Management of acute stroke. (Featured CME Topic: Stroke).Abstract: Stroke ranks as the third leading cause of death and the most common cause of permanent disability in adults. Timely recognition and treatment is imperative to reduce stroke-related morbidity and modality. Patients with acute isehemic stroke should be evaluated for administration of intravenous tissue plasminogen activator tissue plasminogen activator n. Abbr. TPA 1. An enzyme that catalyzes the conversion of plasminogen to plasmin, used to dissolve blood clots rapidly and selectively, especially in the treatment of heart attacks. 2. (t-PA); those who do not qualify for t-PA should receive aspirin therapy in the absence of a contraindication contraindication /con·tra·in·di·ca·tion/ (-in?di-ka´shun) any condition which renders a particular line of treatment improper or undesirable. con·tra·in·di·ca·tion n. . In all stroke patients, intravenous hydration hydration /hy·dra·tion/ (hi-dra´shun) the absorption of or combination with water. hy·dra·tion n. 1. The addition of water to a chemical molecule without hydrolysis. 2. with normal saline should be administered, hypoxia hypoxia Condition in which tissues are starved of oxygen. The extreme is anoxia (absence of oxygen). There are four types: hypoxemic, from low blood oxygen content (e.g., in altitude sickness); anemic, from low blood oxygen-carrying capacity (e.g. should be corrected with supplemental oxygen, and hyperglycemia hyperglycemia: see diabetes. and fever should be treated aggressively. Blood pressure management should be individualized on the basis of stroke pathophysiology and specific treatment plan (e.g., planned thrombolysis thrombolysis /throm·bol·y·sis/ (throm-bol´i-sis) dissolution of a thrombus. throm·bol·y·sis n. pl. throm·bol·y·ses Dissolution or destruction of a thrombus. ) following published guidelines. Evaluation of stroke etiology should be undertaken, and the results should be used to guide secondary stroke prevention efforts. ********** An estimated 730,000 strokes and 300,000 transient ischemic attacks (TIAs) occur in the United States each year.' Stroke ranks as the third leading cause of death and the most common cause of permanent disability in adults; approximately half of all stroke survivors return to some form of employment, although this figure declines with age. (2) At any given time, there are about 4.6 million survivors of stroke, and 170,000 individuals die each year in this country as a direct or indirect consequence of stroke. (3) Most recent estimates place the cost of stroke in the United States in excess of $45 billion per year. (3) Timely recognition and treatment are imperative to reduce stroke-related morbidity and mortality Morbidity and Mortality can refer to:
Clinical Diagnosis Typical Presentation By and large, the diagnosis of stroke is not difficult. Symptoms typically begin suddenly and are referable to the region of the brain that is ischemic Ischemic An inadequate supply of blood to a part of the body, caused by partial or total blockage of an artery. Mentioned in: Antiangiogenic Therapy, Subarachnoid Hemorrhage, Ventricular Fibrillation ischemic or afflicted by hemorrhage. Internal carotid artery distribution strokes often produce unilateral numbness or weakness, or both. In addition, there may be signs of cortical dysfunction such as aphasia, apraxia apraxia Disturbance in carrying out skilled acts, caused by a lesion in the cerebral cortex; motor power and mental capacity remain intact. Motor apraxia is the inability to perform fine motor acts. Ideational apraxia is loss of the ability to plan even a simple action. , agnosia Agnosia An impairment in the recognition of stimuli in a particular sensory modality. True agnosias are associative defects, where the perceived stimulus fails to arouse a meaningful state. , and visual field defects (Table 1). Vertebrobasilar distribution strokes can produce unilateral or bilateral sensorimotor sensorimotor /sen·so·ri·mo·tor/ (sen?sor-e-mo´ter) both sensory and motor. sen·so·ri·mo·tor adj. Of, relating to, or combining the functions of the sensory and motor activities. deficits, often accompanied by signs and symptoms more specific for brainstem or cerebellar cerebellar /cer·e·bel·lar/ (ser?e-bel´ar) pertaining to the cerebellum. Cerebellar Involving the part of the brain (cerebellum), which controls walking, balance, and coordination. dysfunction: vertigo, diplopia diplopia /di·plo·pia/ (di-plo´pe-ah) the perception of two images of a single object. binocular diplopia , disequilibrium, ataxia ataxia (ətăk`sēə), lack of coordination of the voluntary muscles resulting in irregular movements of the body. Ataxia can be brought on by an injury, infection, or degenerative disease of the central nervous system, e.g. , and cranial nerve palsies (Table 2). Because the posterior circulation also supplies parts of the thalamus thalamus (thăl`əməs), mass of nerve cells centrally located in the brain just below the cerebrum and resembling a large egg in size and shape. , internal capsule, and temporal and occipital lobes via the posterior cerebral artery Noun 1. posterior cerebral artery - arises from the basilar artery; divides into three branches arteria cerebri, cerebral artery - any of the arteries supplying blood to the cerebral cortex , strokes in this distribution may present with some combination of sensorimotor symptoms, memory disturbance, and homonymous homonymous /ho·mon·y·mous/ (-i-mus) 1. having the same or corresponding sound or name. 2. pertaining to the corresponding vertical halves of the visual fields of both eyes. visual field impairment. Dysarthria dysarthria /dys·ar·thria/ (dis-ahr´thre-ah) a speech disorder caused by disturbances of muscular control because of damage to the central or peripheral nervous system. dys·ar·thri·a n. is a nonspecific symptom or sign that may occur with stroke in either the carotid or vertebrobasilar distribution. Patients with intracranial hemorrhage (ICH) tend to exhibit a smoothly progressive neurologic decline over the initial hours. They also complain of acute headache and exhibit vomiting or early impairment of consciousness more often than patients with ischemic stroke do. Aside from this last feature, there is nothing at physical examination that reliably enables the clinician to distinguish between ischemic stroke and ICH. The clinical presentation associated with "spontaneous" (ie, nontraumatic) subarachnoid hemorrhage (SAH Subarachnoid hemorrhage (SAH) Loss of blood into the subarachnoid space, the fluid-filled area that surrounds the brain tissue. Mentioned in: Cerebral Aneurysm ) typically serves to distinguish this stroke subtype from all others. If a history can be obtained, acute headache almost invariably is reported. When the hemorrhage is extensive, impaired consciousness is present at initial examination, and acute seizure activity may occur. Focal neurologic deficits are absent unless there is also extension of hemorrhage into the brain parenchyma Parenchyma A ground tissue of plants chiefly concerned with the manufacture and storage of food. The primary functions of plants, such as photosynthesis, assimilation, respiration, storage, secretion, and excretion—those associated with living or ischemia due to vasospasm vasospasm /vaso·spasm/ (va´zo-) (vas´o-spazm) angiospasm; spasm of blood vessels, causing vasoconstriction.vasospas´tic va·so·spasm n. ; ischemia is rarely seen in the acute setting. Stroke Mimickers There are several disorders that may mimic stroke and thus confound diagnosis (Table 3). Patients experiencing seizures can present with focal neurologic deficits, especially in the immediate postictal period when there may be unilateral weakness (ie, Todd paralysis) or other signs also commonly associated with stroke. Such deficits usually resolve over several hours but may persist as long as a day or more. There may be a history of an established seizure disorder. The patient or an observer may relate the occurrence of involuntary, rhythmic movements, but frequently the patient cannot recall the seizure itself, the seizure is unobserved, or the seizure is nonconvulsive and thus unapparent. Although brain neoplasms more commonly cause gradually progressive symptoms and signs, tumors--primary or metastatic--also may mimic stroke. Acute, strokelike deterioration occurs most often when there is hemorrhage within the tumor or tumor-associated seizure activity but, at times, symptoms related to tumors may resemble those from stroke or TIA (1) (Telecommunications Industry Association, Arlington, VA, www.tiaonline.org) A membership organization founded in 1988 that sets telecommunications standards worldwide. It was originally an EIA working group that was spun off and merged with the U.S. for no discernible reason. Systemic infections and toxic-metabolic disturbances may mimic stroke, especially in patients with preexisting pre·ex·ist or pre-ex·ist v. pre·ex·ist·ed, pre·ex·ist·ing, pre·ex·ists v.tr. To exist before (something); precede: Dinosaurs preexisted humans. v.intr. focal brain injury. The acute systemic illness can bring to light old, previously subclinical subclinical /sub·clin·i·cal/ (sub-klin´i-k'l) without clinical manifestations. sub·clin·i·cal adj. Not manifesting characteristic clinical symptoms. Used of a disease or condition. , neurologic deficits. Migrainous aura may be confused with TIA or stroke, especially when it is prolonged and, on rare occasions, ischemic stroke can complicate migraine. With migrainous aura, there is typically a history of prior, similar symptoms that have been associated with headache. Often nausea, vomiting, photophobia photophobia /pho·to·pho·bia/ (-fo´be-ah) abnormal visual intolerance to light.photopho´bic pho·to·pho·bi·a n. 1. , and phonophobia accompany the aura. Hypoglycemia hypoglycemia: see diabetes. hypoglycemia Below-normal levels of blood glucose, quickly reversed by administration of oral or intravenous glucose. Even brief episodes can produce severe brain dysfunction. can acutely produce focal neurologic symptoms and signs that reso lve rapidly after administration of glucose or dextrose dextrose: see glucose. . This diagnosis should be considered and excluded in any patient with apparent stroke who is receiving hypoglycemic hypoglycemic /hy·po·gly·ce·mic/ (-gli-sem´ik) 1. pertaining to, characterized by, or causing hypoglycemia. 2. an agent that lowers blood glucose levels. therapy or is otherwise at risk for low blood sugar. Multiple sclerosis may present acutely with signs and symptoms indistinguishable from stroke on clinical grounds, but a careful history and selective diagnostic testing generally serve to establish the correct diagnosis. Intracranial intracranial /in·tra·cra·ni·al/ (-kra´ne-al) within the cranium. in·tra·cra·ni·al adj. Within the cranium. hematomas (subdural subdural /sub·du·ral/ (-door´al) between the dura mater and the arachnoid. sub·dur·al adj. Located or occurring beneath the dura mater. and epidural) also may present in a strokelike fashion. With chronic subdural hematoma, a history of recent trauma is far from invariable, and this is especially true in cases involving the elderly or individuals who are administered warfarin warfarin (wôr`fərĭn), anticoagulant used to treat blood clots. In large doses it causes bleeding. Warfarin, mixed with bait, is used in rodent control. warfarin Anticoagulant drug, marketed as Coumadin. or are otherwise at risk for spontaneous bleeding. Even so, in the absence of antecedent severe trauma, patients with subdural hematomas most often present with headache, fluctuating depression of consciousness, and no or minimal focal neurologic deficit. At times, infectious encephalitis may mimic ac ute stroke but fever, seizure activity, alteration of consciousness, and abnormal cerebrospinal fluid findings are likely to be present. Acute Stroke Management Initial Management. Once the diagnosis of acute stroke is suspected, the duration of symptom onset must be determined, as time from stroke onset remains the single most important determinant of therapeutic options (Fig. 1). Patients with symptom onset of less than 3 hours should be evaluated for potential treatment with intravenous tissue plasminogen activator (t-PA). All patients should receive intravenous hydration with normal saline, hypoxia should be corrected with supplemental oxygen, hyperglycemia should be treated with insulin, and fever should be treated aggressively with antipyretics. The head of the bed may be placed in the horizontal position for patients with ischemic stroke and no elevation of intracranial pressure (ICP (1) (Internet Cache Protocol) A protocol used by one proxy server to query another for a cached Web page without having to go to the Internet to retrieve it. See CARP and proxy server. ). (4) An electrocardiogram electrocardiogram /elec·tro·car·dio·gram/ (-kahr´de-o-gram?) a graphic tracing of the variations in electrical potential caused by the excitation of the heart muscle and detected at the body surface. should be performed and patients should receive continuous cardiac monitoring. Blood should be drawn for a complete blood cell with platelet count, prothrombin time test with international normalized ratio International Normalized Ratio Hematology A method of reporting prothrombin time–PT results for Pts receiving oral anticoagulant therapy; the INR is defined by the formula, PTPatient/PTMNPT , partial thromboplastin time Partial Thromboplastin Time Definition The partial thromboplastin time (PTT) test is a blood test that is done to investigate bleeding disorders and to monitor patients taking an anticlotting drug (heparin). test, basic chemistries, fasting lipids, and cardiac markers, when appropriate. Additional blood testing may be appropriate on a case-by-case basis. Oral intake should be withheld until the patient passes a swallow test with sips of water. Patients with hyperacute stroke should undergo emergent brain computed tomography (CT). The major value of acute CT scanning is in differentiating intracerebral hemorrhage from ischemic stroke and other pathologic processes such as subdural hematoma, tumor, and abscess. CT scan may also delineate the extent of ischemia. For all ischemic stroke subtypes, magnetic resonance imaging magnetic resonance imaging (MRI), noninvasive diagnostic technique that uses nuclear magnetic resonance to produce cross-sectional images of organs and other internal body structures. (MRI 1. (application) MRI - Magnetic Resonance Imaging. 2. MRI - Measurement Requirements and Interface. ) demonstrates evidence of ischemic injury to the brain earlier than does CT, and newer MRI techniques (such as diffusion-weighted imaging) have further increased its sensitivity. The clinical implications of early positive MRI or the significance of mismatches in diffusion-weighted and perfusion defects are as yet unclear, but it is conceivable that these or other noninvasive means of assessing ischemic injury may serve to indicate whether hyperacute interventional therapy is likely to be beneficial. Management of Blood Pressure. During brain ischemia, cerebral autoregulation is impaired and cerebral blood flow Cerebral blood flow, or CBF, is the blood supply to the brain in a given time.[1] In an adult, CBF is 750 mls/min or 15% of the cardiac output. On a weight basis, this is 50 to 54 milllitres/100grams/minute. becomes pressure passive (ie, blood flow declines with declining perfusion pressure). Blood pressure should therefore not be treated unless one of the following exists: 1) systolic blood pressure Systolic blood pressure Blood pressure when the heart contracts (beats). Mentioned in: Hypertension (SBP SBP Spontaneous bacterial peritonitis, see there ) exceeds 220 mm Hg or diastolic blood pressure Diastolic blood pressure Blood pressure when the heart is resting between beats. Mentioned in: Hypertension (DBP DBP Diastolic Blood Pressure DBP Development Bank of the Philippines DBP Database Project (Visual Studio File Extension) DBP DNA Binding Protein DBP Disinfection Byproduct DBP Deutsche Bundespost ) exceeds 120 mm Hg after repeated measurements; 2) cardiac ischemia, heart failure, or aortic dissection is present; 3) thrombolytic therapy is planned; or 4) intracerebral hemorrhage is identified. In the latter situation, blood pressure should be maintained below 180/105 mm Hg, with more aggressive control reserved for patients with no prior history of hypertension. (5) Specific treatment recommendations for the management of blood pressure after acute stroke are presented in Tables 4 and 5. (6) Intravenous Thrombolysis. Intravenous thrombolysis with tissue plasminogen activator (t-PA) is indicated for selected patients within 3 hours of ischemic stroke onset. (7,8) It is important to bear in mind that when stroke onset time is unclear (eg, patient awakens with a deficit), onset time is considered to be the time when patients were last known to be in their usual state of health. Inclusion and exclusion criteria for t-PA are listed in Table 6. If blood pressure exceeds 185/110 mm Hg, a single dose of an antihypertensive antihypertensive /an·ti·hy·per·ten·sive/ (-ten´siv) counteracting high blood pressure, or an agent that does this. an·ti·hy·per·ten·sive adj. Reducing high blood pressure. n. can be administered; the patient qualifies for therapy if blood pressure declines below this level. Blood pressure should be monitored every 15 minutes for 2 hours after the start of infusion, then every 30 minutes for 6 hours, and then every 60 minutes for 16 hours. Blood pressure must be maintained below 185/110 mm Hg and antithrombotic agents must be avoided for the first 24 hours post-thrombolysis (Table 5). Other Considerations. Patients with ischemic stroke who do not qualify for intravenous t-PA should be administered aspirin (160-325 mg/d) as it has been shown to modestly reduce the risk of recurrent stroke and death when administered within the first 48 hours poststroke. (9,10) Neurosurgical consultation should be sought for patients with cerebellar hemorrhage or large cerebellar ischemic infarctions. Although currently available data do not support the emergent administration of anticoagulants Anticoagulants Drugs that suppress, delay, or prevent blood clots. Anticoagulants are used to treat embolisms. Mentioned in: Embolism, Heart Valve Replacement for most patients with acute ischemic stroke, nonambulatory patients must receive deep vein thrombosis A blood clot (thrombos) in a vein deep within the muscle, typically in the thigh or calf. It is caused by disease or the lack of activity such as sitting for hours at a computer screen. prophylaxis with heparin or low-molecular weight heparins or heparinoids. (10,11) For those who cannot receive antithrombotic drugs, intermittent external compression stockings should be used. Early mobilization is recommended and the use of an indwelling catheter should be avoided, if possible. Fever should be treated aggressively with antipyretics, and antibiotics should be administered for infectious causes. Phys ical, occupational, and speech therapy should be ordered when indicated. Determining Ischemic Stroke Mechanism For patients with ischemic stroke, the pathophysiologic process has generated the stroke and the specific etiology that underlies that process should be determined. All ischemic strokes typically result from one of these three primary causes: embolism embolism Obstruction of blood flow by an embolus—a substance (e.g., a blood clot, a fat globule from a crush injury, or a gas bubble) not normally present in the bloodstream. Obstruction of an artery to the brain may cause stroke. , large vessel thrombosis, and small vessel thrombosis. Identification of the pathophysiologic mechanism that has generated the stroke under evaluation (eg, cardioembolism) is not synonymous with identification of that stroke's specific etiology (eg, atrial fibrillation). To determine the cause of stroke with any degree of accuracy and without undue expense, one must consider the age and health history of the patient, details of events surrounding the acute stroke, and findings from the bedside evaluation. With these data, the clinician can address those questions that direct the diagnostic management: With which stroke subtype am I dealing? Which specific causes are more likely to to be responsible for this pathophysiologic process? Which tests will enable me to confirm my clinical impression? Even with intensive neurodiagnostic intervention, a specific cause of ischemic stroke will not be identified in a sizable proportion of patients. This is especially true when a young person has had a stroke and the cause is not immediately apparent from the initial bedside evaluation. In several recent studies of large patient groups with acute ischemic stroke, the incidence of stroke of unknown cause ranged from 18 to 40%. (12,13) Whether such cases will exhibit a response to acute or chronic stroke therapy similar to that observed in patients with stroke from an identifiable cause is unclear. Complications of Stroke Neurologic complications of stroke include stroke progression, seen in over 25% of patients, or recurrence, which is less common with a rate dependent on the mechanism of the index event. Seizures can occur in up to 10% of patients at some point after stroke and are more common after subarachnoid subarachnoid /sub·arach·noid/ (sub?ah-rak´noid) between the arachnoid and the pia mater. Subarachnoid Referring to the space underneath the arachnoid mater. oir intracerebral hemorrhage and large lesions involving the cerebral cortex. Stroke-related seizures are usually easily controlled with a single anticonvulsant anticonvulsant /an·ti·con·vul·sant/ (-kon-vul´sant) inhibiting convulsions, or an agent that does this. an·ti·con·vul·sant n. A drug that prevents or relieves convulsions. . Increased ICP is the most lethal poststroke complication and may be a direct effect of a hematoma hematoma /he·ma·to·ma/ (he?mah-to´mah) a localized collection of extravasated blood, usually clotted, in an organ, space, or tissue. or brain edema. Brain edema after ischemic stroke (usually cytotoxic) typically becomes symptomatic after 1 to 4 days. Signs and symptoms of raised ICP include depressed level of consciousness, pupillary pu·pil·lar·y adj. Of or affecting the pupil of the eye. pupillary pertaining to or emanating from the pupil. pupillary aperture the pupil. asymmetry, abducens abducens /ab·du·cens/ (ab-doo´senz) [L.] drawing away. abducens [L.] drawing away. abducens nerve see abducent nerve, and Table 14. nerve palsy, papilledema, and periodic breathing. Treatment of raised ICP should include fluid restriction, elevation of the head of the bed, administration of osmotic diuretics, and hyperventilation hyperventilation /hy·per·ven·ti·la·tion/ (-ven?ti-la´shun) 1. abnormally increased pulmonary ventilation, resulting in reduction of carbon dioxide tension, which, if prolonged, may lead to alkalosis. 2. . Some degree of vascular cognitive impairm ent or frank dementia can occur in up to 33 to 50% of patients. Recent evidence suggests that cholinesterase inhibitors may be of value in treating these patients. (14, 15) Patients should be monitored for poststroke depression, which occurs in up to 60% of patients and is treatable with antidepressants and/or psychotherapy. (16) Medical complications after stroke include cardiac abnormalities (eg, arrhythmia, myocardial infarction), pulmonary embolism, infection (eg, urinary tract, pneumonia), and gastrointestinal bleeding. Patient and Caregiver Education Patients and caregivers should be educated regarding both short- and long-term clinical expectations. Symptoms of post-stroke depression should be reviewed and patients instructed to seek treatment if appropriate. Applicable secondary stroke preventive strategies should be discussed and stroke symptoms should be reviewed. The use of emergency medical services An Emergency medical service (abbreviated to initialism "EMS" in many countries) is a service providing out-of-hospital acute care and transport to definitive care, to patients with illnesses and injuries which the patient believes constitutes a medical emergency. should be encouraged should the patient experience recurrent stroke symptoms. Emerging Therapies For patients with ischemic stroke in whom intravenous thrombolysis is not indicated, consideration can be given to the administration of intra-arterial thrombolysis if the appropriate facilities and personnel are available. A prospective, randomized controlled trial A randomized controlled trial (RCT) is a scientific procedure most commonly used in testing medicines or medical procedures. RCTs are considered the most reliable form of scientific evidence because it eliminates all forms of spurious causality. of intra-arterial prourokinase (17) showed a treatment benefit for selected patients with middle cerebral artery Noun 1. middle cerebral artery - one of two branches of the internal carotid artery; divides into three branches arteria cerebri, cerebral artery - any of the arteries supplying blood to the cerebral cortex stroke, but prourokinase is not currently available for use. These data have led to the adoption of protocols for the administration of intra-arterial t-PA at some centers. The safety and efficacy of the combination of a lower dose of intravenous t-PA followed by intra-arterial t-PA are currently under investigation. Other antithrombotic agents under clinical investigation for ischemic stroke include intravenous heparin administered within 12 hours of stroke onset, a platelet glycoprotein IIb/IIIa antagonist (abciximab), and a direct thrombin inhibitor Direct thrombin inhibitors (DTIs) are a class of medication that act as anticoagulants (delaying blood clotting) by directly inhibiting the enzyme thrombin. Some are in clinical use, while others are undergoing clinical development. (argatroban). Various neuroprotective strategies have been under investigation for administration in isolation or in combination with a thrombolytic agent, but unfortunately no agent has proven effective to date. Mild hypothermia is a powerful neuroprotective strategy in preclinical models and pilot studies in stroke (18) and the recent positive trials after cardiac arrest (19,20) have generated significant interest in this strategy. It is likely that no single agent or intervention will be the "magic bullet" for all patients with stroke but that future management will involve combinations of strategies and directed therapies based on stroke subtype, location, and/or diffusion and perfusion MRI findings.
Table 1
Anterior circulations stroke symptoms and signs
More
specific Less specific Uncommon
Aphasia Unilateral numbness or weakness Ataxia
Apraxia Visual field deficit Vertigo/disequilibrium
Agnosia Dysarthria Nausea/vomiting
Headache
Table 2
Posterior circulation stroke symptoms and signs
More specific Less specific
Ataxia Dysarthria
Diplopia Headache
Vertigo/disequilibrium Unilateral numbness or weakness
Bilateral numbness or weakness Nausea/vomiting
Visual field deficit
Table 3
Stroke mimickers
Seizure
Mass lesion
Migraine
Hypoglycemia
Systemic infection
Toxic-metabolic encephalopathy
Multiple sclerosis
Intracranial (eg, subdural or epidural) hematoma
Table 4
Antihypertensive therapy for hemorrhagic stroke (a)
Blood pressure (b) Treatment
1. SBP >230 or DBP Sodium nitroprusside (0.5-10
>120 mm Hg [micro]g/kg/min) or nitroglycerine
drip (at 10-20 [micro]g/min).
2. SBP >180 or DBP Consider 10 mg labetalol (c) IVP.
>105 mm Hg May repeat or double labetalol every
10 to 20 min to a maximum dose
of 300 mg. Alternatively,
administer initial labetalol
bolus and then start labetalol
drip at 2 to 8 mg/min.
3. Hypertension relative to If prehemorrhage BP is estimated to
prestroke condition have been considerably lower (eg,
120/80 mm Hg), then antihypertensive
therapy may be appropriate to approximate
premorbid pressures, particularly
in the first hours after
subarachnoid hemorrhage.
(a) Reproduced from Advanced Cardiac Life Support Copyright [C] 1997
American Heart Association. (6) DBP, diastolic blood pressure; SBP,
systolic blood pressure; BP, blood pressure; min, minutes; IVP,
Intravenous push.
(b) All initial blood pressures should be verified before treatment by
repeating reading in 5 min.
(c) Labetalol should be avoided in patients with asthma, cardiac
failure, or severe abnormalities in cardiac conduction. For refractory
hypertension, alternative therapy may be considered with sodium
nitroprusside or enalapril.
Table 5
Antihypertensive therapy for acute ischemic stroke (a)
Blood Pressure (b) Treatment
Nonthrombolytic candidates
DBP > 140 mm Hg Sodium nitroprusside
(0.5[micro]g/kg/min). Aim for 10
to 20% reduction in DBP.
SBP > 220, DBP > 120, 10 to 20 mg labetalol (d) IV push
or MAP (c) > 130 mm Hg over 1 to 2 min.
May repeat or double
labetalol every 20 min to
a maximum dose of 150 mg.
SBP < 220, DBP > 120, or Emergency
MAP (c) 130 mm Hg antihypertensive therapy is
deferred in the absence of aortic
dissection, acute
myocardial infarction
severe congestive heart failure,
or hypertensive encephalopathy.
Thrombolytic candidates
Pretreatment 1 to 2 inches of nitropaste or 1
SBP > 185 or to 2 doses of 10 to 20
DBP > 110 mm Hg mg labetalol (d) IV push.
If BP is not reduced and maintaine
to < 185/110 mm Hg, the patient
should not be treated with tPA.
During and after treatment
Monitor BP BP is monitored every 15 min for 2
hours then every 30 min for 6 hours, and
then every 1 hour for 16 hours.
DBP > 140 mm Hg Sodium nitroprusside
(0.5 [micro]g/kg/min)
DBP > 230 or DBP (1) 10 mg labetalol (d) IVP over
121 to 140 mm Hg 1 to 2 min. May repeat or double
labetalol every 10 min to a
maximum dose of 150 mg or give
the initial labetalol bolus and
then start a labetalol drip at
2 to 8 mg/min.
(2) If BP not controlled by
labetalol, consider sodium
nitroprusside.
4. SBP 180 to 230 or DBP 10 mg labetalol (d) IVP. May
105 to 120 mm Hg repeat or double labetalol every
10 to 20 min to maximum dose of
150 mg or give initial labetalol
bolus and start a labetalol drip
at 2 to 8 mg/min.
(a) Reproduced from Advanced Cardiac Life Support Copyright [c] 1997
American Heart Association. (6) DBP, diastolic blood pressure; SBP,
systolic blood pressure, MAP, mean arterial pressure; BP, blood
pressure; min, minutes; tPA. tissue plasminogen activator; IV,
intravenous.
(b) All initial blood pressures should be verified before treatment by
repeating reading in 5 min.
(c) As estimated by one third the sum of systolic and double diastolic
pressure.
(d) Labetalol should be avoided in patients with asthma, cardiac
failure, or severe abnormalities in cardiac conduction. For refractory
hypertension, alternative therapy may be considered with sodium
nitroprusside or enalapril.
Table 6
Inclusion and exclusions criteria for administration of intravenous
tissue plasminogen activator for acute stroke (a)
Inclusion
Age >18 yr
Ischemic stroke by clinical assessment
Persistent neurologie deficit beyond
sensory defi cit or ataxia
Cranial computed tomography negative
for hemorrhage
Initiation of treatment within 3 hours
after symptom onset
Exclusion
Treatment initiated >3 hours after
symptom onset
Neurologic deficit that is rapidly
improving based on history or
observation
CT scan shows major early infarct
signs (eg, substantial edema, mass
effect, midline shift)
Patient taking oral anticoagulants
or with PT >15 seconds (INR > 1.7)
Patient receiving heparin within the
preceding 48 hours who has a
prolonged PTT
Platelet count <100,000/[mm.sup.3]
Pretreatment systolic blood pressure
>185 mm Hg or diastolic pressure >110
mm Hg or if aggressive treatment is
required to reduce blood pressure to
the specified limits before thrombolytic
therapy
Prior stroke or any serious head trauma
in the preceding 3 months
Major surgery within the preceding 21 days
Prior intracerebral hemorrhage
Gastrointestinal or urinary tract
hemorrhage within the preceding 14 days
Seizure at the onset of stroke
Symptoms suggestive of SAH
Arterial puncture at a noncompressible
site within the previous 7 days
(a) CT, computed tomographic; PT, prothrombin time; INR, international
normalized ratio; PTT, partial thromboplastin time; SAH, subarachnoid
hemorrhage.
Accepted November 7, 2002. References (1.) Broderick J, Brott T, Kothari R, Miller R, Khoury J, Pancioli A, et al. The Greater Cincinnati/Northern Kentucky Stroke Study: Preliminary first-ever and total incidence rates of stroke among blacks. Stroke 1998;29:415-421. (2.) Black-Schaffer RM, Osberg JS. Return to work after stroke: Development of a predictive model. Arch Phys Med Rehabil 2002;71:285-290. (3.) American Heart Association American Heart Association (AHA), n.pr a national voluntary health agency that has the goal of increasing public and medical awareness of cardiovascular diseases and stroke, and thereby reducing the number of associated deaths and disabilities. . Targeting the Facts. Dallas, American Heart Association, 2002 (pamphlet). (4.) Schwarz S, Georgiadis D, Aschoff A, Schwab S. Effects of body position on intracranial pressure and cerebral perfusion in patients with large hemispheric stroke. Stroke 2002;33:497-501. (5.) Broderick JP, Adams HP Jr, Barsan W, Feinberg W, Feldmann E, Grotta J, et al. Guidelines for the management of spontaneous intracerebral hemorrhage: A statement for healthcare professionals from a special writing group of the Stroke Council, American Heart Association. Stroke 1999;30:905-915. (6.) Cummins RO (ed). Acute stroke, in Textbook of Advanced Cardiac Life Support Advanced Cardiac Life Support See ACLS. . Dallas, American Heart Association, 1997, pp 10-1-10-28. (7.) Quality Standards Subcommittee, American Academy of Neurology The American Academy of Neurology (AAN) is a professional society for neurologists and neuroscientists. As a medical specialty society it was established in 1949 by A.B. Baker of the University of Minnesota to advance the art and science of neurology, and thereby promote the best . Practice advisory: Thrombolytic therapy for acute ischemic stroke: Summary statement. Report of the Quality Standards Subcommittee of the American Academy of Neurology. Neurology 1996;47:835-839. (8.) Adams HP, Brott TG, Furlan AJ, Gomez CR, Grotta J, Helgasan CM, et al. Guidelines for thrombolytic therapy for acute stroke: A supplement to the guidelines for the management of patients with acute isehemic stroke--A statement for healthcare professionals from a special writing group of the Stroke Council, American Heart Association. Circulation 1996;94:1167-1174. (9.) Chen Z, Sandercock P, Pan H, Counsell C, Collins R, Liu L, et al. Indications for early aspirin use in acute ischemic stroke: A combined analysis of 40,000 randomized ran·dom·ize tr.v. ran·dom·ized, ran·dom·iz·ing, ran·dom·iz·es To make random in arrangement, especially in order to control the variables in an experiment. patients from the Chinese Acute Stroke Trial and the International Stroke Trial. Stroke 2000;31:1240-1249. (10.) Coull BM, Williams LS, Goldstein LB, Meschia JF, Heitzman D, Chaturvedi S, et al. Anticoagulants and antiplatelet agents in acute isehemic stroke: Report of the Joint Stroke Guideline Development Committee of the American Academy of Neurology and the American Stroke Association (a Division of the American Heart Association). Neurology 2002;59:13-22. (11.) Adams HP Jr. Emergent Use of anticoagulation for treatment of patients with ischemic stroke. Stroke 2002;33:856-861. (12.) Frey JL, Jahnke HK, Bulfinch EW. Differences in stroke between white, Hispanic, and Native American patients: The Barrow Neurological Institute Stroke Database. Stroke 1998;29:29-33. (13.) Sacco RL, Ellenberg JH, Mohr JP, Tatemichi TK, Hier DB, Price TR, et al. Infarcts of undetermined cause: The NINCDS NINCDS National Institute of Neurological and Communication Disorders and Stroke Stroke Data Bank. Ann Neural 1989;25:382-390. (14.) Erkinjuntti T, Kurz A, Gauthier S, Bullock R, Lilienfeld S, Rao C, et al. Efficacy of galanthamine in probable vascular dementia and Alzheimer's disease combined with cerebrovascular disease: A randomized trial. Lancet 2002;359:1283-1290. (15.) Moretti R, Torre P, Antonello RM, Cazzato G. Rivastigmine in subcortical subcortical /sub·cor·ti·cal/ (-kor´ti-k'l) beneath a cortex, such as the cerebral cortex. vascular dementia: A comparison trial on efficacy and tolerability for 12 months follow-up. Eur J Neurol 2001;8:361-362. (16.) Provinciali L, Coccia M. Poststroke and vascular depression: A critical review. Neurol Set 2002;22:417-428. (17.) Furlan A, Higashida R, Wcchsler L, Gent M, Rowley J, Kase C, et al; The PROACT PROACT Neurology A clinical trial–Prolyse in Acute Cerebral Thromboembolism Investigators. Intra-arterial prourokinase for acute ischemic stroke: The PROACT II Study--A randomized controlled trial. JAMA JAMA abbr. Journal of the American Medical Association 1999;282:2003-2011. (18.) Kammersgaard LP, Rasmussen BH, Jorgensen HS, Reith J, Weber U, Olsen TS. Feasibility and safety of inducing modest hypothermia in awake patients with acute stroke through surface cooling: A case-control study. The Copenhagen Stroke Study. Stroke 2000;31:2251-2256. (19.) The Hypothermia after Cardiac Arrest Study Group. Mild therapeutic hypothermia to improve the neurologic outcome after cardiac arrest. N Engl J Med 2002;346:549-556. (20.) Bernard SA, Gray TW, Buist MD, Jones BM, Silvester W, Gutteridge G, et al. Treatment of comatose survivors of out-of-hospital cardiac arrest with induced hypothermia. N Engl J Med 2002;346:557-563. RELATED ARTICLE: Key Points * Timely recognition and treatment are imperative to reduce stroke-related morbidity and mortality. * Patients with acute ischemic stroke should be evaluated for the administration of intravenous tissue plasminogen activator (t-PA); those who do not qualify for t-PA should receive aspirin therapy in the absence of a contraindication. * In all stroke patients, intravenous hydration with normal saline should be administered, hypoxia should be corrected with supplemental oxygen, and hyperglycemia and fever should be treated aggressively. * Blood pressure management should be individualized on the basis of stroke pathophysiology and specific treatment plan (e.g., planned thrombolysis) following published guidelines. * Evaluation of stroke etiology should be undertaken and used to guide secondary stroke prevention efforts. From the Stroke Center, University of South Alabama The University of South Alabama is a public, doctoral-level university in Mobile, Alabama, USA. It was created by the Alabama Legislature in 1963, and replaced existing extension programs operated in Mobile by the University of Alabama. College of Medicine, Mobile, AL. Reprint requests to Richard M. Zweifler, MD, Stroke Center, University of South Alabama College of Medicine, 2451 Fillingim Street, Mobile, AL 36617. Email: rzweifle@usouthal.edu Copyright [c] 2003 by The Southern Medical Association 0038-4348-03/9604-0380 |
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