sickle cell disease, polycythemia, and
thrombocytosis increase the risk for stroke.
Prothrombin time (PT) and activated partial thromboplastin time (aPTT)
tests: Many patients with acute stroke are on anticoagulants, such as
heparin or warfarin. Treatment decisions, such as thrombolytic use, require
data on coagulation status. An elevated international normalized ratio (INR)
may preclude patients from receiving thrombolytics.
Cardiac enzymes: Not infrequently patients with acute stroke also experience
acute myocardial ischemia. In addition to ECG findings, increased cardiac
enzymes might suggest concomitant cardiac injury.
Arterial blood gas (ABG) analysis: Although infrequent in patients with
suspected hypoxemia, ABG defines the severity of hypoxemia and may detect
acid-base disturbances. If considering thrombolytics, arterial punctures
should be avoided unless absolutely necessary.
Additional laboratory tests are tailored to the individual patient. They may
include rapid plasma reagent (RPR), toxicology screen, fasting lipid profile,
sedimentation rate, pregnancy test, antinuclear antibody (ANA), rheumatoid
factor, and homocysteine. In select patients with possible hypercoagulable
states, protein C, protein S, antithrombin III, and Factor V Leiden testing
may be required. These blood abnormalities mainly contribute to venous
thrombosis but may be relevant in patients with cardiac shunts or cerebral
venous thromboses. The anticardiolipin antibody and the lupus inhibitor, both
antiphospholipid antibodies, correlate with arterial stroke, as well as with
deep venous thrombosis, pulmonary embolism, myocardial infarction, and
miscarriage.
Imaging Studies
CT is, and probably will likely remain, the most commonly used form of
neuroimaging in the acute evaluation of patients with apparent acute stroke.
Noncontrast CT is very sensitive in detecting intracerebral and subarachnoid
hemorrhage, as well as subdural hematomas. Treatment algorithms are
dichotomous for the presence of intracranial blood, and recanalization
strategies for ischemic stroke require the absence of intracranial hemorrhage
on CT scan.
Although CT is not very sensitive for early ischemia (<6 h), several
findings can suggest ischemic changes relatively early in the time course of
stroke. Loss of the gray-white matter interface, loss of sulci, and loss of
the insular ribbon are subtle signs of early ischemia.
Early mass effect and areas of hypodensity suggest irreversible injury and
identify patients at higher risk of postfibrinolysis hemorrhage. Significant
hypodensity on the baseline scan should prompt a question about the time of
onset. Hypodensity in an area greater than one third of the MCA distribution
is considered by many a contraindication for thrombolytics.
A dense MCA sign suggests a clot in the MCA, potentially producing large
hemispheric strokes.
CT may demonstrate other causes of the patient's symptoms, including
neoplasm, hemorrhagic stroke, epidural and subdural hemorrhage, aneurysm,
abscess, arteriovenous malformation, and hydrocephalus.
CT angiography may demonstrate the location of vascular occlusion. CT
perfusion studies are capable of producing perfusion images and together
with CT angiography are becoming more available and utilized in the acute
evaluation of stroke patients.
MRI with magnetic resonance angiography (MRA) is a major advance in the
neuroimaging of stroke. MRI not only provides great structural detail but also
can demonstrate impaired metabolism. A major limitation of MRI is its
availability and the skills required to interpret the images.
Diffusion-weighted MRI (DW-MRI) can detect areas of ischemic brain injury
earlier in the evolution of ischemia than standard T1/T2-weighted MRI images
or CT scan by detecting changes in water molecule mobility.
Perfusion MRI (PW-MRI) uses injected contrast material to demonstrate areas
of decreased perfusion. These sequences in combination with DW-MRI yields
areas of diffusion-weighted imaging/perfusion-weighted imaging
(DW-MRI/PW-MRI) mismatch, theoretically identifying potentially salvageable
tissues.
MRA: This noninvasive technique demonstrates vascular anatomy and occlusive
disease of the head and neck.
Digital subtraction angiography is considered the definitive method for
demonstrating vascular lesions, including occlusions, stenoses, dissections,
and aneurysms. Cerebrovascular angiography not only provides useful
information on the extracranial and intracranial vasculature, but also allows
for intra-arterial therapies, both intra-arterial thrombolytics and
investigational catheter devices. Angiography requires special facilities and
a skilled operator and it carries a stroke risk of 1%.
MR spectroscopy is an experimental technique that may have potential for
distinguishing areas of salvageable neurons from those that are injured
irreversibly.
Carotid duplex scanning is one of the most useful tests in evaluating patients
with stroke. Increasingly, it is being performed earlier in the evaluation,
not only to define the cause of the stroke but also to stratify patients for
either medical management or carotid intervention if they have carotid
stenoses. Patients with symptomatic critical stenoses on carotid duplex
scanning may require anticoagulation before intervention is performed.
Transcranial Doppler ultrasonography (TCD) can assess the location and degree
of arterial occlusions in the extracranial carotid and large intracranial
vessels, including the middle cerebral and vertebrobasilar arteries. It can
also be used to detect restoration of flow after thrombolytic therapy, and the
recent Combined Lysis of Thrombus in Brain Ischemia Using Transcranial
Ultrasound and Systemic TPA (CLOTBUST) study has suggested that TCD may even
facilitate recanalization.
The use of single-photon emission computed tomography (SPECT) in stroke is
still relatively experimental and available only at select institutions; it
can theoretically define areas of altered regional blood flow.
Other Tests
Echocardiography: Transthoracic echocardiography (TTE) and transesophageal
echocardiography (TEE) are useful tools in evaluating patients with possible
cardiogenic sources of their stroke. TEE is more sensitive than TTE and can
evaluate the aortic arch and thoracic aorta for plaques or dissections.
Electrocardiography/ECG: Stroke and cardiovascular disease share many risk
factors. ECG may demonstrate cardiac arrhythmias, such as atrial fibrillation,
or may indicate acute ischemia. All patients with stroke should have an ECG as
part of their initial evaluation.
Chest radiography should be performed when clinically indicated.
Procedures
Lumbar puncture (LP): An LP is required to rule out meningitis or subarachnoid
hemorrhage when the CT scan is negative but the clinical suspicion remains
high.
Treatment
Medical Care
Medical care for AIS occurs on a continuum, beginning in the prehospital setting
and ending at home after discharge. Stroke centers and organized protocols for
the acute and in-house treatment of stroke patients have been shown to decrease
morbidity and mortality associated with stroke.4,5 Prehospital care personnel
are critical elements in the AIS chain of survival.6 Emergency medical
services (EMS) personnel should begin with the ABCs and, once the patient's
condition is stable, should perform a more directed assessment and administer
supportive treatment.
Prehospital stroke assessment tools, such as the Cincinnati Prehospital
Stroke Scale or Los Angeles Prehospital Stroke Scale, identify patients with
potential stroke.7 Providing supplemental oxygen when indicated,
establishing intravenous lines, measuring serum glucose, and administering
glucose in hypoglycemic patients are elements of prehospital stroke care.
Equally important is prehospital triage and notification of a potential
stroke patient. This allows for early mobilization of necessary resources,
such as a stroke team, radiology, and pharmacy.
With the creation and certification of primary stroke centers, regional
health care systems should determine the best triage policy for potential
stroke patients in their area.
The goal of acute stroke management in the emergency department is rapid and
efficient care. Continuing from the assessment of the ABCs, stroke patient
evaluation and, if eligible, fibrinolytic therapy should be administered
within 1 hour from presentation as shown below.
Table 2. NINDS and ACLS Recommended Stroke Evaluation Time Benchmarks for
Potential Thrombolysis Candidate8,9 Open table in new window
[ CLOSE WINDOW ]Table Time IntervalTime Target
Door to doctor10 min
Access to neurologic expertise15 min
Door to CT scan completion25 min
Door to CT scan interpretation45 min
Door to treatment60 min
Admission to monitored bed3 h
Time IntervalTime Target
Door to doctor10 min
Access to neurologic expertise15 min
Door to CT scan completion25 min
Door to CT scan interpretation45 min
Door to treatment60 min
Admission to monitored bed3 h
Again, general stroke management is a team effort with the nursing and medical
staff working closely together. General stroke care issues are outlined in the
table below.
General Management of Patients With Acute Stroke:
Blood glucoseTreat hypoglycemia with D50
Treat hyperglycemia with insulin if serum glucose >200 mg/dL
Blood pressureSee recommendations for thrombolysis candidates and
noncandidates (Table 4)
Cardiac monitorContinuous monitoring for ischemic changes or atrial
fibrillation
Intravenous fluidsAvoid D5W and excessive fluid administration
IV isotonic sodium chloride solution at 50 mL/h unless otherwise indicated
Oral intakeNPO initially; aspiration risk is great, avoid oral intake
until swallowing assessed
OxygenSupplement if indicated (Sa02 <93%, hypotensive, etc)
TemperatureAvoid hyperthermia, oral or rectal acetaminophen, and cooling
blankets as needed
Emergency management of patients with intracerebral hemorrhage (ICH) has been
updated in a new guideline of the The American Heart Association/American
Stroke Association.12 Among the changes in the new guideline are the use of
contrasted CT or CTA to look for active bleeding, intracranial pressure
monitoring for patients with Glasgow Coma Score <8, and maintenance of
normal glucose.
The guidelines leave undecided issues such as aggressive blood pressure
reduction, use of intraventricular tPA, prophylactic antiepileptic therapy,
and external ventricular drainage.
Many centers may have critical pathways in place for the treatment of ICH,
but few have protocols for the management of the disease.
The guidelines also mention evaluation of causes of recurrent hemorrhage
such as amyloid angiopathy, with apolipoprotein studies and use of MRI to
detect microbleeds.
The new guidelines echoe earlier guidelines in stating that surgery has not
proven beneficial in patients with cerebral hemorrhage, except in cerebellar
hemorrhage.
The new guidelines for the management of spontaneous intracerebral
hemorrhage can be found here.
Hypoglycemia and hyperglycemia need to be identified and treated early in the
evaluation. Not only can both produce symptoms that mimic ischemic stroke, but
both also can aggravate ongoing neuronal ischemia. Administration of glucose
in hypoglycemia produces profound and prompt improvement, while insulin should
be started for patients with stroke and hyperglycemia. Ongoing studies will
help determine the optimal level of glycemic control.13 Hyperthermia is
infrequently associated with stroke but can increase morbidity. Administration
of acetaminophen, by mouth or per rectum, is indicated in the presence of
fever (temperature >100.4°F).
Supplemental oxygen is recommended when the patient has a documented oxygen
requirement. To date, conflicting evidence exists that supernormal oxygenation
improves outcome.
Optimal blood pressure targets remain to be determined. Many patients are
hypertensive on arrival. Recent American Stroke Association guidelines have
reinforced the need for caution in lowering blood pressures acutely. Table 4
shows current recommendations for both candidates and noncandidates for
thrombolytic therapy.
In the small proportion of patients with stroke who are relatively
hypotensive, pharmacologically increasing blood pressure may improve flow
through critical stenoses.
Table 4. Blood Pressure Management in Patients With Stroke*
Open table in new window
[ CLOSE WINDOW ]Table Blood PressureTreatment
Candidates for fibrinolysisPretreatment:
SBP >185 or DBP >110 mm HgLabetalol 10-20 mg IVP 1-2 dosesor
Enalapril 1.25 mg IVP
Posttreatment:
DBP >140 mm HgSBP >230 mm Hg or
DBP 121-140 mm Hg
SBP 180-230 mm Hg or DBP 105-120 mm Hg
Sodium nitroprusside (0.5 mcg/kg/min)
Labetalol 10-20 mg IVP and consider labetalol infusion at 1-2 mg/min or
nicardipine 5 mg/h IV infusion and titrate
Labetalol 10 mg IVP, may repeat and double every 10 min up to maximum dose
of 150 mg
Noncandidates for fibrinolysisDBP >140 mm Hg
SBP >220 or
DBP 121-140 mm Hg or
MAP >130 mm Hg
SBP <220 mm Hg or
DBP 105-120 mm Hg or
MAP <130 mm Hg
Sodium nitroprusside 0.5 mcg/kg/min; may reduce approximately 10-20%
Labetalol 10-20 mg IVP over 1-2 min; may repeat and double every 10 min up
to maximum dose of 150 mg or nicardipine 5 mg/h IV infusion and titrate
Antihypertensive therapy indicated only if AMI, aortic dissection, severe
CHF, or hypertensive encephalopathy present
*Adopted from 2005 Advanced Cardiac Life Support (ACLS) guidelines and
2007 American Stroke Association Scientific Statement
Abbreviations: SBP - systolic blood pressure; DBP - diastolic blood
pressure; IVP - intravenous push; MAP - mean arterial pressure
Blood PressureTreatment
Candidates for fibrinolysisPretreatment:
SBP >185 or DBP >110 mm HgLabetalol 10-20 mg IVP 1-2 doses
or
Enalapril 1.25 mg IVP
Posttreatment:
DBP >140 mm Hg
SBP >230 mm Hg or
DBP 121-140 mm Hg
SBP 180-230 mm Hg or DBP 105-120 mm Hg
Sodium nitroprusside (0.5 mcg/kg/min)
Labetalol 10-20 mg IVP and consider labetalol infusion at 1-2 mg/min or
nicardipine 5 mg/h IV infusion and titrate
Labetalol 10 mg IVP, may repeat and double every 10 min up to maximum dose
of 150 mg
Noncandidates for fibrinolysisDBP >140 mm Hg
SBP >220 or
DBP 121-140 mm Hg or
MAP >130 mm Hg
SBP <220 mm Hg or
DBP 105-120 mm Hg or
MAP <130 mm Hg
Sodium nitroprusside 0.5 mcg/kg/min; may reduce approximately 10-20%
Labetalol 10-20 mg IVP over 1-2 min; may repeat and double every 10 min up
to maximum dose of 150 mg or nicardipine 5 mg/h IV infusion and titrate
Antihypertensive therapy indicated only if AMI, aortic dissection, severe
CHF, or hypertensive encephalopathy present
*Adopted from 2005 Advanced Cardiac Life Support (ACLS) guidelines and
2007 American Stroke Association Scientific Statement
Abbreviations: SBP - systolic blood pressure; DBP - diastolic blood
pressure; IVP - intravenous push; MAP - mean arterial pressure
Labetalol (Normodyne)
Adrenergic receptor-blocking agent with both nonselective beta-adrenergic and
selective alpha1 competitive receptor-blocking actions. Produces dose-related
decreases in blood pressure without inducing reflex tachycardia.
DosingInteractionsContraindicationsPrecautionsAdult
10-20 mg IV over 1-2 min; may repeat or double q10min; total dose not to exceed
150 mg
May initiate IV drip at 1-2 mg/min and increase to 2-8 mg/min
Pediatric
Not establishedDosingInteractionsContraindicationsPrecautionsDecreases effect of
diuretics and increases toxicity of methotrexate, lithium, and salicylates; may
diminish reflex tachycardia resulting from nitroglycerin use without interfering
with hypotensive effects; cimetidine may increase blood levels; glutethimide may
decrease effects by inducing microsomal enzymes
DosingInteractionsContraindicationsPrecautionsDocumented hypersensitivity;
bronchial asthma; heart block; cardiac failure; cardiogenic shock; symptomatic
bradycardia; hypotension
DosingInteractionsContraindicationsPrecautionsPregnancyC - Fetal risk revealed
in studies in animals but not established or not studied in humans; may use if
benefits outweigh risk to fetusPrecautionsCaution in impaired hepatic function;
discontinue therapy if signs of liver dysfunction; in elderly patients, response
rate may be lower and incidence of toxicity higher
Enalapril (Vasotec)
Angiotensin-converting enzyme (ACE) inhibitor. By inhibiting ACE, decreases
circulating angiotensin II levels and suppresses renin-angiotensin-aldosterone
system, lowering overall blood pressure.
DosingInteractionsContraindicationsPrecautionsAdult
0.625-1.25 mg IV; may repeat if inadequate response
Pediatric
Not establishedDosingInteractionsContraindicationsPrecautionsNSAIDs may reduce
hypotensive effects; may increase digoxin, lithium, and allopurinol levels;
rifampin decreases levels; probenecid may increase levels; diuretics may
increase hypotensive effects
DosingInteractionsContraindicationsPrecautionsDocumented hypersensitivity;
history of ACE-induced angioedema or idiopathic or hereditary angioedema; acute
renal failure; hyperkalemia
DosingInteractionsContraindicationsPrecautionsPregnancyD - Fetal risk shown in
humans; use only if benefits outweigh risk to fetusPrecautionsCaution in renal
impairment, valvular stenosis, or severe CHF
Nicardipine (Cardene)
A calcium channel blocker, inhibiting calcium ion influx into vascular smooth
muscle and myocardium.
DosingInteractionsContraindicationsPrecautionsAdult
Start 5 mg/h IV, increase by 2.5 mg/h q5-15min to a maximum of 15 mg/h
Pediatric
Not establishedDosingInteractionsContraindicationsPrecautionsMay increase
carbamazepine, digoxin, cyclosporine, and theophylline levels; when administered
with amiodarone, may cause bradycardia and a decrease in cardiac output; when
administered with beta-blockers, may increase cardiac depression; cimetidine may
increase levels
DosingInteractionsContraindicationsPrecautionsDocumented hypersensitivity;
severe CHF; sick sinus syndrome; second- or third-degree AV block; hypotension
(<90 mm Hg systolic)
DosingInteractionsContraindicationsPrecautionsPregnancyC - Fetal risk revealed
in studies in animals but not established or not studied in humans; may use if
benefits outweigh risk to fetusPrecautionsCaution in impaired renal or hepatic
function; may increase LFTs, and hepatic injury may occur.
Diazepam (Valium)
Act on GABA receptor complex in limbic system and thalamus, producing calming
effect. Useful in controlling active seizures and should be augmented by
longer-acting anticonvulsants, such as phenytoin or phenobarbital.
DosingInteractionsContraindicationsPrecautionsAdult
5 mg IV q5-10min; total dose not to exceed 20 mg
Pediatric
Not establishedDosingInteractionsContraindicationsPrecautionsPhenothiazines,
barbiturates, alcohols, and MAOIs increase CNS toxicity; drugs that impair
hepatic function, such as cimetidine, may increase risk of sedation
DosingInteractionsContraindicationsPrecautionsDocumented hypersensitivity; acu
te
narrow-angle glaucoma or open-angle glaucoma
DosingInteractionsContraindicationsPrecautionsPregnancyD - Fetal risk shown in
humans; use only if benefits outweigh risk to fetusPrecautionsMay cause
significant sedation and obscure neurologic examination findings; caution in
impaired hepatic function; caution with other CNS depressants, low albumin
levels, or hepatic disease (may increase toxicity)
Lorazepam (Ativan)
Short-acting benzodiazepine with moderately long half-life. Has become drug of
choice in many centers for treating active seizures.
DosingInteractionsContraindicationsPrecautionsAdult
1-4 mg IV over 2-10 min; may repeat q10-15min
Pediatric
Not establishedDosingInteractionsContraindicationsPrecautionsAlcohol,
phenothiazines, barbiturates, and MAOIs increase CNS toxicity; valproate or
probenecid may increase serum concentrations
DosingInteractionsContraindicationsPrecautionsDocumented hypersensitivity; acu
te
narrow-angle glaucoma
DosingInteractionsContraindicationsPrecautionsPregnancyD - Fetal risk shown in
humans; use only if benefits outweigh risk to fetusPrecautionsCaution in renal,
pulmonary, or hepatic impairment, myasthenia gravis, organic brain syndrome,
altered mental status, alcohol intoxication, or Parkinson disease
Antipyretic agents
Hyperthermia in acute stroke is potentially harmful and should be treated.
Agents with potential bleeding risk should be avoided if possible.
Alteplase (Activase)
Commercially manufactured recombinant DNA fibrinolytic protein approved for
treatment of AMI, AIS, and acute massive pulmonary embolism.
DosingInteractionsContraindicationsPrecautionsAdult
0.9 mg/kg IV; not to exceed 90 mg/dose; infuse over 60 min with 10% of total
dose administered as initial IV bolus over 1 min
Pediatric
Not establishedDosingInteractionsContraindicationsPrecautionsDrugs that alter
platelet function (eg, aspirin, dipyridamole, clopidogrel, abciximab) may
increase risk of bleeding prior to, during, or after alteplase therapy
Note that criteria for use of IV t-PA preclude use of antiplatelet or
antithrombotic agents for 24 h following t-PA infusion
DosingInteractionsContraindicationsPrecautionsDocumented hypersensitivity;
active internal bleeding; stroke within last 3 mo; recent intracranial or
intraspinal surgery or trauma; intracranial hemorrhage on pretreatment
evaluation; suspicion of subarachnoid hemorrhage, intracranial neoplasm,
arteriovenous malformation, or aneurysm; bleeding diathesis; severe uncontrolled
hypertension
DosingInteractionsContraindicationsPrecautionsPregnancyC - Fetal risk revealed
in studies in animals but not established or not studied in humans; may use if
benefits outweigh risk to fetusPrecautionsNoncompressible arterial punctures and
internal jugular and subclavian venous punctures must be avoided to minimize
bleeding from noncompressible sites; in event of serious bleeding, immediately
discontinue alteplase; monitor patients for allergic-type reactions, such as
anaphylactoid reaction, laryngeal edema, rash, and urticaria
Follow-up
Further Inpatient Care
Inpatient care is tailored to the severity of the acute stroke and comorbid
illnesses. Recent studies support the admission to a dedicated stroke unit
with specially trained staff to reduce morbidity and mortality rates.21,25,26
The goals of early supportive care after admission (adapted from the American
Stroke Associations guidelines) include the following:
Observe changes in the patient's condition that might prompt different
medical or surgical interventions. Notably, 25% of patients worsen in the
first 24-48 hours after admission.
Facilitate medical or surgical measures aimed at improving outcome after
stroke. This includes evaluation for carotid stenoses and cardioembolic
sources.
Institute measures to prevent subacute complications. Foley catheters
increase the risk for urinary tract infection and should be used only when
absolutely necessary. Sequential compression stockings, subcutaneous
heparin, and low-molecular-weight heparin decrease the risk of deep vein
thrombosis.
The CLOTS Trials Collaboration assessed the effectiveness of graduated
compression stockings (GCS) to reduce the risk of deep vein thrombosis (DVT)
after stroke. The group evaluated 2518 patients admitted to the hospital who
were immobile following acute stroke. Doppler ultrasound established
baseline and follow-up assessment for development of DVT. No difference was
noted between patients allocated to GCS and those who did not use GCS,
although skin breaks, ulcers, blisters, and skin necrosis were significantly
the rates of stroke in patients with coronary artery disease and elevated or
high-normal levels of low-density lipoprotein (LDL) cholesterol.
Medications to address hypertension, hyperlipidemia, and diabetes mellitus
should be reviewed with the patient prior to discharge.
Transfer
EMS triage and transfer of patients with stroke is an important issue in
stroke care. The recommendation for the establishment of stroke centers, as
well as Joint Commission certification, has helped define for consideration
the elements of both primary and comprehensive stroke centers.25,28 The
reader is referred to the eMedicine article by Helmi Lutsep, MD, Stroke Team
Creation and Management.
With the organization of regional stroke care delivery systems, EMS agencies
in many states and regions are being instructed to selectively triage patients
with potential stroke to stroke centers that have demonstrated capabilities to
evaluate and treat these patients in a timely fashion.
As part of each hospital's stroke protocol and pathway, criteria for patient
transfer to other medical facilities must be established before the actual
need. If available, patients with acute stroke should be admitted to stroke
units.
Hospitals without neuroimaging capabilities should stabilize and immediately
transfer patients with potential stroke to centers with CT scan
availability.
Hospitals without intensive care units or access to timely neurosurgical
expertise should transfer patients who are candidates for thrombolytics or
who have received thrombolytics to institutions that can provide those
services.
Patients with large hemispheric strokes who may be at significant risk for
edema and increased ICP and who may require neurosurgical expertise should
be transferred before clinical deterioration occurs.
Deterrence/Prevention
The acute hospitalization is focused not only on treating the acute stroke but
also on identifying risk factors for recurrent stroke and beginning to modify
these risk factors if possible.
See more about primary and secondary prevention of stroke in eMedicine's
article Medical Treatment of Stroke.
Complications
Complications associated with reperfusion strategies are as follows.
Postfibrinolytic complications center around a bleeding issue. Of greatest
concern is intracerebral hemorrhage, typically occurring within the first 12
hours after treatment. Despite careful patient selection and protocol
adherence, symptomatic intracerebral hemorrhage (sICH) rates of
approximately 5-6%, remain steady. A recent study by Goldstein et al,
demonstrated significant growth in fibrinolysis-induced sICH hematoma volume
after first detection, suggesting opportunities to mitigate hematoma growth
and further deterioration.29 The optimal mechanisms to correct pre-existing
or fibrinolysis-induced coagulopathies remain to be determined.
Even without fibrinolysis, intra-arterial mechanical thrombectomy is also
associated with increased risk of sICH, in part due to these patients
experiencing larger strokes. Thus, strict adherence to postreperfusion
guidelines, such as strict blood pressure control, should be observed.
Other potential sites of bleeding include GI tract, oropharynx and
nasopharynx (gingiva, nares), genitourinary tract (associated with Foley
catheters), skin (typically at sites of intravenous lines), and sites of
intra-arterial access for IA procedures.
t-PA is also associated with a roughly 1% rate of orolingual angioedema.
Other nonhemorrhagic complications following a stroke can be divided into
those occurring acutely, typically within 72 hours, and those occurring later.
Acute complications include cerebral edema, increased ICP, and possible
herniation, hemorrhagic transformation, aspiration pneumonia, and seizures.
Subacute complications include pneumonia, deep venous thrombosis and
pulmonary emboli, urinary tract infections, decubitus ulcers, contractures,
spasticity, joint problems such as the shoulder-hand syndrome, and
malnutrition.
A significant number of stroke survivors also experience depression.
Identification and treatment of depression is extremely important in
maximizing quality of life, not only for stroke survivors, but also for
their families and care providers.
Prognosis
The prognosis after AIS varies greatly, depending upon the premorbid
condition, stroke severity, age, and poststroke complications.30 Mortality
rate: In the Framingham and Rochester stroke studies, the overall mortality
rate at 30 days after stroke was 28%. The mortality rate at 30 days after
ischemic stroke was 19%. The 1-year survival rate for patients with ischemic
stroke in the Framingham study was 77%.
Morbidity: In stroke survivors from the Framingham Heart Study, 31% needed
help caring for themselves, 20% needed help when walking, and 71% had impaired
vocational capacity in long-term follow-up.
Patient Education
Education is paramount in the fight to prevent and treat stroke. Education
must include all elements of the stroke chain of survival. While medical
education is often difficult and requires constant reinforcement, it has
potential for minimizing the stroke burden.
Public education must involve all age groups. Incorporating stroke into basic
life support (BLS) and cardiopulmonary resuscitation (CPR) curricula is just
one way to reach a younger audience. Avenues to reach an audience with a
higher stroke risk include using local churches, employers, and senior
organizations to promote stroke awareness.
Prehospital care providers are essential to timely stroke care. Course
curriculum for prehospital care providers is beginning to include more
information on stroke than ever before. Through certification and ACLS
instruction, as well as continuing medical education classes, prehospital care
providers can remain current on stroke and promote stroke awareness in their
own communities.
Physician and nursing staff involved in the care of patients who have had a
stroke, both in the emergency department and in the hospital, should
participate in scheduled stroke education. This will help them maintain the
skills required to treat stroke patients effectively and to remain current on
medical advances for all stroke types.
For excellent patient education resources, visit eMedicine's Stroke Center.
Also, see eMedicine's patient education articles Stroke and Transient Ischemic
Attack (Mini-stroke).
Miscellaneous
Medical/Legal Pitfalls
In patients with TIAs, failure to recognize the potential for further stroke
and perform a timely assessment for stroke risk factors exposes the patient to
undue risk of stroke and clinicians to potential litigation. TIAs confer a 10%
risk of stroke within 30 days. Recent studies suggest that of the strokes
occurring after a TIA, half occurred within 48 hours of the TIA.
Failure to thoroughly document the evaluation and treatment plan of the
patient with acute stroke is behind a significant proportion of medical
malpractice cases involving stroke. Carefully consider thrombolytic therapy in
all patients presenting within 3 hours of symptom onset, and reasons for
treating (risk/benefit analysis) or not treating the patient must be
documented clearly.