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Management of Acute Ischemic Stroke Anna Finley Caulfield, MD * , Christine A.C. Wijman, MD, PhD Department of Neurology and Neurological Sciences, Neurocritical Care Program, Stanford Stroke Center, Stanford University School of Medicine, 701 Welch Road, B-325, Palo Alto, CA 94304, USA Stroke is the third leading cause of death and the leading cause of dis- ability in the United States and is associated with a tremendous cost bur- den to society [1]. Most strokes are ischemic, but about 15% of strokes are caused by intracerebral or subarachnoid hemorrhage. Currently, there is only one drug approved by the US Food and Drug Administration (FDA), intravenous tissue plasminogen activator (tPA), for the treatment of acute ischemic stroke within 3 hours of symptom onset [2]. Many stroke patients do not receive intravenous tPA, however, most commonly because they present beyond the 3-hour therapeutic window. More recently devel- oped therapeutic strategies offer the hope of safe and effective treatment beyond the 3-hour time window in selected patients. This article is an up- date of a recent publication that reviewed established and novel treatments for acute ischemic stroke and the management issues that may arise in the first hours to days after symptom onset [3]. Blood pressure management, management of intracranial hypertension, and temperature management are discussed in greater detail elsewhere in this issue. Initial management The initial management of acute ischemic stroke involves medical stabi- lization, including airway protection and ventilatory and hemodynamic Material for this article is reprinted in part from the American Academy of Neurology 2006 meeting syllabus titled ‘‘Critical Care for Cerebrovascular Patients: What General Neurologists Need to Know’’; with permission. This is an updated version of an article that originally appeared in Critical Care Clinics, volume 22, issue 4. * Corresponding author. E-mail address: [email protected] (A. Finley Caulfield). 0733-8619/08/$ - see front matter Ó 2008 Elsevier Inc. All rights reserved. doi:10.1016/j.ncl.2008.03.016 neurologic.theclinics.com Neurol Clin 26 (2008) 345–371

Management of Acute Ischemic Stroke

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  • Department of Neurology and Neurological Sciences, Neurocritical Care Program,

    Neurol Clin 26 (2008) 345371Stanford Stroke Center, Stanford University School of Medicine, 701 Welch Road,

    B-325, Palo Alto, CA 94304, USA

    Stroke is the third leading cause of death and the leading cause of dis-ability in the United States and is associated with a tremendous cost bur-den to society [1]. Most strokes are ischemic, but about 15% of strokesare caused by intracerebral or subarachnoid hemorrhage. Currently, thereis only one drug approved by the US Food and Drug Administration(FDA), intravenous tissue plasminogen activator (tPA), for the treatmentof acute ischemic stroke within 3 hours of symptom onset [2]. Many strokepatients do not receive intravenous tPA, however, most commonly becausethey present beyond the 3-hour therapeutic window. More recently devel-oped therapeutic strategies oer the hope of safe and eective treatmentbeyond the 3-hour time window in selected patients. This article is an up-date of a recent publication that reviewed established and novel treatmentsfor acute ischemic stroke and the management issues that may arise in therst hours to days after symptom onset [3]. Blood pressure management,management of intracranial hypertension, and temperature managementare discussed in greater detail elsewhere in this issue.

    Initial management

    The initial management of acute ischemic stroke involves medical stabi-lization, including airway protection and ventilatory and hemodynamic

    Material for this article is reprinted in part from the American Academy of NeurologyManagement of Acute Ischemic Stroke

    Anna Finley Cauleld, MD*,Christine A.C. Wijman, MD, PhD2006 meeting syllabus titled Critical Care for Cerebrovascular Patients: What General

    Neurologists Need to Know; with permission.

    This is an updated version of an article that originally appeared in Critical Care Clinics,

    volume 22, issue 4.

    * Corresponding author.

    E-mail address: [email protected] (A. Finley Caulfield).

    0733-8619/08/$ - see front matter 2008 Elsevier Inc. All rights reserved.doi:10.1016/j.ncl.2008.03.016 neurologic.theclinics.com

  • s ef-with

    a goal to keep oxygen saturation greater than 95% [4]. If a patient requires

    chemia, increased ICP, pain, or long-standing underlying hypertension [4].e in-

    clude concerns for hemorrhagic transformation of the ischemic infarct

    and worsening cerebral edema. Lowering blood pressure may compromisecerebral blood ow in the area surrounding the infarct, however, resultingTheoretic advantages of treating hypertension in acute ischemic strokendotracheal intubation, short-acting sedatives should be used, and the he-modynamic changes associated with intubation should be minimized[5,9,10]. No prospective trials have been undertaken to establish the idealmode of ventilation in intubated stroke patients. A commonly used modefor patients who are awake but in need of airway protection is pressure sup-port ventilation, whereas synchronized intermittent mandatory ventilationor assist control ventilation is recommended for patients who have intracra-nial hypertension or are comatose [5]. Excessive positive end-expiratorypressures (ie, O10 cm H2O) may be deleterious in patients with elevatedintracranial pressure (ICP) [11,12].

    Mechanically ventilated patients frequently require sedation; however,sedatives may cause hypotension and additional brain injury by lowering ce-rebral perfusion pressure [1315]. Propofol, popular because of its short du-ration of action, has been associated with a propofol infusion syndromewhen used at high doses for prolonged periods. This syndrome originallywas described in pediatric patients, but it also can occur in adults. It presentswith metabolic acidosis, rhabdomyolysis, hypotension, bradyarrhythmias,and death [16]. Frequent discontinuation of sedatives is indicated to monitorcarefully for changes in the patients neurologic status.

    Blood pressure and uid management

    Patients with acute ischemic stroke often have elevated blood pressures inthe rst few days after symptom onset. Elevated blood pressure may occurfor a variety of reasons, including physiologic compensation for cerebral is-altered level of consciousness [8]. Hypoxemia may worsen the injurioufects of cerebral ischemia, and patients must be monitored closelysupport, followed by neurologic assessment, brain imaging, and evaluationof the appropriateness of thrombolytic therapy [4,5].

    Airway and ventilatory support

    Patients with acute stroke are at risk for respiratory failure from aspira-tion and pneumonia [6,7] often in the setting of diculty protecting the air-way and clearing secretions because of facial or bulbar weakness or an

    346 FINLEY CAULFIELD & WIJMANin stroke extension.In normotensive individuals, cerebral blood ow is maintained over

    a wide range of mean arterial pressures (50150 mm Hg) [17,18]. Chronicallyhypertensive patients require a higher range of mean arterial pressures to

  • ce-that

    elevated blood pressures should not be lowered, unless the patient has re-

    ceived thrombolytic treatment; has a hypertensive emergency (aortic dissec-tion, hypertensive encephalopathy, acute renal failure, acute pulmonaryedema, or acute myocardial infarction); or has another contraindicationto elevated blood pressure, such as recent surgery. In the absence of con-trolled clinical trials, the American Stroke Association guidelines recom-mend that antihypertensive agents should be withheld unless the systolicblood pressure is greater than 220 mm Hg or the diastolic blood pressureis greater than 120 mm Hg [20,2225]. If patients have received thrombolytictherapy, the guidelines advocate maintaining systolic blood pressure lessthan or equal to 180 mm Hg and diastolic blood pressure less than or equalto 105 mm Hg [2,2225]. If blood pressure lowering is indicated, it should beinstituted cautiously to avoid hypotension. A variety of intravenous agentsmay be used to lower blood pressures. a- and b-adrenergic blockers (labeta-lol), calcium channel blockers (nicardipine), and angiotensin-converting en-zyme inhibitors (enalaprilat) are preferred in patients with acute strokebecause these agents are less likely to cause cerebral vasodilation and ICPelevation, eects that might be anticipated with sodium nitroprusside orhydralazine [4,5,2630].

    Some patients with acute cerebral ischemia resulting from severe extra-cranial or intracranial vessel stenosis may benet from induced hypertension[31]. Typically, mean arterial pressure is increased 20% to 25% from base-line using intravenous isotonic uids, phenylephrine, dopamine, or norepi-nephrine, while the patients neurologic status and hemodynamic stabilityare monitored closely. The impact of this therapy on stroke outcome isbeing evaluated in ongoing clinical trials.

    In patients with ischemic brain injury, a key therapeutic goal is to max-imize brain perfusion and collateral blood ow to the injured area. It isimportant to assess the patients volume status and correct any dehydra-tion. Because stroke patients may be dehydrated on admission, andmany of them cannot tolerate intake of oral uids, normal saline infusionstypically are started immediately. Hypotonic uids should be avoided be-cause these may contribute to worsening cerebral edema and increasedICP [32].

    Neurologic examination

    Assessing the patient for neurologic decits may be accomplished in anhave long-standing hypertension, blood pressure lowering may result inrebral hypoperfusion and worsening ischemia. It is generally acceptedmaintain normal cerebral blood ow [1921]. Because many stroke patients

    347MANAGEMENT OF ACUTE ISCHEMIC STROKEecient and reproducible manner by using the National Institutes of HealthStroke Scale (NIHSS) [25,33,34]. This is a series of neurologic tests designedto assess the patients level of alertness; comprehension; and motor, sensory,visual, and language function (Table 1) [2].

  • Table 1

    The National Institutes of Health Stroke Scale

    Tested item Title Responses and scores

    1a Level of consciousness 0 Alert1 Drowsy2 Obtunded3 Coma/unresponsive

    1b Orientation questions (two) 0 Answers both correctly1 Answers one correctly2 Answers neither correctly

    1c Response to commands (two) 0 Performs both tasks correctly1 Performs one task correctly2 Performs neither task

    2 Gaze 0 Normal horizontal movements1 Partial gaze palsy2 Complete gaze palsy

    3 Visual elds 0 No visual eld defect1 Partial hemianopsia2 Complete hemianopsia3 Bilateral hemianopsia

    4 Facial movement 0 Normal1 Minor facial weakness2 Partial facial weakness3 Complete unilateral paralysis

    5 Motor function arm 0 No drifta. left 1 Drift before 10 secondsb. right 2 Falls before 10 seconds

    3 No eort against gravity4 No movement

    6 Motor function leg 0 No drifta. left 1 Drift before 5 secondsb. right 2 Falls before 5 seconds

    3 No eort against gravity4 No movement

    7 Ataxia 0 Absent1 Ataxia in one limb2 Ataxia in two limbs

    8 Sensory 0 Normal1 Mild sensory loss2 Severe sensory loss

    9 Language 0 Normal1 Mild aphasia2 Severe aphasia3 Mute or global aphasia

    10 Articulation 0 Normal1 Mild dysarthria2 Severe dysarthria

    11 Extinction or inattention 0 Normal1 Mild (loss 1 sensory modality)2 Severe (loss 2 modalities)

    Adapted from the National Institutes of Neurological Disorders and Stroke (NINDS).

    National Institute of Health Stroke Scale. Available at http://www.ninds.nih.gov/doctors/

    index.htm.

    348 FINLEY CAULFIELD & WIJMAN

  • Diagnostic work-up

    Brain imaging

    CT and MRI can assess rapidly the type of stroke (hemorrhagic versusischemic) and the condition of the cerebral vasculature. Advances in CTand MRI techniques of cerebral perfusion hold the promise of identifyingpatients with salvageable brain tissue who could benet from recanalizationtherapies beyond the 3-hour time window.

    The most widely used and available brain imaging technology is CT. Anoncontrast head CT scan quickly excludes an intracranial hemorrhageand sometimes reveals an occluded artery that appears hyperdense becauseof fresh clot in the vessel lumen (Fig. 1A). The admission CT scan also mayshow early signs of infarction, including swelling of the brain parenchyma(sulcal eacement); hypoattenuation (hypodensity) of the brain paren-chyma; or loss of gray-white matter dierentiation (Fig. 1B) [3537]. Earlysigns of cerebral infarction in the 3-hour time window slightly increase therisk of hemorrhagic transformation after intravenous tPA, but are not con-sidered a contraindication for tPA treatment [38]. A large area of hypoden-sity on the admission CT scan obtained within the 3-hour time window isuncommon, however, and warrants verication of the accuracy of the re-ported time of symptom onset. Because a noncontrast head CT scan mayfail to detect subarachnoid hemorrhage in approximately 10% of cases,a lumbar puncture to assess for the presence of subarachnoid blood is man-datory in patients who present with a clinical history of a sudden severeheadache and a normal brain CT scan [39].

    CT angiography of the head and neck may be used to assess the intracra-nial and cervical circulation for stenoses and occlusions [40]. CT angiogra-phy uses a helical scanner to map out a contrast bolus as it passes throughthe vessels. It requires adequate peripheral intravenous access for injectionof an iodine-based contrast bolus (150170 mL). Although CT angiographyincreases the incidence of renal dysfunction, this risk is relatively small; inone series of patients undergoing cerebral CT angiography and CT perfu-sion, only 4 (0.37%) of 1075 subjects had an increase in creatinine equalto or greater than 0.5 mg/dL [41]. CT angiography may be particularly use-ful in patients who present just outside of the treatment window for intrave-nous thrombolysis, and who may be candidates for intra-arterial clot lysisbecause it can provide valuable information as to the location and extentof the clot. CT angiography also may be useful to assess the head andneck vessels in patients who cannot undergo MRI because of the presenceof pacemakers or other metal objects in the body, claustrophobia, or criticalillness precluding extended periods in a MRI scanner. Perfusion CT assesses

    349MANAGEMENT OF ACUTE ISCHEMIC STROKEcerebral perfusion of the brain by tracking the rst pass of an intravenouslyadministered bolus of contrast material using helical CT scanning [42]. Thistechnique is promising because of its ability to measure absolute cerebral

  • Fig. 1. Nonenhanced brain CT scan obtained approximately 3 hours after sudden onset of left-

    sided weakness. (A) Hyperdense signal (hyperdense middle cerebral artery sign) is present in the

    right middle cerebral artery consistent with a large clot. (B) Subtle early infarct signs with loss of

    gray-white matter dierentiation are seen in the corresponding right middle cerebral artery ter-

    ritory (arrows).

    350 FINLEY CAULFIELD & WIJMANblood ow to help identify the degree of reversibility of brain injury, but it islimited in that not all vascular territories can be imaged completely. Severalstudies have found that perfusion CT may be capable of dierentiating be-tween regions of brain infarction and ischemic penumbra [43]. A completeCT examination including noncontrast CT, CT angiography, and perfusionCT can be performed in approximately 10 minutes [42].

    MRI has better resolution of the brain parenchyma and, in particular,evaluates the brainstem and cerebellum with higher resolution thanCT [44]. MRI diusion-weighted imaging (DWI) detects early cytotoxicedema by measuring the random diusion of water molecules, which is re-stricted almost immediately in ischemic brain injury because of failure ofthe energy-requiring active sodium and water transport mechanism. DWIshows an abnormal signal within minutes of ischemia onset, whereas non-contrast brain CT may take several hours for an infarction to become ap-parent [4547]. Not all brain lesions with restricted diusion are causedby cerebral infarcts. Brain tumors, seizures, brain infections, Creutzfeldt-Jakob disease, and toxic-metabolic disorders sometimes also cause areasof brain injury with restricted diusion on DWI. Magnetic resonance angi-ography evaluates the blood vessels of the brain and neck. When it is usedwithout a contrast agent, magnetic resonance angiography creates vessel im-ages by taking advantage of the ow voids caused by moving blood in themagnetic eld. One of the drawbacks of magnetic resonance angiographyis that it may overestimate the degree of arterial stenosis or give the impres-sion of an arterial occlusion when a complete occlusion may not exist.

  • Contrast-enhanced magnetic resonance angiography is thought to decreasethe likelihood of overestimation of the severity of luminal stenosis [48,49].

    MRI perfusion-weighted imaging (PWI) was developed to measure rela-tive blood ow in the brain. A bolus injection of paramagnetic contrastagent is given and tracked on the rst pass through the brain parenchyma.A variety of parameters may be measured from this injection and displayedon perfusion maps, including bolus arrival time, mean transit time, and rel-ative cerebral blood volume [42,46,50,51]. Perfusion maps may take 5 to40 minutes of postprocessing time. The use of PWI and DWI may identifypatients who would benet from recanalization therapy outside the estab-lished 3-hour time window for intravenous tPA. An example of a patientin the 3- to 6-hour window with a mismatch between a large perfusion decitand a small diusion abnormality and a persistent corresponding vessel oc-clusion is presented in Fig. 2 [52]. The patient received intravenous tPA 3 to

    351MANAGEMENT OF ACUTE ISCHEMIC STROKEFig. 2. MRI of the brain with diusion-weighted imaging (DWI) on the left, perfusion-

    weighted imaging (PWI) in the middle, and magnetic resonance angiography on the right.

    (Top row) MRI obtained approximately 5 hours after acute onset of aphasia and right-sided

    weakness showing a small area of infarction (white) on DWI, a large area of decreased perfusion

    of the left middle cerebral artery brain territory (white) at risk for infarction on PWI, and absent

    ow in the left middle cerebral artery ow on magnetic resonance angiography. (Bottom row)

    MRI obtained 4.5 hours later (after intravenous tissue plasminogen activator [tPA] administra-tion) shows marked improvement in the PWI and reconstitution of ow in the left middle

    cerebral artery. There is a marked improvement in neurologic function (National Institutes

    of Health Stroke Scale [NIHSS] changed from 16 to 5) and no growth of the DWI lesion.

    (Courtesy of Gregory W. Albers, MD, Palo Alto, CA.)

  • blood gas measurements; (2) cardiac biomarkers, including troponin and

    ver-sus 2.1%; P .01). The International Stroke Trial enrolled 19,435 patients

    for randomized treatment with aspirin alone (300 mg/d), subcutaneous hep-arin alone, aspirin and heparin combined, or neither agent within 48 hoursof stroke onset [55]. In the aspirin-only group, there were signicantly fewerrecurrent strokes within the rst 2 weeks (2.8% versus 3.9%) and a trendtoward a reduction of death or dependence at 6 months (61.2% versustality (3.3% versus 3.9%; P .04) and recurrent ischemic stroke (1.6%brain natriuretic peptide; (3) liver function tests and ammonia level (forpatients with an unexplained altered level of consciousness); (4) chestradiograph (for patients with respiratory distress or hypoxia); (5) blood cul-tures (for patients with fever raising a concern for septic emboli); (6) urinetoxicology screen (for patients with possible substance abuse); (7) electroen-cephalogram (for suspected seizures); (8) lumbar puncture (for suspectedmeningitis or subarachnoid hemorrhage); and (9) CT of the cervical spineif neck trauma has occurred or is suspected [4].

    Treatment of acute ischemic stroke

    Antiplatelet therapy in acute ischemic stroke

    For patients who are not eligible for tPA, aspirin is the only antiplateletdrug that has been evaluated in the acute treatment of stroke. The ChineseAcute Stroke Trial enrolled 21,106 patients to receive aspirin, 160 mg/d, orplacebo within 48 hours of stroke onset with continued therapy for 4 weeks[54]. The aspirin-treated group had a small but signicant decrease in mor-6 hours after symptom onset, which resulted in vessel recanalization and res-olution of the PWI decit. The patients neurologic status improved sub-stantially (NIHSS improved from 16 to 5). If the vessel had remainedoccluded, the DWI lesion likely would have grown to the size of the corre-sponding PWI lesion, reducing the chances of clinical improvement.

    Emergent laboratory evaluation and other tests

    In addition to brain imaging, several laboratory tests must be performedexpeditiously to evaluate whether the patient is a candidate for tPA, includ-ing a complete blood count, coagulation parameters, and serum glucose(Box 1) [2,4,22,53]. An electrocardiogram is indicated in all patients withacute stroke to detect myocardial ischemia and cardiac arrhythmias, suchas atrial brillation. Blood urea nitrogen and creatinine levels should bechecked, in particular in patients who will be exposed to iodine-based con-trast agents. In selected patients, one should consider obtaining (1) arterial

    352 FINLEY CAULFIELD & WIJMAN63.5%). Based on the results of these trials, most experts agree that patientsshould be treated within 48 hours of ischemic stroke with aspirin [25,53]. Inpatients who receive tPA, antiplatelet therapy should start 24 hours afterthrombolytic therapy [2,4,22,25,53].

  • Box 1. Characteristics of patients with ischemic stroke whocould be treated with recombinant tissue plasminogen activator

    Diagnosis of ischemic stroke causing measurable neurologicdeficit

    Neurologic signs should not be clearing spontaneouslyNeurologic signs should not be minor and isolatedCaution should be exercised in treating a patient with majordeficits

    Symptoms of stroke should not suggest subarachnoidhemorrhage

    Onset of symptoms less than 3 hours before beginning treatmentNo head trauma or prior stroke in previous 3 monthsNo myocardial infarction in the previous 3 monthsNo gastrointestinal or urinary tract hemorrhage in previous21 days

    No major surgery in the previous 14 daysNo arterial puncture at a noncompressible site in the previous7 days

    No history of previous intracranial hemorrhageBlood pressure not elevated (systolic

  • tPA is a brin-specic thrombolytic agent that activates plasminogen toform plasmin, a protease that cleaves brin. The National Institute of Neu-

    Intravenous thrombolytic therapy beyond the 3-hour time windowrologic Disorders and Stroke (NINDS) acute stroke study group enrolled624 patients presenting within 3 hours of symptom onset in a randomized,double-blind, placebo-controlled, two-part study evaluating the eect of in-travenous tPA (at 75% of the recommended dose for myocardial infarction)for all types of ischemic stroke [2]. The rst part of the study measured earlyresponse to tPA and showed improvement in the NIHSS score by 4 or morepoints at 24 hours after treatment [2,53]. The 3-month functional outcomeevaluation also showed improved neurologic outcomes in the tPA group,which paved the way for verication of these results in the second part ofthe study. The primary end point for part two was a combined 3-month out-come assessment using several rating scales: the NIHSS, Barthel index, mod-ied Rankin scale, and Glasgow outcome scale. All outcome measuresshowed benet in the tPA group with 11% to 13% absolute dierence inneurologic scores in the tPA-treated patients [53]. The symptomatic intra-cranial hemorrhage rate was higher in the tPA group (6.4%) than in the pla-cebo group (0.6%) (P!.001) [2]. Mortality rates at 3 months were similar inboth groups, however, at 17% for the tPA group and 21% for the placebogroup (P .30) [2]. Based on these results, the FDA approved the use ofintravenous tPA within 3 hours from stroke onset at a dose of 0.9 mg/kg,with a maximum dose of 90 mg [2,53,56,57]. Box 1 lists the characteristicsof patients with ischemic stroke who are eligible for treatment with tPA [22].

    Since the approval of intravenous tPA, two prospective, monitored,phase 4 studies have shown similar results [58,59]. These studies were de-signed to assess the safety prole and clinical ecacy of intravenous tPAtherapy for acute ischemic stroke in clinical practice. The Standard Treat-ment with Alteplase to Reverse Stroke study enrolled 389 patients andshowed that 43% of patients treated with intravenous tPA had independentfunctional outcomes (dened as a modied Rankin score of 02) at 1 monthpost treatment [58]. The percentage of symptomatic intracranial hemorrhagewas 3.3%, and mortality was 13% at 1 month. The Canadian Activase forStroke Eectiveness Study enrolled 1132 patients and found that 36% oftPA-treated patients had favorable outcomes at 3 months [59]. The rate ofsymptomatic intracranial hemorrhage was 4.6% and mortality was 21%at 3 months.Intravenous thrombolytic therapy within the 3-hour time window354 FINLEY CAULFIELD & WIJMANThe European Cooperative Acute Stroke Study (ECASS) consisted oftwo trials evaluating the use of intravenous tPA within 6 hours of symptomonset in patients with a moderate-to-severe hemispheric stroke [60,61].ECASS I [60] used 85% of the dose for myocardial infarction (1.1 mg/kg,

  • ased/kg,

    100 mg maximum), which was substantially higher than in the NINDS

    tPA study. In ECASS II, 800 patients were enrolled with a primary end pointof 3-month favorable outcome dened as a modied Rankin score of 0 to1 (asymptomatic or no signicant disability despite symptoms). The tPA-treated group faired slightly better at 3 months than the placebo groupwith a 3.7% higher percentage of patients with favorable outcomes[4,53,60,61].

    The Alteplase Thrombolysis for Acute Noninterventional Therapy in Is-chemic Stroke trial was a randomized, placebo-controlled trial evaluatingthe use of 0.9 mg/kg of intravenous tPA in the 3- to 5-hour treatment win-dow [62]. The study was stopped early when interim analysis revealed a lowlikelihood of benet in the treatment group. Several clinical trials evaluatedintravenous streptokinase for acute stroke in Europe and Australia. TheMulti-center Acute Stroke TrialdItaly and Multi-center Acute StrokeTrialdEurope used a 6-hour time window for intravenous treatment with1.5 million U of streptokinase (100% of myocardial infarction dosage)[63,64]. The Australia Streptokinase Trial used the same dose, but shortenedthe time window to 4 hours [65]. All three trials were stopped early becauseof an unacceptable high number of deaths and symptomatic intracranialhemorrhages in the treatment groups.

    Newer thrombolytic and antiplatelet agents

    Recent studies have evaluated alternative thrombolytic agents, such asancrod (Viprinex), a viper-derived enzyme that cleaves brinogen and pro-motes endogenous release of plasminogen activator from the vessel wall[4,6668]. The phase III Ancrod Study compared intravenous Ancrodwith placebo within 6 hours of stroke symptom onset and found no dier-ence in 3-month functional success dened as survival with a Barthel indexof greater than or equal to 95 (or return to prestroke value) between thetreated group (42%) and the placebo group (42%) [69]. Desmoteplase, a pro-group compared with 7% in the placebo group (P!.001). This increrate of hemorrhage in ECASS I likely is related to the tPA dose (1.1 mgmaximum dose 100 mg), and ECASS II [61] used 75% of the dose formyocardial infarction (0.9 mg/kg, maximum dose 90 mg). In ECASS I,620 patients were enrolled, but 17% had protocol violations mainly becauseof misinterpretations of the admission brain CT scans. After excluding thepatients with protocol violations, modied Rankin scores (asymptomaticor minimal disability) were signicantly better in the tPA group comparedwith the placebo group. Among all patients enrolled in ECASS I, therewas a 20% symptomatic intracranial hemorrhage rate in the treatment

    355MANAGEMENT OF ACUTE ISCHEMIC STROKEtease found in vampire bat saliva, is similar to human plasminogen activa-tor, but in laboratory models works faster and causes a more sustainedvessel recanalization compared with tPA. Based on promising phase II trialresults (DEDAS and DIAS trials), it was evaluated in the DIAS 2 trial in the

  • clot,while passing the catheter through the clot and mechanically disrupting it,

    allows for a lower tPA dose and a decreased risk of systemic hemorrhagiccomplications. A disadvantage of intra-arterial thrombolytic therapy isthe time and expertise required for catheterization, restricting this therapeu-tic modality to medical centers that have interventional neuroradiologistsand critical care services available 24 hours a day.

    Prolyse in Acute Cerebral Thromboembolism (PROACT) was a random-ized clinical trial evaluating the ecacy of intra-arterial prourokinase plusintravenous heparin compared with placebo plus intravenous heparin in pa-tients presenting with middle cerebral artery occlusions less than 6 hours old[78,79]. Mechanical disruption of the clot was not permitted. PROACT I[78] randomized 46 patients and showed that intra-arterial prourokinase in-fusion was associated with superior recanalization rates compared with pla-cebo. The symptomatic intracranial hemorrhage rate was 15.4% in theprourokinase group versus 7.1% in the placebo group. In PROACT II[79], there was a statistically signicant benet with 40% of prourokinase-treated patients having a good 3-month functional outcome (modiedRankin score %2) compared with 25% of the control group. Symptomaticintracranial hemorrhage occurred in 10% of the prourokinase group andDirect administration of intra-arterial thrombolytic agents into the3- to 9-hour time window for acute stroke patients with a presumed penum-bra based on MRI or CT imaging results [70,71]. The preliminary results ofthis trial were presented at the 2007 European Stroke Conference and showno signicant dierence in 3-month clinical outcome between the desmote-plase-treated and the placebo groups [72].

    Glycoprotein IIb/IIIa antagonists also are being evaluated alone(AbESST, SaTIS, SETIS) and in combination with low-dose intravenoustPA (the Clear Stroke Trial) [7376]. The ReoPro Retavase Reperfusionof Stroke Safety StudydImaging Evaluation trial is assessing the use of ab-ciximab alone and in conjunction with escalating doses of reteplase. Prelim-inary results suggest promise for the combination therapy, but not forabciximab alone [77].

    Although several novel pharmacologic agents hold promise for acute is-chemic stroke patients, current care of patients with acute ischemic strokestill emphasizes NINDS- and FDA-dened use of intravenous tPA dosedat 0.9 mg/kg with a maximum dose of 90 mg. The risk of symptomatic in-tracranial hemorrhage is approximately 6% when the NINDS- and FDA-approved guidelines are strictly adhered to (see Box 1).

    Intra-arterial thrombolysis

    356 FINLEY CAULFIELD & WIJMAN2% of the control group (P .063). Because prourokinase is not availablein the United States for clinical use, tPA and urokinase have been usedinstead for intra-arterial thrombolysis with favorable outcomes in selectedpatients [53,78,79].

  • ase-

    nicalMechanical thrombolysis

    Several endovascular devices have been developed in recent years to re-move clots from the cerebral circulation. These devices have been tested inpatients with acute stroke who are ineligible for or who failed intravenoustPA treatment [8185]. The Mechanical Embolus Removal in Cerebral Is-chemia (MERCI) retrieval device has been studied most extensively andwas approved by the FDA for use in acute stroke patients who are inel-ently ongoing and have incorporated the use of endovascular mechadevices.Combined intravenous and intra-arterial thrombolysis

    The combination of intravenous and intra-arterial thrombolysis has beeninvestigated in several pilot studies and may be more eective than eithertherapy alone in patients with acute, very large vessel occlusions. The Na-tional Institutes of Health Interventional Management of Stroke trial I(IMS I) investigated the feasibility and safety of a combined intravenousand intra-arterial approach to recanalization in patients with ischemicstroke and a substantial neurologic decit (NIHSSR10) [80]. The study en-rolled 80 patients, and their outcome was compared with historical intrave-nous tPA controls. The patients received 0.6 mg/kg of intravenous tPA over30 minutes within 3 hours from stroke symptom onset followed by intra-arterial tPA within 5 hours if a vessel occlusion was still present on angiog-raphy. The 3-month mortality rate and the symptomatic intracerebralhemorrhage rate in IMS patients were similar to intravenous tPAtreatedpatients in the NINDS tPA Stroke Trial. IMS subjects showed a nonsignif-icant trend toward better clinical outcomes than historical intravenous tPAcontrols (odds ratio 1.35; 95% condence interval, 0.782.37). The results ofthis study and other pilot studies suggest that a combined intravenous plusintra-arterial approach to recanalization is feasible and safe. Further studiesassessing the ecacy of this combined approach to recanalization are pres-also may be considered for intra-arterial thrombolytic therapy on a cby-case basis [4,53].Intra-arterial thrombolytic therapy for acute stroke is not approved bythe FDA, but may be considered in patients with middle cerebral artery oc-clusions who can be treated within 3 to 6 hours after symptom onset andwho have no (or minimal) signs of infarction on their baseline CT scans[4,53]. Given the high mortality associated with basilar artery and internalcarotid artery bifurcation (carotid T) occlusions, patients with these lesions

    357MANAGEMENT OF ACUTE ISCHEMIC STROKEigible or fail intravenous tPA therapy [85]. The device is deployed just be-yond the clot with release of two nitinol helices and pulled back into theclot with the remainder of the helices deployed (Fig. 3). It is twisted threeto ve times to capture the clot better. A balloon is inated in the internal

  • carotid artery temporarily to prevent forward ow, while the clot is re-coiled into the positioning catheter and out the body. The MERCI devicewas tested in an uncontrolled, nonrandomized trial conducted in twoparts [85]. The trial enrolled 151 patients who had stroke symptom dura-tion of 3 to 8 hours or less than 3 hours with a contraindication for tPA.

    Fig. 3. (A, B) The MERCI retrieval device (Concentric Medical): illustration of the clot re-

    moval process. (Courtesy of Concentric Medical, Inc., Mountain View, CA; with permission.

    All Rights Reserved. 2008.)

    358 FINLEY CAULFIELD & WIJMANPatients also had a substantial neurologic decit (NIHSS R8) and an oc-clusion of a treatable vessel. Partial or complete recanalization wasachieved in 46% of patients on intention-to-treat analysis, and almosthalf (46%) of these had good neurologic outcomes at 90 days (modiedRankin score of 02). Clinically signicant procedural complicationswere reported in 7% of patients. The Multi-MERCI trial tested a newerdevice (L5) and allowed pretreatment with intravenous tPA [86]. Withthe newer device this trial, although not statistically signicant, seemedpromising for better recanalization rates of 68% versus 60% (P .15),lower mortality (35% versus 44%, P .12), and higher favorable out-comes (35% versus 28%, P .19) compared with the MERCI trial[86]. Further studies of the MERCI device are forthcoming in the MR-Rescue and the IMS III trials.

    Primary angioplasty and stenting have been shown to be superior tothrombolytic therapy in patients with acute myocardial infarction. Thismethod is most eective in atherosclerotic arteries that have in situ throm-bus rather than in blood vessels that are occluded by embolic material[81,87]. Many strokes are caused by artery-to-artery embolism or cardi-oembolism, however, and these types of clots tend to rebound into an occlu-sive position despite angioplasty. With further technologic renements,angioplasty and stenting may play a more important role in the manage-ment of acute ischemic stroke in the future [88,89].

  • Neuroprotective strategies

    Many neuroprotective agents that were promising in laboratory modelsof focal ischemia have not shown benet in clinical studies, partly because

    Anticoagulation in acute ischemic strokeof limitations in trial design. Interest in neuroprotective agents for patientswith acute ischemic stroke remains, however, and several phase 3 studies arepresently ongoing. One of the most robust neuroprotective strategies in ex-perimental stroke models is mild-to-moderate hypothermia (2C5C belownormal brain temperature) [9092]. Hypothermia consistently has been as-sociated with a marked reduction in ischemic damage and improved behav-ioral outcomes in these models. The benecial eects seem to be greatestwhen hypothermia is initiated early. The therapeutic window of mild hypo-thermia in patients with acute ischemic stroke is unknown, but likely to belimited to several hours after ischemia onset. The feasibility of hypothermiafor acute ischemic stroke patients has been tested in several clinical pilot tri-als. The Cooling for Acute Ischemic brain Damage study was a phase 2 ran-domized clinical trial using hypothermia in patients less than 12 hours fromstroke onset. There was no signicant clinical benet in 18 patients treatedwith hypothermia compared with 22 patients who received standard medicaltherapy. The study showed, however, that endovascular cooling at 33C wasfeasible and tolerated by most patients [93]. The Intravascular Cooling forthe Treatment of StrokedLonger window trial is presently ongoing. Thisis a multicenter, controlled, randomized trial designed to investigate the fea-sibility and safety of a combination of therapeutic hypothermia with intra-venous tPA in the 0- to 6-hour window in awake stroke patients [94].

    The Stroke-Acute Ischemic NXY-059 Treatment (SAINT) trials were de-signed to evaluate the therapeutic benet of intravenous NXY-059, a nitroneradical trapping agent, administered within 6 hours of stroke onset [95,96].The SAINT I trial enrolled more than 1700 patients with acute ischemicstroke and showed a modest, but statistically signicant (P .038) im-proved outcome in the treatment group as measured by the modied Rankinscale at 90 days; however, the denitive SAINT II trial, which enrolled morethan 3300 patients, did not conrm these results [95,96]. Ongoing phase IIItrials evaluating neuroprotective agents in acute ischemic stroke include theField Administration of Stroke TherapydMagnesium trial assessing thebenet of intravenous magnesium within 2 hours from stroke onset andthe Albumin in Acute Stroke study, a trial of high-dose albumin within5 hours of symptom onset [9799].359MANAGEMENT OF ACUTE ISCHEMIC STROKEThere is no evidence to support urgent anticoagulation to prevent strokerecurrence or extension in patients with acute stroke [25,53,100]. Intrave-nous heparin infused for 7 days was evaluated in a small randomized, con-trolled study with 225 patients with acute ischemic stroke [101]. No

  • study among Asian stroke patients with large artery occlusive disease (intra-

    cranial and extracranial), low-molecular-weight heparin (nadroparin) over-all did not support a signicant benet over aspirin in acute stroke patients[107]. Benets observed in secondary outcome measures, however, may war-rant further study of low-molecular-weight heparins in acute stroke patientsattributed to large artery atherosclerosis.

    Complications of stroke

    Hemorrhagic transformation

    A feared complication of thrombolytic therapy in stroke patients is intra-cranial hemorrhage. Symptomatic intracerebral hemorrhage occurs in ap-proximately 6% of patients receiving intravenous tPA for acute ischemicstroke and has been associated with high morbidity and mortality [2,108].Risk factors for symptomatic intracerebral hemorrhage after thrombolytictherapy include symptom severity, early infarct signs on admission brainCT, older age, elevated systolic blood pressure, low platelet count, elevatedserum glucose, history of diabetes, history of congestive heart failure, longertime to treatment, and low levels of plasminogen activator inhibitor[109120]. The presence of one or more of these risk factors should not beconsidered a contraindication to tPA treatment, however, in a patientwho otherwise qualies based on the NINDS criteria.

    The biologic half-life of tPA at the clot site is approximately 45 minutes,signicant dierence in stroke progression or neurologic outcome was foundbetween the treatment and the control groups. Analysis of the combinedheparin groups from International Stroke Trial showed that a decreased re-current stroke risk at 14 days was oset by an increased risk of intracranialhemorrhage [55]. The low-dose heparin group (5000 U twice a day) had de-creased mortality with only a slight and nonsignicant increase in bleedingrisk. The low-dose heparin in combination with aspirin group had the lowestrate of stroke recurrence and no signicant increase in bleeding risk com-pared with patients on only low-dose heparin. A subgroup analysis of pa-tients who presented with atrial brillation and acute ischemic strokeshowed a signicant reduced risk of recurrent ischemic strokes (4.9% versus2.8%), but the increased risk of intracranial hemorrhage negated any poten-tial benets (2.1% versus 0.4%) at 14 days [53,55].

    Studies evaluating low-molecular-weight heparins in acute ischemicstroke failed to show a benecial eect [102105]. In a subgroup analysisof the TOAST trial, however, better outcomes were observed in patientswith stroke caused by large artery atherosclerosis [103,105,106]. In a recent

    360 FINLEY CAULFIELD & WIJMANand most tPA-related intracranial hemorrhages occur in the rst few hoursafter treatment. If a patient has a signicant neurologic change during intra-venous tPA administration, the infusion should be stopped, and an emer-gent head CT scan should be obtained. Laboratory tests should be

  • in this issue. Because of the concern of compromising cerebral blood ow,tem-

    porizing measure until more denitive therapies can be initiated. Corticoste-

    roid therapy, although eective in decreasing cerebral edema in patientswith brain tumors and brain abscesses, does not improve cerebral edemaassociated with ischemic or hemorrhagic stroke and ought to be avoidedbecause corticosteroids are of no benet and may worsen outcome [132].hyperventilation should be used only in emergency situations and as aperformed immediately, including coagulation parameters, brinogen, andcomplete blood count with platelets. If a symptomatic intracerebral hemor-rhage is diagnosed, emergent infusion of fresh frozen plasma (510 mL/kg)and cryoprecipitate (0.1 bag/kg) is recommended [121].

    Cerebral edema

    Patients with ischemic stroke with cerebral edema and mass eect are atrisk for brain herniation, brainstem compression, coma, and death. Exam-ples are patients with large hemispheric infarctions involving the middle ce-rebral artery territory and patients with large cerebellar infarctions. Masseect caused by ischemic infarcts typically peaks 3 to 5 days after symptomonset. The clinical examination is more sensitive in detecting worsening ce-rebral edema, local tissue shifts, and impending uncal or transtentorial her-niation than continuous ICP monitoring because the clinical deteriorationcaused by regional tissue injury and compression precedes a global increasein ICP in most patients [5,122,123].

    In patients with suspected elevated ICP, initial management should con-sider adequacy of airway, breathing, and circulatory function. The headshould be elevated 30 degrees to decrease ICP and optimize cerebral venousreturn [124,125]. Hyperosmolar therapy should be instituted using mannitol,hypertonic saline, or both [126128]. Mannitol extracts intracellular andinterstitial water from the brain. This agent also is a free radical scavenger,inhibits programmed cell death, and lowers blood viscosity [129]. It is ad-ministered as a 0.5 to 1 g/kg loading dose and can be followed by bolusesof 0.25 g/kg every 6 hours. The main complications associated with manni-tol use are hypovolemia, hypotension, and electrolyte disturbances resultingfrom osmotic diuresis. Hypertonic saline has been proposed as an alterna-tive to mannitol and may be of particular advantage in hypovolemic pa-tients. Rebound edema may occur after abrupt cessation of mannitol orhypertonic saline [128]. Experimental and clinical studies suggest potentialbenets of hypertonic saline over mannitol in the treatment of stroke-relatedbrain edema and increased ICP [130,131]. More details on the treatment ofincreased ICP and the use of hyperosmolar therapy can be found elsewhere

    361MANAGEMENT OF ACUTE ISCHEMIC STROKECraniectomy has been proposed as a lifesaving measure in patients withlarge hemispheric infarction accompanied by mass eect space-occupyingedema (Fig. 4). The goal of surgery is to reverse mass eect and brain tissueshifts, decrease ICP, improve cerebral perfusion, and prevent secondary

  • Fig. 4. Nonenhanced CT scan 3 days after a right middle cerebral artery territory infarction

    that required a hemicraniectomy to decrease tissue shifts and prevent transtentorial herniation

    and death.362 FINLEY CAULFIELD & WIJMANinjury. Several observational studies demonstrated a decrease in mortalityand improved neurologic outcome, in particular in young patients (age!60 years) with hemispheric infarctions who underwent decompressivehemicraniectomy when compared with historic controls [133135]. Basedon these encouraging reports, three randomized controlled trials were un-dertaken in Europe to assess the benecial eect of decompressive surgeryin patients with space-occupying hemispheric strokes. A meta-analysis com-bining data from the three studies was recently published and demonstratedthat decompressive hemicraniectomy reduced mortality and improvedfunctional outcome [136]. A substantial proportion of survivors (40%)had a 12-month modied Rankin scale score of 4, however, leading theauthors to conclude that the decision to perform decompressive surgeryshould be made on an individual basis in every patient [136]. Decompres-sive surgery also may benet patients with large cerebellar infarctions, inparticular patients with hydrocephalus, brainstem compression, and neuro-logic deterioration.

    Deep venous thrombosis

    Deep venous thrombosis and pulmonary embolism are a cause of earlydeath in 5% of stroke patients [137]. Low-dose heparin or low-molecular-weight heparin may be used for prevention of deep venous thrombosis [53].In the PROTECT study, citraparin, a low-molecular-weight heparin, wasfound to be at least as eective as unfractionated heparin (5000 units

  • rapyosis

    prophylaxis in the rst 24 hours [2,4,22,25,53]. Sequential compression

    ningately

    correct elevated blood sugars with short-acting insulin. Further studies are

    needed to investigate the benet of tight blood glucose control on strokeoutcome [144].

    Fever

    Hyperthermia adversely aects stroke outcome in animal models andin observational clinical studies [91,145147]. Proposed mechanisms bywhich hyperthermia may worsen outcome include promotion of an in-ammatory response, an increase in release of excitotoxic amino acids,and an increase in cerebral metabolic demand in an already compromisedcerebral blood ow state [147149]. Pneumonia and urinary tract infec-tions are common in stroke patients and must be worked-up aggressivelyin a febrile patient. Deep venous thrombosis also may cause fevers andshould be considered in patients with unexplained fevers. Further studiesBased on these observations it is recommended to avoid dextrose-contaiintravenous infusions and serially to check blood glucose and adequdevices are indicated in nonambulatory stroke patients who are unableto receive heparin or low-molecular-weight heparin [53].

    Hyperglycemia

    Hyperglycemia has been associated with larger cerebral infarct volumesin animal models [140]. In humans, worsened outcomes have been reportedin patients with elevated admission glucose levels [141]. Hyperglycemia hasalso been associated with increased cerebral edema volumes and higher hem-orrhagic transformation rates with or without intravenous tPA administra-tion [113,142,143]. Stroke patients often have surges in their blood glucoselevels because of the sympathetic stress response in the acute phase [4].the two groups [139]. Patients who have received thrombolytic theshould not receive anticoagulation therapy for deep venous thrombsubcutaneous three times a day) in preventing proximal deep venousthromboembolism, pulmonary embolism, and death related to venousthromboembolism in patients with acute ischemic stroke [138]. Majorbleeding events were similar between the citraparin (1.1%) and the unfrac-tionated heparin (1.8%) treated groups [138]. In the PREVAIL study,enoxaparin signicantly reduced the risk of thromboembolism (relativerisk reduction 43%) compared with unfractionated heparin (5000 unitssubcutaneous twice a day) (P .0001) [139]. Symptomatic intracranialhemorrhage and extracranial major hemorrhages were similar between

    363MANAGEMENT OF ACUTE ISCHEMIC STROKEare needed to evaluate the therapeutic impact of antipyretic agents andcooling therapies in acute stroke. A detailed discussion on temperaturemanagement in patients with neurologic injuries can be found elsewherein this issue.

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    Intravenous tPA should be administered to all patients with acute ische-mic stroke who present within 3 hours of stroke onset and meet the NINDSinclusion and exclusion criteria. The risk of symptomatic intracranial hem-orrhage with intravenous tPA is approximately 6%. Intra-arterial tPA andmechanical thrombectomy are alternative treatment strategies for acutestroke patients who are ineligible for or fail intravenous tPA treatment. Fur-ther studies are needed to assess the benet of these treatments. Patientswith acute ischemic stroke should be maintained euglycemic, euvolemic,and normothermic. Permissive hypertension may be benecial, but in pa-tients receiving tPA blood pressures should be maintained at or less than180/105 mm Hg. Patients with life-threatening cerebral edema from hemi-spheric infarctions require hyperosmolar therapy and may benet fromearly surgical decompression. Novel management strategies under investiga-tion include the use of multimodal imaging to identify patients who mightbenet from tPA beyond the 3-hour time window, new thrombolytic agents,and neuroprotective therapies.

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    Management of Acute Ischemic StrokeInitial managementAirway and ventilatory supportBlood pressure and fluid managementNeurologic examination

    Diagnostic work-upBrain imagingEmergent laboratory evaluation and other tests

    Treatment of acute ischemic strokeAntiplatelet therapy in acute ischemic strokeIntravenous thrombolytic therapy within the 3-hour time windowIntravenous thrombolytic therapy beyond the 3-hour time windowNewer thrombolytic and antiplatelet agentsIntra-arterial thrombolysisCombined intravenous and intra-arterial thrombolysisMechanical thrombolysisNeuroprotective strategiesAnticoagulation in acute ischemic stroke

    Complications of strokeHemorrhagic transformationCerebral edemaDeep venous thrombosisHyperglycemiaFever

    SummaryReferences