Stroke’Update’and’Treatment Improvement · Context • APSS’ • SAP’ •...
Transcript of Stroke’Update’and’Treatment Improvement · Context • APSS’ • SAP’ •...
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Stroke Update and Treatment Improvement
Michael D Hill
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Disclosure Slide • In the last 5 years:
– I have been funded by CIHR, HSF Alberta/NWT/Nunavut, CSN, AHFMR, NINDS (NIH)
– I have received speaker fees/honouraria from Hoffmann-‐La Roche Canada Ltd., Sanofi Canada, Boehringer-‐Ingelheim Canada, Novo-‐Nordisk Canada
– I have been an advisor to NovoNordisk Canada, Genentech Ltd, Stem Cell TherapeuQcs, Vernalis Group Ltd., Sanofi Canada; Portola therapeuQcs
– I hold no stock or direct investment in any pharmaceuQcal or device company (except those possibly in mutual funds)
– I believe you/we should “give the juice” (ie. tPA) far more oZen that we do
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Outline
• QuICR and SCN IntroducQon • Thrombolysis for Acute Stroke • Imaging for Acute Stroke and for TIA/Minor Stroke
• Endovascular and Red Deer’s role
2015-‐09-‐21 3
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Context
• APSS • SAP • QuICR QI objecQves – Door-‐to-‐needle
• Endovascular – TIA/minor stroke
2015-‐09-‐21 4
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2015-‐09-‐21 Calgary Stroke Program 5
Stroke is a clinical syndrome defined by imaging
1. Ischemia: AIS and TIA (85%)
2. Intracerebral hemorrhage (7.5%)
3. Sub-‐arachnoid hemorrhage (7.5%)
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2015-‐09-‐21 Calgary Stroke Program 6
Stroke PresentaQon
• Stroke is SUDDEN (seconds to minutes) • Stroke is usually PAINLESS • Deficits may not be maximal at onset and may progress
• Stroke is the most common cause of sudden focal neurological deficits IN ALL AGE GROUPS (including you!)
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2015-‐09-‐21 Calgary Stroke Program 7
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2015-‐09-‐21 Calgary Stroke Program 8
AIS Diagnosis
• Clinical • CT scan – SensiQve for severe stroke – 20% sensiQve for all stroke – ie. Misses small ischemic lesions
– Takes a trained eye • MRI (DWI) – Highly sensiQve for all ischemic stroke
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1. Principles of Emergency Stroke Treatment
• Speed • Rapid diagnosis – ICH – SAH – AIS – TIA – CVST
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Speed
• System issue – process engineering at all levels from pre-‐hospital, triage, imaging, treatment
• Applies to all stroke types
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EMS Bypass to Stroke Centres
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Human Nature? onsetER= 113.783-.54981Doorndle
Onse
t-to
-do
or
(min
) tim
e
Door-to-needle time (min)0 50 100 150 200
0
30
60
90
120
150
180
210
240
For each 10 minute delay in ER arrival, treatment was 18 minutes faster!
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Diagnosis
1. If they have a deficit when you see them, no maler how slight, it will be a stroke.
2. Examine language/speech, power, sensaQon, vision and co-‐ordinaQon. – SensaQon, vision, co-‐ordinaQon commonly
missed. 3. Imaging – usually CT – Push the paQent to CT. You should have a CT
within 25 minutes of arrival at triage.
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2. Thrombolysis
• Offer thrombolysis to disabled paQents with acute ischemic stroke – No hemorrhage on imaging – Not a wipe out stroke on imaging – Early in the Qme window – You should treat with a door-‐to-‐needle Qme < 60 minutes and ideally faster than that
– No general medical thrombolysis contraindicaQons
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Stroke Clinical Trials: Thrombolysis
• MAST-‐E, MAST-‐I, ASK • ECASS-‐1 • NINDS tPA Stroke Trial • ECASS-‐2 • ATLANTIS • EPITHET • DIAS • ECASS-‐3 • IST-‐3
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Time and outcome [Lees et al. Lancet 2010; 375: 1695–1703]
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0–90 min, n=311; 91–180 min, n=618; 181–270 min, n=801; 270–360 min, n=1046. Values do not equal 100% because of rounding.
The ATLANTIS, ECASS, and NINDS rt-‐PA Study Group InvesQgators. Lancet 2004; 363 (9411): 768-‐774.
Time is an effect modifier
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IV tPA Qme relaQonship Qme is brain [Emberson et al. Lancet 2014]
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• Early treatment with IV tPA reduced death and disability at 90 days
• The lower bound of the confidence interval cross unity at approximately 5 hours
• Speed is a criQcal factor in treatment
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Do: Treat improving stroke…
• 30% of paQents deemed too mild or rapidly improving are disabled or dead at hospital discharge (Barber et al., Neurology)
– DO treat if not completely beler – DO treat if fluctuaQng
• Rule of thumb • Disabled = Can’t walk OR can’t talk OR can’t see OR can’t hold arm up against gravity
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Treat minor stroke? Effect of rt−PA on a good stroke outcome (mRS 0−1) by stroke
severity
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3. Ischemic stroke: Blood pressure
• Treat blood pressure for thrombolysis – tPA in one arm – Labetalol in the other
• For all other ischemic strokes, leave the BP alone – It is elevated because of stroke – It comes down normally in the first 48h – Rapid treatment in the sewng of a blocked artery can worsen ischemia
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Hemorrhage: Blood Pressure
• SAH – treat the blood pressure – Reduced risk of early re-‐bleeding from aneurysm – Once aneurysm is secured, let the BP ride high
• Possible need for induced hypertension later to deal with SAH-‐associated vasospasm
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Endovascular Trials
2015-‐09-‐21 ESCAPE Trial 23
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ICH Pathophysiology Early hematoma expansion
2.0 hours a+er onset 6.5 hours a+er onset
• Continued arterial bleeding • Secondary bleeding into peri-lesional tissue • Peri-lesional edema
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ICH: Treat the BP?
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ICH-‐ADAPT [Butcher et al. Stroke. 2013;44:620-‐626]
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ICH-‐ADAPT [Butcher et al. Stroke. 2013;44:620-‐626]
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Hemorrhage: Blood pressure
• Safe to treat to 140 mmHg systolic • Benefit is modest or nil • Unknown if certain sub-‐groups benefit • Ongoing trials: – ICH-‐ADAPT-‐2 – ATACH
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4. AnQplatelets • NO: Thrombolysis paQents: – No anQplatelets in the first 24h [Danish trial???]
• NO: Hemorrhage paQents • YES: All other ischemia / TIA, give anQplatelets immediately – “2 ASA to chew” – ASA PR for those who cannot safely swallow
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5. DisposiQon
• Thrombolysis paQents à step-‐down unit for 12-‐24h à then to a stroke unit
• SAH paQents à to OR or neuro-‐angio suite for definiQve management of their aneurysm
• ICH paQents à to a stroke unit. 95% do not require Nsx; they require stroke service admission
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DisposiQon
• Ischemic stroke (no thrombolysis) à Stroke unit care
à DVT prevenQon à Swallowing screens and dysphagia management to prevent aspiraQon pneumonia
à Early mobiizaQon and rehabiliaQon therapy à DiagnosQc work-‐up for stroke mechanism and insQtuQon of appropriate secondary prevenQon
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DisposiQon: Management of Minor Stroke and TIA “TIA”
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Kaplan-Meier Life-Table Analysis of Survival Free from Stroke and All Adverse Events after index TIA (JAMA 2000; 284: 2901-6)
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Risk of Stroke, MI, Death aZer TIA – 21.8% at one year
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DisposiQon: Management of Minor Stroke and TIA
1. Make the correct diagnosis. 2. Use imaging tools to help you. 3. Risk straQfy your paQent – ABCD2 does not work (Perry CMAJ) – Risk depends on mechanism • Large artery – caroQds and verts • Atrial fibrillaQon • Lacunar or small vessel
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CT/CTA positive
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Antiplatelets: FASTER
• 2 x 2 factorial design • ASA, ASA + clopidogrel, ASA + simvastatin,
ASA + clopidogrel + simvastatin • 7500 patients • randomise within 12 hours of symptom
onset
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FASTER study [Kennedy et al. Lancet Neurology 2008]
Risk Difference (CI95)
Risk Ratio (CI95)
Clopidogrel v Placebo
-3.8% (-9.4 to 1.9)
0.7 (0.3 to 1.2)
Simvastatin v Placebo
3.3% (-2.3 to 8.9)
1.5 (0.8 to 2.8)
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FASTER study [Kennedy et al. Lancet Neurology 2008]
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CHANCE
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Wang Y, Wang Y, Zhao X, et al; CHANCE InvesQgators. Clopidogrel with aspirin in acute minor stroke or transient ischemic alack. N Engl J Med. 2013;369:11-‐9.
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AnQcoagulate A.fib Immediately?
IST trial • fixed dose sc heparin 15000 U • reduced recurrent stroke slightly in those with afib
HAEST trial • LMWH • ~7% risk of early stroke in both groups
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Quality Improvement
• Early referral to a TIA clinic • Wu C et al – ReducQon in stroke risk at 90d of 50%
• Probably sensible but evidence is lacking? • What intervenQons exactly?
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Speed of RevascularizaQon
Stromberg et al. Stroke May 2012 • 11.5% 0-‐2d • 3.6% 3-‐7d
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Calgary Model
• Diagnose • Image everyone – CT and CTA • Clean CT and CTA
à HOME with outpaQent clinic follow-‐up à ASA + clopidogrel à If a.fib then start anQcoagulaQon immediately (coumadin, NOACs)
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• Abnormal CTA à Intracranial occlusion à TEMPO trial to thrombolyse
à CaroQd atheroscleroQc disease – admit for endarterectomy or medical mgmt of caroQd disease
à Other occlusion – admit and observe
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DOOR-‐TO-‐NEEDLE IMPROVEMENT PROJECT
2015-‐09-‐21 47
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Time lost is Brain lost !
1.9 million neurons lost per minute
Stroke. 2006 Jan;37(1):263-‐6
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Speed malers
For 1000 treated pa7ents, every 15-‐minutes of faster treatment resulted in:
• 18 more paQents with improved ambulaQon at discharge
• 8 more with fully independent ambulaQon
• 7 more discharged home
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Meretoja et al. Neurology 2012; 79: 306-‐313
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Calgary DNT
2015-‐09-‐21 52
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