This document provides guidelines for the acute treatment of stroke based on severity. It defines stroke and classifies severity as TIA, mild, moderate, or severe stroke. Guidelines are given for diagnostic tests, treatment, and management based on stroke type (ischemic vs hemorrhagic) and severity. Treatment includes supportive care, monitoring, diagnostic imaging, thrombolysis if indicated, and rehabilitation. Secondary prevention involves long-term management of risk factors and comorbidities. Appendices provide additional details on differential diagnosis, stroke scales, and specific treatment recommendations.
Management of acute ischemic stroke (2013 ahaKNBadmin
Stroke is the 4th leading cause of death in the US. Less than 50% of stroke patients call 911 within an hour of symptoms and are transported to the most appropriate hospital. Public education on stroke signs is a priority. The document outlines recommendations for stroke diagnosis and treatment including patient positioning, oxygenation, temperature control, blood pressure and sugar management, fibrinolysis with rtPA within 3-4.5 hours, anticoagulation, antiplatelets, and preventing complications. Decompressive surgery is recommended for large hemispheric or cerebellar infarcts to reduce mortality. Thromboprophylaxis is also discussed for traumatic brain injury patients.
This patient presented with acute onset right facial droop and right arm weakness consistent with a transient ischemic attack. However, CT imaging showed a large area of hypodensity involving over one third of the middle cerebral artery territory, making the patient ineligible for IV tPA. The patient's blood pressure was also uncontrolled despite medication, further precluding thrombolysis. For acute stroke management, guidelines recommend maintaining blood pressure below 180/105 mmHg but correcting any hypotension. Starting an IV heparin drip for new atrial fibrillation is not recommended acutely.
Health Policy - Use of IV tPA for Acute Ischemic StrokesZach Jarou
Stroke is a leading cause of death and disability in the US. Treatment with the drug tPA within 3 hours of stroke onset can reverse deficits, but it is underutilized due to its risk of hemorrhage and narrow treatment window. The document argues that public education on stroke symptoms and increasing the treatment window to 4.5 hours based on evidence from trials could increase tPA use and reduce disability, but its risks still require careful patient selection.
Ambulatory blood pressure monitoring (ABPM) involves using a portable device to measure blood pressure at regular intervals over 24 hours. ABPM provides important information about blood pressure patterns that office measurements cannot detect, such as nocturnal hypertension. The diagnosis of hypertension is based on ABPM readings showing average blood pressure above 130/80 mmHg for 24 hours or 135/85 mmHg during the day and 120/70 mmHg at night. ABPM can help identify conditions like white coat hypertension and assess treatment effectiveness better than office readings alone. While costly, ABPM provides valuable clinical information and its use should be expanded.
Management of acute ischemic stroke (2013 ahaKNBadmin
Stroke is the 4th leading cause of death in the US. Less than 50% of stroke patients call 911 within an hour of symptoms and are transported to the most appropriate hospital. Public education on stroke signs is a priority. The document outlines recommendations for stroke diagnosis and treatment including patient positioning, oxygenation, temperature control, blood pressure and sugar management, fibrinolysis with rtPA within 3-4.5 hours, anticoagulation, antiplatelets, and preventing complications. Decompressive surgery is recommended for large hemispheric or cerebellar infarcts to reduce mortality. Thromboprophylaxis is also discussed for traumatic brain injury patients.
This patient presented with acute onset right facial droop and right arm weakness consistent with a transient ischemic attack. However, CT imaging showed a large area of hypodensity involving over one third of the middle cerebral artery territory, making the patient ineligible for IV tPA. The patient's blood pressure was also uncontrolled despite medication, further precluding thrombolysis. For acute stroke management, guidelines recommend maintaining blood pressure below 180/105 mmHg but correcting any hypotension. Starting an IV heparin drip for new atrial fibrillation is not recommended acutely.
Health Policy - Use of IV tPA for Acute Ischemic StrokesZach Jarou
Stroke is a leading cause of death and disability in the US. Treatment with the drug tPA within 3 hours of stroke onset can reverse deficits, but it is underutilized due to its risk of hemorrhage and narrow treatment window. The document argues that public education on stroke symptoms and increasing the treatment window to 4.5 hours based on evidence from trials could increase tPA use and reduce disability, but its risks still require careful patient selection.
Ambulatory blood pressure monitoring (ABPM) involves using a portable device to measure blood pressure at regular intervals over 24 hours. ABPM provides important information about blood pressure patterns that office measurements cannot detect, such as nocturnal hypertension. The diagnosis of hypertension is based on ABPM readings showing average blood pressure above 130/80 mmHg for 24 hours or 135/85 mmHg during the day and 120/70 mmHg at night. ABPM can help identify conditions like white coat hypertension and assess treatment effectiveness better than office readings alone. While costly, ABPM provides valuable clinical information and its use should be expanded.
2015 AHA/ASA Focused Update of the 2013 Guidelines for the Early Management of Patients With Acute Ischemic Stroke Regarding Endovascular Treatment
Stroke. 2015;46:3020-3035.
The Intensive Care Management of Acute Ischemic Stroke Ade Wijaya
The document provides an overview of the intensive care management of acute ischemic stroke. It discusses indications for ICU admission including oxygenation and ventilation, hemodynamic and fluid management, fever control, and other aspects of care such as anemia, hemorrhagic transformation, and cerebral edema monitoring. The goal of treatment is stabilization and prevention of secondary complications after a stroke occurs.
Acute ischemic stroke is an emergency. There are good thrombolytic agents available now. Aspirin or clopidogrel along with statins should be given to all stroke patients. Control of BP and sugar is of paramount importance.
2018 AHA ASA guideline - guidelines for the early management of patients with...Vinh Pham Nguyen
The document provides guidelines for the early management of acute ischemic stroke, covering prehospital stroke management and systems of care, emergency evaluation and treatment, and in-hospital supportive care. It recommends public education on stroke signs and calling 911, designating stroke centers and teams, and using telemedicine to expand access to stroke expertise. The goal is to optimize early management through improved systems and rapid treatment to increase utilization of therapies like IV alteplase and endovascular procedures.
1. The document discusses the management of hypertensive crisis, defining hypertensive emergency as elevated blood pressure with acute target organ damage and hypertensive urgency as elevated blood pressure without organ damage.
2. Treatment of hypertensive emergency requires reducing blood pressure gradually by 25% over 8-12 hours, then another 25% reduction, with the final 50% reduction over 24 hours to avoid complications.
3. Intravenous drugs like sodium nitroprusside and hydralazine are used along with constant monitoring of vital signs and target organs to slowly reduce blood pressure while preventing further organ injury.
1) Preoperative hypertension is common and increases the risk of perioperative complications, however well-controlled hypertension may not need surgery postponement.
2) Isolated systolic hypertension over 180 mmHg and high pulse pressure over 80 mmHg are associated with increased risk and reasonable to postpone surgery.
3) Left ventricular hypertrophy and diastolic dysfunction from long-standing hypertension increase perioperative risk and require careful fluid management during surgery.
This talk covers the most important aspects of treatment of acute ischemic stroke, such as thrombolysis, use of antiplatelets, BP and sugar control and general supportive care.
Acute stroke early recognition and managementwebzforu
1. Stroke is a major health problem in the US, with over 750,000 new strokes each year and stroke being a leading cause of death.
2. Treatments such as IV tPA and intra-arterial therapies are effective if administered within 3-6 hours of stroke onset but currently only 1-3% of stroke patients receive treatment.
3. Reasons for the lack of treatment include patients' inability to recognize stroke symptoms, physicians' reluctance to treat, and lack of organized systems to rapidly diagnose and treat stroke.
This document provides an overview of stroke management. It discusses the general management of ischemic stroke, intracerebral hemorrhage (ICH), and cerebral venous thrombosis (CVT). For ischemic stroke, it outlines pre-hospital management, supportive care including blood pressure and glucose control, IV thrombolysis, mechanical thrombectomy, and antiplatelet/anticoagulant treatment. For ICH, it discusses supportive care, blood pressure control, complications management, surgical treatment, and recurrence prevention. For CVT, it notes anticoagulation is the mainstay of treatment.
The following powerpoint presentation is about the current AF guidelines, prepared by Dr Jawad Siraj, who is a final year resident as Cardiology Unit, PGMI, LRH, Peshawar
Anaesthesia for endovascular treatment in acute ischemic stroke - Mads Rasmus...scanFOAM
A talk by Mads Rasmussen at the 2017 meeting of the Scandinavian Society of Anaestesiology and Intensive Care Medicine.
All available content from SSAI2017: https://scanfoam.org/ssai2017/
Content delivered in collaboration between scanFOAM, SSAI & SFAI.
The guidelines provide recommendations for the secondary prevention of stroke in patients with previous ischemic stroke or transient ischemic attack (TIA). Key recommendations include: aggressively treating hypertension, diabetes, dyslipidemia and other vascular risk factors; initiating antiplatelet therapy; and considering carotid endarterectomy for severe carotid stenosis. Lifestyle modifications such as smoking cessation, weight control, diet and exercise are also encouraged. The guidelines were updated from 1999 based on new clinical trial evidence.
This document discusses best practices for early management of acute ischemic stroke cases at Apollo Hospitals in Hyderabad, India. It outlines a multidisciplinary approach involving a dedicated stroke team that works to ensure patients receive rapid diagnosis, treatment, and rehabilitation according to established guidelines and timelines. The goals are to complete initial evaluations within set time periods and provide organized care through protocols, algorithms, and a stroke activation system to minimize mortality and disability from stroke.
Stroke is a leading cause of death and disability. All doctors should have a basic knowledge about stroke management. This presentation gives a summary of treatment options in acute brain stroke.
ACEP Clinical Policy
Critical Issues in the Evaluation and Management of Adult Patients Presenting to the Emergency Department With Seizures
Ann Emerg Med. 2014;63:437-447.
Management of hypertension in acute strokeSudhir Kumar
Hypertension is an important and common risk factor for brain stroke- both ischemia and hemorrhagic subtypes. Appropriate management of blood pressure is crucial for good recovery rom acute stroke, and prevent recurrence of stroke. This presentation looks at the role played by hypertension in causing first ever and recurrent strokes. The current guidelines are also discussed.
Perioperative Care of the Cardiac Surgery Patient
This document outlines key aspects of perioperative care for cardiac surgery patients, including:
1) Preoperative evaluation to assess risk factors and optimize medical conditions;
2) Intraoperative management focusing on organ protection and hemodynamic optimization;
3) Postoperative care in the ICU addressing common complications like arrhythmias, bleeding, and pulmonary issues.
The document summarizes the 2020 ESC Guidelines for the management of acute coronary syndromes in patients presenting without persistent ST-segment elevation. Key recommendations include:
- Using the ESC 0h/2h algorithm with blood sampling at 0h and 2h if an hs-cTn test with a validated 0h/2h algorithm is available.
- Considering measuring BNP or NT-proBNP for prognostic information.
- Considering prasugrel in preference to ticagrelor for NSTE-ACS patients proceeding to PCI.
- Recommending an early invasive strategy within 24h for high-risk patients based on factors like diagnosis of NSTEMI or GRACE risk score >140.
This document defines hypertensive crises and differentiates between hypertensive urgency and emergency. It describes the signs, symptoms, and treatment for each. For the clinical vignette, the diagnosis is hypertensive emergency based on retinal findings of end-organ damage. The next step in management is intravenous antihypertensive medication to reduce blood pressure by 25% over 2-6 hours in the intensive care unit, followed by oral antihypertensives and close follow-up.
Management of Heart Failure in the ED Setting:
An Evidence-Based Review of the Literature
J Emerg Med, 2018 Sep 26.
doi: 10.1016/j.jemermed.2018.08.002
This document discusses risk factors and management of various types of stroke. It identifies several risk factors for stroke including age over 50, hypertension, diabetes, hyperlipidemia, smoking, and atrial fibrillation. Primary prevention strategies include controlling hypertension and diabetes, smoking cessation, and anticoagulation for atrial fibrillation. Acute ischemic stroke is initially evaluated with CT head to rule out hemorrhage, and may be treated with thrombolytics if indicated. Secondary prevention involves lifestyle modifications and long-term antithrombotic therapy.
2015 AHA/ASA Focused Update of the 2013 Guidelines for the Early Management of Patients With Acute Ischemic Stroke Regarding Endovascular Treatment
Stroke. 2015;46:3020-3035.
The Intensive Care Management of Acute Ischemic Stroke Ade Wijaya
The document provides an overview of the intensive care management of acute ischemic stroke. It discusses indications for ICU admission including oxygenation and ventilation, hemodynamic and fluid management, fever control, and other aspects of care such as anemia, hemorrhagic transformation, and cerebral edema monitoring. The goal of treatment is stabilization and prevention of secondary complications after a stroke occurs.
Acute ischemic stroke is an emergency. There are good thrombolytic agents available now. Aspirin or clopidogrel along with statins should be given to all stroke patients. Control of BP and sugar is of paramount importance.
2018 AHA ASA guideline - guidelines for the early management of patients with...Vinh Pham Nguyen
The document provides guidelines for the early management of acute ischemic stroke, covering prehospital stroke management and systems of care, emergency evaluation and treatment, and in-hospital supportive care. It recommends public education on stroke signs and calling 911, designating stroke centers and teams, and using telemedicine to expand access to stroke expertise. The goal is to optimize early management through improved systems and rapid treatment to increase utilization of therapies like IV alteplase and endovascular procedures.
1. The document discusses the management of hypertensive crisis, defining hypertensive emergency as elevated blood pressure with acute target organ damage and hypertensive urgency as elevated blood pressure without organ damage.
2. Treatment of hypertensive emergency requires reducing blood pressure gradually by 25% over 8-12 hours, then another 25% reduction, with the final 50% reduction over 24 hours to avoid complications.
3. Intravenous drugs like sodium nitroprusside and hydralazine are used along with constant monitoring of vital signs and target organs to slowly reduce blood pressure while preventing further organ injury.
1) Preoperative hypertension is common and increases the risk of perioperative complications, however well-controlled hypertension may not need surgery postponement.
2) Isolated systolic hypertension over 180 mmHg and high pulse pressure over 80 mmHg are associated with increased risk and reasonable to postpone surgery.
3) Left ventricular hypertrophy and diastolic dysfunction from long-standing hypertension increase perioperative risk and require careful fluid management during surgery.
This talk covers the most important aspects of treatment of acute ischemic stroke, such as thrombolysis, use of antiplatelets, BP and sugar control and general supportive care.
Acute stroke early recognition and managementwebzforu
1. Stroke is a major health problem in the US, with over 750,000 new strokes each year and stroke being a leading cause of death.
2. Treatments such as IV tPA and intra-arterial therapies are effective if administered within 3-6 hours of stroke onset but currently only 1-3% of stroke patients receive treatment.
3. Reasons for the lack of treatment include patients' inability to recognize stroke symptoms, physicians' reluctance to treat, and lack of organized systems to rapidly diagnose and treat stroke.
This document provides an overview of stroke management. It discusses the general management of ischemic stroke, intracerebral hemorrhage (ICH), and cerebral venous thrombosis (CVT). For ischemic stroke, it outlines pre-hospital management, supportive care including blood pressure and glucose control, IV thrombolysis, mechanical thrombectomy, and antiplatelet/anticoagulant treatment. For ICH, it discusses supportive care, blood pressure control, complications management, surgical treatment, and recurrence prevention. For CVT, it notes anticoagulation is the mainstay of treatment.
The following powerpoint presentation is about the current AF guidelines, prepared by Dr Jawad Siraj, who is a final year resident as Cardiology Unit, PGMI, LRH, Peshawar
Anaesthesia for endovascular treatment in acute ischemic stroke - Mads Rasmus...scanFOAM
A talk by Mads Rasmussen at the 2017 meeting of the Scandinavian Society of Anaestesiology and Intensive Care Medicine.
All available content from SSAI2017: https://scanfoam.org/ssai2017/
Content delivered in collaboration between scanFOAM, SSAI & SFAI.
The guidelines provide recommendations for the secondary prevention of stroke in patients with previous ischemic stroke or transient ischemic attack (TIA). Key recommendations include: aggressively treating hypertension, diabetes, dyslipidemia and other vascular risk factors; initiating antiplatelet therapy; and considering carotid endarterectomy for severe carotid stenosis. Lifestyle modifications such as smoking cessation, weight control, diet and exercise are also encouraged. The guidelines were updated from 1999 based on new clinical trial evidence.
This document discusses best practices for early management of acute ischemic stroke cases at Apollo Hospitals in Hyderabad, India. It outlines a multidisciplinary approach involving a dedicated stroke team that works to ensure patients receive rapid diagnosis, treatment, and rehabilitation according to established guidelines and timelines. The goals are to complete initial evaluations within set time periods and provide organized care through protocols, algorithms, and a stroke activation system to minimize mortality and disability from stroke.
Stroke is a leading cause of death and disability. All doctors should have a basic knowledge about stroke management. This presentation gives a summary of treatment options in acute brain stroke.
ACEP Clinical Policy
Critical Issues in the Evaluation and Management of Adult Patients Presenting to the Emergency Department With Seizures
Ann Emerg Med. 2014;63:437-447.
Management of hypertension in acute strokeSudhir Kumar
Hypertension is an important and common risk factor for brain stroke- both ischemia and hemorrhagic subtypes. Appropriate management of blood pressure is crucial for good recovery rom acute stroke, and prevent recurrence of stroke. This presentation looks at the role played by hypertension in causing first ever and recurrent strokes. The current guidelines are also discussed.
Perioperative Care of the Cardiac Surgery Patient
This document outlines key aspects of perioperative care for cardiac surgery patients, including:
1) Preoperative evaluation to assess risk factors and optimize medical conditions;
2) Intraoperative management focusing on organ protection and hemodynamic optimization;
3) Postoperative care in the ICU addressing common complications like arrhythmias, bleeding, and pulmonary issues.
The document summarizes the 2020 ESC Guidelines for the management of acute coronary syndromes in patients presenting without persistent ST-segment elevation. Key recommendations include:
- Using the ESC 0h/2h algorithm with blood sampling at 0h and 2h if an hs-cTn test with a validated 0h/2h algorithm is available.
- Considering measuring BNP or NT-proBNP for prognostic information.
- Considering prasugrel in preference to ticagrelor for NSTE-ACS patients proceeding to PCI.
- Recommending an early invasive strategy within 24h for high-risk patients based on factors like diagnosis of NSTEMI or GRACE risk score >140.
This document defines hypertensive crises and differentiates between hypertensive urgency and emergency. It describes the signs, symptoms, and treatment for each. For the clinical vignette, the diagnosis is hypertensive emergency based on retinal findings of end-organ damage. The next step in management is intravenous antihypertensive medication to reduce blood pressure by 25% over 2-6 hours in the intensive care unit, followed by oral antihypertensives and close follow-up.
Management of Heart Failure in the ED Setting:
An Evidence-Based Review of the Literature
J Emerg Med, 2018 Sep 26.
doi: 10.1016/j.jemermed.2018.08.002
This document discusses risk factors and management of various types of stroke. It identifies several risk factors for stroke including age over 50, hypertension, diabetes, hyperlipidemia, smoking, and atrial fibrillation. Primary prevention strategies include controlling hypertension and diabetes, smoking cessation, and anticoagulation for atrial fibrillation. Acute ischemic stroke is initially evaluated with CT head to rule out hemorrhage, and may be treated with thrombolytics if indicated. Secondary prevention involves lifestyle modifications and long-term antithrombotic therapy.
Acute coronary syndrome in emergency departmentrigomontejo
This document discusses acute coronary syndrome, including unstable angina, NSTEMI, and STEMI. It outlines the risk factors, symptoms, diagnosis, and management of these conditions. For STEMI specifically, it describes evaluating patients for fibrinolysis or PCI based on time of presentation, contraindications, and cardiac status. Key treatments discussed include aspirin, oxygen, nitrates, beta blockers, ACE inhibitors, and anti-platelet medications to reduce mortality and complications from myocardial infarction.
1) The document discusses the management of patients with cerebrovascular disorders such as stroke, which is a leading cause of death and long-term disability in the US.
2) It covers the prevention, types, pathophysiology, manifestations, and medical management of ischemic and hemorrhagic strokes.
3) Nursing interventions are aimed at improving mobility, self-care, communication and preventing complications during recovery from stroke.
The document provides 11 cognitive aids developed by the Society for Neuroscience in Anesthesia and Critical Care to assist anesthesia teams facing neuroanesthetic emergencies. Each cognitive aid outlines the differential diagnosis, treatment steps to stabilize the patient, and treatment guidance for common neurosurgical emergencies including acute stroke, aneurysm rupture, intraoperative aneurysm rupture, autonomic hyperreflexia, bleeding during spine surgery, and delayed emergence after craniotomy. The cognitive aids are not protocols but are meant to provide resources during emergent situations.
Hypertensive crisis refers to severely elevated blood pressure that can lead to organ damage and is categorized as hypertensive urgency or emergency depending on the presence of end-organ damage; treatment of urgency involves gradual oral medication while emergency requires immediate intravenous drugs to reduce blood pressure to prevent further damage; careful diagnosis and monitoring of blood pressure and organs is needed along with selecting appropriate drugs based on the situation.
This document discusses hypertensive crises, including definitions, epidemiology, pathophysiology, assessment, diagnosis, and management. It defines hypertensive emergencies as elevated blood pressure with acute end-organ damage, while hypertensive urgencies involve impending end-organ damage. The typical patient presenting with crisis is middle-aged, noncompliant with medications, and may use substances. Treatment of emergencies requires immediate blood pressure reduction in the ICU to prevent further damage, while urgencies can be treated gradually as uncontrolled hypertension. Nitroprusside is very effective but has limitations like toxicity risks with prolonged use.
The document discusses acute coronary syndrome (ACS), which includes STEMI, NSTEMI, and unstable angina representing varying degrees of coronary artery occlusion. A 12-lead ECG within 10 minutes of arrival is central to diagnosis and risk stratification. STEMI shows ST elevation and elevated enzymes, while NSTEMI shows ST depression/T-wave inversion and elevated enzymes. The primary goals are early reperfusion for STEMI patients via fibrinolysis within 30 minutes or PCI within 90 minutes. Treatment involves oxygen, aspirin, nitroglycerin, morphine and reperfusion therapies like fibrinolytics or PCI, with important timelines to maximize outcomes for ACS patients.
During atrial fibrillation, the heart's upper chambers — called the atria — beat chaotically and irregularly. They beat out of sync with the lower heart chambers, called the ventricles. For many people, AFib may have no symptoms. But AFib may cause a fast, pounding heartbeat, shortness of breath or light-headedness.
Cardioversion is a procedure that uses electric shock or drugs to convert an abnormal heart rhythm back to normal. There are two main types - electrical cardioversion, which delivers a synchronized electric shock, and pharmacological cardioversion, which uses antiarrhythmic drugs. Electrical cardioversion can be elective or emergency, while pharmacological cardioversion utilizes various classes of drugs like beta blockers, sodium channel blockers, and calcium channel blockers to restore normal rhythm. The document outlines the differences between cardioversion and defibrillation, indications and contraindications for cardioversion, recommendations, procedure steps, complications, and drug options for pharmacological cardioversion.
This document discusses hypertension and hypertensive emergencies. It begins with an introduction to hypertension, defining it as elevated blood pressure on 3 or more occasions. It notes the high prevalence of hypertension in Malawi.
It then discusses factors that influence the consequences of blood pressure levels, including age, race, glucose levels, and smoking. It also lists potential secondary causes of hypertension like renal disease.
The document goes on to define categories of hypertension from mild to malignant based on blood pressure levels. It distinguishes between hypertensive emergencies, where immediate treatment is needed to prevent end organ damage, hypertensive urgencies with slightly lower blood pressures, and chronic hypertension without symptoms. It provides guidelines for evaluating
Ischaemic stroke is caused by blockage of arteries in the brain and accounts for 87% of all strokes. The main types are thrombosis, embolism, and hypoperfusion. Risk factors include atherosclerosis, small vessel disease, and cardiogenic embolism from conditions like atrial fibrillation. Symptoms depend on the affected brain region and may include weakness, sensory loss, speech problems, and visual issues. Treatment involves stabilizing vital functions, managing blood pressure and glucose, and administering thrombolysis within 4.5 hours or revascularization procedures for selected patients to restore blood flow. Secondary prevention focuses on controlling risk factors and long-term anticoagulation or antiplatelet therapy.
This document discusses the management of peri-arrest arrhythmias. It defines arrhythmias and describes their assessment and general treatment options. It covers the management of specific arrhythmias like bradycardia and tachycardias. It also discusses the pharmacology of common antiarrhythmic drugs like amiodarone, atropine, digoxin. The document provides guidelines on stabilizing patients and restoring normal heart rhythm in peri-arrest settings.
PHARMACOTHERAPY POINTERS FOR ISCHEMIC STROKE [MALAYSIAN CPGs].pdfsamthamby79
The document provides guidelines for the pharmacotherapy of ischemic stroke. It discusses the causes, signs and symptoms, and risk factors for ischemic stroke. It also outlines the management of acute ischemic stroke, including indications for intravenous thrombolysis with rt-PA and intra-arterial thrombolysis. The CHA2DS2-VASc and HAS-BLED scores for assessing stroke and bleeding risk in atrial fibrillation are also covered. The document provides detailed guidance on anticoagulation therapy for stroke prevention, including warfarin dosing, monitoring, and management.
This document outlines recommendations from a symposium on stroke management organized by the European Federation of Neurological Societies. It covers recommendations for organizing stroke care, risk factors and primary prevention, acute stroke care including general therapy, specific therapies, rehabilitation, and secondary prevention. Key recommendations include treating patients in specialized stroke units, initiating thrombolysis within 3 hours of onset for ischemic stroke, and controlling risk factors like hypertension, diabetes, hypercholesterolemia and smoking to prevent primary strokes.
The document discusses the approach to anesthesia for patients with cardiac disease undergoing non-cardiac surgery. It emphasizes the importance of preoperative evaluation and risk stratification to determine the safest anesthetic plan. During surgery, careful monitoring is recommended to detect any deterioration in cardiac function. The appropriate selection of anesthetic drugs and techniques can help minimize stress on the heart. Overall, the key is choosing an anesthetic that provides stability for the patient's cardiac condition.
Acute coronary syndrome (ACS) refers to conditions caused by reduced blood flow in the coronary arteries. This can be due to plaque buildup narrowing the arteries or plaque rupture leading to clot formation. ACS includes ST-elevation myocardial infarction (STEMI), non-ST-elevation myocardial infarction (NSTEMI), and unstable angina (UA). Patients present with chest pain and may have ECG changes or elevated cardiac biomarkers. Treatment involves oxygen, nitroglycerin, aspirin, and morphine (MONA) along with long-term therapies like antiplatelets, beta-blockers, statins, and ACE inhibitors to prevent future events.
Temple of Asclepius in Thrace. Excavation resultsKrassimira Luka
The temple and the sanctuary around were dedicated to Asklepios Zmidrenus. This name has been known since 1875 when an inscription dedicated to him was discovered in Rome. The inscription is dated in 227 AD and was left by soldiers originating from the city of Philippopolis (modern Plovdiv).
Communicating effectively and consistently with students can help them feel at ease during their learning experience and provide the instructor with a communication trail to track the course's progress. This workshop will take you through constructing an engaging course container to facilitate effective communication.
Strategies for Effective Upskilling is a presentation by Chinwendu Peace in a Your Skill Boost Masterclass organisation by the Excellence Foundation for South Sudan on 08th and 09th June 2024 from 1 PM to 3 PM on each day.
How to Setup Warehouse & Location in Odoo 17 InventoryCeline George
In this slide, we'll explore how to set up warehouses and locations in Odoo 17 Inventory. This will help us manage our stock effectively, track inventory levels, and streamline warehouse operations.
Beyond Degrees - Empowering the Workforce in the Context of Skills-First.pptxEduSkills OECD
Iván Bornacelly, Policy Analyst at the OECD Centre for Skills, OECD, presents at the webinar 'Tackling job market gaps with a skills-first approach' on 12 June 2024
Philippine Edukasyong Pantahanan at Pangkabuhayan (EPP) CurriculumMJDuyan
(𝐓𝐋𝐄 𝟏𝟎𝟎) (𝐋𝐞𝐬𝐬𝐨𝐧 𝟏)-𝐏𝐫𝐞𝐥𝐢𝐦𝐬
𝐃𝐢𝐬𝐜𝐮𝐬𝐬 𝐭𝐡𝐞 𝐄𝐏𝐏 𝐂𝐮𝐫𝐫𝐢𝐜𝐮𝐥𝐮𝐦 𝐢𝐧 𝐭𝐡𝐞 𝐏𝐡𝐢𝐥𝐢𝐩𝐩𝐢𝐧𝐞𝐬:
- Understand the goals and objectives of the Edukasyong Pantahanan at Pangkabuhayan (EPP) curriculum, recognizing its importance in fostering practical life skills and values among students. Students will also be able to identify the key components and subjects covered, such as agriculture, home economics, industrial arts, and information and communication technology.
𝐄𝐱𝐩𝐥𝐚𝐢𝐧 𝐭𝐡𝐞 𝐍𝐚𝐭𝐮𝐫𝐞 𝐚𝐧𝐝 𝐒𝐜𝐨𝐩𝐞 𝐨𝐟 𝐚𝐧 𝐄𝐧𝐭𝐫𝐞𝐩𝐫𝐞𝐧𝐞𝐮𝐫:
-Define entrepreneurship, distinguishing it from general business activities by emphasizing its focus on innovation, risk-taking, and value creation. Students will describe the characteristics and traits of successful entrepreneurs, including their roles and responsibilities, and discuss the broader economic and social impacts of entrepreneurial activities on both local and global scales.
Walmart Business+ and Spark Good for Nonprofits.pdfTechSoup
"Learn about all the ways Walmart supports nonprofit organizations.
You will hear from Liz Willett, the Head of Nonprofits, and hear about what Walmart is doing to help nonprofits, including Walmart Business and Spark Good. Walmart Business+ is a new offer for nonprofits that offers discounts and also streamlines nonprofits order and expense tracking, saving time and money.
The webinar may also give some examples on how nonprofits can best leverage Walmart Business+.
The event will cover the following::
Walmart Business + (https://business.walmart.com/plus) is a new shopping experience for nonprofits, schools, and local business customers that connects an exclusive online shopping experience to stores. Benefits include free delivery and shipping, a 'Spend Analytics” feature, special discounts, deals and tax-exempt shopping.
Special TechSoup offer for a free 180 days membership, and up to $150 in discounts on eligible orders.
Spark Good (walmart.com/sparkgood) is a charitable platform that enables nonprofits to receive donations directly from customers and associates.
Answers about how you can do more with Walmart!"
LAND USE LAND COVER AND NDVI OF MIRZAPUR DISTRICT, UPRAHUL
This Dissertation explores the particular circumstances of Mirzapur, a region located in the
core of India. Mirzapur, with its varied terrains and abundant biodiversity, offers an optimal
environment for investigating the changes in vegetation cover dynamics. Our study utilizes
advanced technologies such as GIS (Geographic Information Systems) and Remote sensing to
analyze the transformations that have taken place over the course of a decade.
The complex relationship between human activities and the environment has been the focus
of extensive research and worry. As the global community grapples with swift urbanization,
population expansion, and economic progress, the effects on natural ecosystems are becoming
more evident. A crucial element of this impact is the alteration of vegetation cover, which plays a
significant role in maintaining the ecological equilibrium of our planet.Land serves as the foundation for all human activities and provides the necessary materials for
these activities. As the most crucial natural resource, its utilization by humans results in different
'Land uses,' which are determined by both human activities and the physical characteristics of the
land.
The utilization of land is impacted by human needs and environmental factors. In countries
like India, rapid population growth and the emphasis on extensive resource exploitation can lead
to significant land degradation, adversely affecting the region's land cover.
Therefore, human intervention has significantly influenced land use patterns over many
centuries, evolving its structure over time and space. In the present era, these changes have
accelerated due to factors such as agriculture and urbanization. Information regarding land use and
cover is essential for various planning and management tasks related to the Earth's surface,
providing crucial environmental data for scientific, resource management, policy purposes, and
diverse human activities.
Accurate understanding of land use and cover is imperative for the development planning
of any area. Consequently, a wide range of professionals, including earth system scientists, land
and water managers, and urban planners, are interested in obtaining data on land use and cover
changes, conversion trends, and other related patterns. The spatial dimensions of land use and
cover support policymakers and scientists in making well-informed decisions, as alterations in
these patterns indicate shifts in economic and social conditions. Monitoring such changes with the
help of Advanced technologies like Remote Sensing and Geographic Information Systems is
crucial for coordinated efforts across different administrative levels. Advanced technologies like
Remote Sensing and Geographic Information Systems
9
Changes in vegetation cover refer to variations in the distribution, composition, and overall
structure of plant communities across different temporal and spatial scales. These changes can
occur natural.
ISO/IEC 27001, ISO/IEC 42001, and GDPR: Best Practices for Implementation and...PECB
Denis is a dynamic and results-driven Chief Information Officer (CIO) with a distinguished career spanning information systems analysis and technical project management. With a proven track record of spearheading the design and delivery of cutting-edge Information Management solutions, he has consistently elevated business operations, streamlined reporting functions, and maximized process efficiency.
Certified as an ISO/IEC 27001: Information Security Management Systems (ISMS) Lead Implementer, Data Protection Officer, and Cyber Risks Analyst, Denis brings a heightened focus on data security, privacy, and cyber resilience to every endeavor.
His expertise extends across a diverse spectrum of reporting, database, and web development applications, underpinned by an exceptional grasp of data storage and virtualization technologies. His proficiency in application testing, database administration, and data cleansing ensures seamless execution of complex projects.
What sets Denis apart is his comprehensive understanding of Business and Systems Analysis technologies, honed through involvement in all phases of the Software Development Lifecycle (SDLC). From meticulous requirements gathering to precise analysis, innovative design, rigorous development, thorough testing, and successful implementation, he has consistently delivered exceptional results.
Throughout his career, he has taken on multifaceted roles, from leading technical project management teams to owning solutions that drive operational excellence. His conscientious and proactive approach is unwavering, whether he is working independently or collaboratively within a team. His ability to connect with colleagues on a personal level underscores his commitment to fostering a harmonious and productive workplace environment.
Date: May 29, 2024
Tags: Information Security, ISO/IEC 27001, ISO/IEC 42001, Artificial Intelligence, GDPR
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2. ACUTE STROKE TREATMENT
Definition of “stroke”
Sudden onset of focal neurological deficit lasting more than 24 hours due to an
underlying vascular pathology
Table 8: Definition of stroke severity
TIA and MILD STROKE MODERATE STROKE SEVERE STROKE
TIA: Deficits resolve within
24 hours but usually lasts
less than 1 hour without
evidence of acute infarction
on neuroimaging
or
Alert patients with any of
the following:
Mild pure motor weakness
of one side of the body,
defined as: can raise
arm above shoulder,
has clumsy hand, or
can ambulate without
assistance
Pure sensory deficit
Slurred but intelligible
speech
Vertigo with
incoordination (e.g.,
gait disturbance,
unsteadiness or clumsy
hand)
Visual field defects alone
Combination of (a) and (b)
Awake patient with
significant motor and/or
sensory and/or language
and/or visual deficit
or
Disoriented, drowsy or
stuporous patient, but with
purposeful response to
painful stimuli
Comatose patient with non-
purposeful response,
decorticate, or decerebrate
posturing to painful stimuli
or
Comatose patient with no
response to painful stimuli
See Guidelines for TIA
and Mild Stroke
See Guidelines for
Moderate Stroke
See Guidelines for Severe
Stroke
3. GUIDELINES FOR TIA AND MILD STROKE
Management
Priorities
Ascertain clinical diagnosis of stroke or TIA (history and physical exam are
very important)
• Exclude common stroke mimickers (Appendix I)
Provide basic emergent supportive care (ABCs of resuscitation)
Monitor neuro-vital signs, BP, MAP, RR, temperature, pupils
Perform stroke scales (NIHSS, GCS) (Appendix II)
Monitor and manage BP; treat if SBP>220 or DBP>120 or MAP>130
(Appendix III).
Precautions:
• Avoid precipitous drop in BP (BP not >20% of baseline MAP)
(Appendix III). Do not use rapid-acting sublingual agents; when
needed, use easily titratable IV or oral antihypertensive medication
• Ensure appropriate hydration. If IVF is needed, use 0.9% NaCl
Emergent
Diagnostics
• Complete blood count (CBC)
• Blood sugar (CBG, HGT or
RBS)
• Electrocardiogram (ECG)
• PT/PTT
• Plain CT scan of the brain as
soon as possible; computation
of hematoma volume
(Appendix IV)
IschemicEarly
Specific
Treatment
Non-cardioembolic
(Thrombotic, Lacunar)
Cardioembolic
(Appendix V)
Hemorrhagic
4. CT Scan
Confirmed
(Appendix V)
Aspirin 160-325 mg/day
start as early as
possible and continue
for 14 days (for
secondary prevention,
see under “Delayed
Management and
Treatment”)
Neuroprotection
(Appendix V-D)
Early rehabilitation once
stable within 72 hours
Consider
anticoagulation with IV
heparin or SQ low
molecular-weight
heparin (LMWH)
(Appendix VI)
or
Aspirin 160-325 mg/day
(if anticoagulation is not
possible or
contraindicated)
Neuroprotection
(Appendix V-D)
Early rehabilitation once
stable within 72 hours
If infective endocarditis
is suspected, give
antibiotics and do not
anticoagulate
TIA
Aspirin 160-325 mg/day
If crescendo TIA (multiple events within hours,
increasing severity and duration of deficits),
consider anticoagulation with IV heparin or SQ
LMWH
Early neurology and/
or neurosurgeon
consult for all ICH is
recommended
Monitor and maintain
BP: MAP 110-130
mmHg (lower limit
preferred) (Appendix
III)
Neuroprotection
(Appendix V-D)
Early rehabilitation
once stable within 72
hours
Give anticonvulsants
only if with seizures
Steroids are not
recommended
Monitor and correct
metabolic
parameters
Correct coagulation /
bleeding
abnormalities
Follow
recommendations for
neurosurgical
intervention
(Appendix VII)
For aneurysmal
SAH, refer to next
chapter.
5. CT Scan Not
Available
No specific emergent drug treatment recommended
Neuroprotection (Appendix V-D)
Consult a neurologist or neurosurgeon
Early supportive rehabilitation
Admit to Hospital
(Stroke Unit)
Urgent Outpatient Work-upPlace of
Treatment
1. Stroke onset within 48 hours
2. Patients requiring any specific
active intervention, such as:
BP control, monitoring and
stabilization
Cardiac stabilization, including AF,
CHF, acute MI
Hydration
Anticoagulation, if cardioembolic
3. Rapidly worsening deficits
4. Recurrent TIA within the past 2
weeks, especially those with
increasing severity and duration of
deficits, cardiac arrhythmia, or
carotid bruit
1. Single TIA more than 2 weeks
2. Transient monocular
blindness alone
3. Stable mild strokes >48 hours
from ictus not requiring
specific active intervention
Advise immediate re-consult or
admission if there is worsening of
deficit
IschemicDelayed
Management Thrombotic/Lacunar Cardioembolic
Hemorrhagic
6. and
Treatment
(Secondary
Prevention)
Control of risk factors
Antiplatelets (aspirin,
ticlopidine, dipyridamole,
extended-release
dipyridamole + aspirin
combination, clopidogrel,
cilostazol) (Appendix VIII)
Carotid ultrasound: If this
reveals >70% stenosis,
refer to
neurologist/neurosurgeon/
vascular surgeon for
decision-making regarding
CEA or stenting
Recommend transcranial
Doppler (TCD) to
document intracranial
stenosis
Echocardiography
and/or cardiology
consult
If age <75 and
PT/INR available,
anticoagulation with
coumadin
(target INR: 2-3)
If age >75, aspirin
80-325 mg/day or
coumadin (target
INR: 2.0 [1.6 – 2.5])
Long-term strict BP
control and
monitoring
Consider angiogram
if age <45 years,
normotensive, no
clear cause of ICH,
and/or is a candidate
for surgery
7. GUIDELINES FOR MODERATE STROKE
Management
Priorities
Ascertain clinical diagnosis of stroke (history and physical exam are very
important)
• Exclude common stroke mimickers (Appendix I)
Basic emergent supportive care (ABCs of resuscitation)
Neuro-vital signs, BP, MAP, RR, temperature, pupils
Perform stroke scales (NIHSS, GCS) (Appendix II)
Monitor and manage BP; treat if SBP>220 or DBP>120 or MAP>130
(Appendix III).
Precaution: Avoid precipitous drop in BP (not >20% of baseline MAP)
(Appendix III). Do not use rapid-acting sublingual agents; when
needed use easily titratable IV or oral antihypertensive medication.
Identify comorbidities (cardiac disease, diabetes, liver disease, gastric
ulcer, etc.)
Recognize and treat early signs and symptoms of increased ICP
(Appendix IX)
Ensure appropriate hydration. If IVF is needed, use 0.9% NaCl
Emergent
Diagnostics
• CBC
• CBG, HGT or RBS
• PT/PTT
• Serum Na+
and K+
• ECG
Plain CT scan of brain as
soon as possible;
computation of hematoma
volume (Appendix IV)
IschemicEarly
Specific
Treatment
Non-cardioembolic
(Thrombotic, Lacunar)
Cardioembolic
(Appendix V)
Hemorrhagic
8. CT scan
confirmed
(Appendix V)
If within 3 hours of
stroke onset, consider
IV recombinant tissue
plasminogen activator
(rtPA) and refer to
specialist
If within 6 hours of
stroke onset and in
specialized centers,
consider intra-arterial
(IA) thrombolysis
Aspirin 160-325
mg/day, start as early
as possible
Neuroprotection
(Appendix V-D)
Early supportive
rehabilitation
If within 3 hours of
stroke onset, consider
IV rtPA and refer to
specialist
If within 6 hours of
stroke onset and in
specialized centers,
consider IA
thrombolysis
Aspirin 160-325
mg/day, start as early
as possible
If source of embolism
can be demonstrated,
consider early
anticoagulation
Neuroprotection
(Appendix V-D)
Early supportive
rehabilitation
If infective endocarditis
is suspected, give
antibiotics and do not
anticoagulate
Early neurology and/ or
neurosurgical consult
for all ICH is
recommended
Monitor and maintain
BP: MAP 110-130
mmHg (lower limit
preferred)
Neuroprotection
(Appendix V-D)
Give anticonvulsants
only if with seizures
Steroids are not
recommended
Monitor and correct
metabolic parameters
Correct
coagulation/bleeding
abnormalities
Follow
recommendations for
neurosurgical
intervention (Appendix
VII)
Early rehabilitation
once stable
For aneurysmal SAH,
refer to next chapter.
9. Likely Ischemic Likely Hemorrhagic
CT scan not
available
No specific emergent drug treatment
recommended
Neuroprotection (Appendix V-D)
Refer to neurologist
Early supportive rehabilitation
Refer to
neurologist/neurosurgeon for
further diagnostic work-ups
and/or subsequent surgery
Neuroprotection (Appendix V-D)
Early supportive rehabilitation
Place of
Treatment
Hospital – Intensive Care Unit or Stroke Unit
Ischemic
Thrombotic/Lacunar Cardioembolic
HemorrhagicDelayed
Management
and
Treatment
(Secondary
Prevention)
Control of risk factors
Antiplatelets (aspirin,
ticlopidine, dipyridamole,
extended-release
dipyridamole + aspirin
combination, clopidogrel,
cilostazol) (Appendix VIII)
Carotid ultrasound: If this
reveals >70% stenosis,
refer to
neurologist/neurosurgeon/
vascular surgeon for
decision-making regarding
CEA or stenting
Recommend TCD to
document intracranial
stenosis
Echocardiography
and/or cardiology
consult
INR 2.0 (1.6 – 2.5)
If age <75 and
PT/INR available,
anticoagulation with
coumadin
(target INR: 2-3)
If age >75, aspirin
80-325 mg/day or
coumadin (target
INR: 2.0 [1.6 – 2.5])
Long-term strict BP
control and
monitoring
Consider CT
angiography, MRA,
or 4-vessel
angiography in
suspected cases of
aneurysm, AV
malformation or
vasculitis
10. GUIDELINES FOR SEVERE STROKE
Management
Priorities
Ascertain clinical diagnosis of stroke (history and physical exam are very
important)
• Exclude common stroke mimickers (Appendix I)
Basic emergent supportive care (ABCs of resuscitation)
Neuro-vital signs, BP, MAP, RR, temperature, pupils
Perform stroke scales (NIHSS, GCS) (Appendix II)
Monitor and manage BP; treat if SBP>220 or DBP>120 or MAP>130
(Appendix III).
Precautions:
• Avoid precipitous drop in BP (not >20% of baseline MAP) (Appendix
III). Do not use rapid-acting sublingual agents; when needed, use easily
titratable IV or oral antihypertensive medication (Appendix IIIB)
Identify comorbidities (cardiac disease, diabetes, liver disease, gastric
ulcer, etc.)
Recognize and treat early signs and symptoms of increased ICP
(Appendix IX)
Ensure appropriate hydration. If IVF is needed, use 0.9% NaCl
Emergent
Diagnostics
• CBC
• CBG, HGT or RBS
• PT/PTT
• Serum Na+
and K+
• ECG
Plain CT scan of brain;
computation of hematoma
volume (Appendix IV)
Early
Specific
Treatment
Ischemic Hemorrhagic
11. Non-cardioembolic
(Thrombotic)
Cardioembolic
(Appendix V)
CT scan
confirmed
(Appendix V)
May give aspirin 160-
325 mg/day
In posterior circulation
strokes within 6 hour
of onset, consider IA
thrombolysis and refer
to specialist
Neuroprotection
(Appendix V-D)
If cerebellar infarct,
consult neurosurgeon
as soon as possible
Early supportive
rehabilitation
May give aspirin 160-
325 mg/day
In posterior circulation
strokes within 6 hours
of onset, consider IA
thrombolysis and refer
to specialist
Neuroprotection
(Appendix V-D )
If cerebellar infarct,
consult neurosurgeon
as soon as possible
Early supportive
rehabilitation
Supportive treatment:
1. Mannitol 20% 0.5 -
1 g/kgBW q 4-6
hours for 3-7 days
2. Neuroprotection
(Appendix V-D)
Neurosurgery consult
if:
Patient not herniated;
bleed located in
putamen, pallidum,
cerebellum; family
is willing to accept
consequences of
irreversible coma or
persistent
vegetative state and
goal is reduction of
mortality
(Appendix VII)
2. ICP monitoring is
contemplated and
salvage surgery is
considered
Early supportive
rehabilitation
CT scan not
available
No specific emergent drug treatment recommended
Neuroprotection (appendix V-D)
Refer to neurologist
Place of
Treatment
Intensive Care Unit
Discuss prognosis with relatives of the patient in most compassionate
manner
Ischemic
Delayed
Management
and
Treatment Thrombotic Cardioembolic
Hemorrhagic
12. (Secondary
Prevention)
Control of risk factors
Antiplatelets (Aspirin,
ticlopidine,
dipyridamole,
extended-release
dipyridamole + aspirin
combination,
clopidogrel or
cilostazol)
(Appendix VIII)
Echocardiography
and/or cardiology
consult
If age <75 and PT/INR
available,
anticoagulation with
coumadin (target
INR=2.0-3.0)
If age >75, aspirin 80-
325 mg/day or
coumadin with target
INR 2.0 (1.6-2.5)
Long-term strict BP
control and monitoring
Consider CT
angiography, MRA, or
4-vessel angiography
in suspected cases of
aneurysm, AV
malformation or
vasculitis
13. APPENDIX I
Differential Diagnoses of Stroke
A. The presence of any of the following should alert the physician to
consider conditions other than stroke:
- Gradual progressive course and insidious onset
- Pure hemifacial weakness including forehead (Bell’s palsy)
- Trauma
- Fever prior to onset of symptoms
- Recurrent seizures
- Weakness with atrophy
- Recurrent headaches (migraine, tension-type headache)
B. Conditions that mimic stroke in the emergency department (according
to decreasing frequency):
1. Seizures
2. Systemic infection
3. Brain tumor
4. Toxic-metabolic
5. Positional vertigo
6. Cardiac
7. Syncope
8. Trauma
9. Subdural hematoma
10. Herpes encephalitis
11. Transient global amnesia
12. Dementia
13. Demyelinating disease
14. Cervical spine fracture
15. Myasthenia gravis
16. Parkinsonism
17. Hypertensive encephalopathy
18. Conversion disorder
Bibliography
Hand P, Kwan J, Lindley R, et al. Distinguishing a stroke and mimic at the
bedside. Stroke 2006;37:769 – 775.
Libman RB, Wirkowski E, Alvir J, Rao H. Conditions that mimic stroke in the
emergency department. Arch Neurol 1995;52:1119-1122.
The Brain Matters Stroke Initiative. Acute Stroke Management Workshop
Syllabus. Basic Principles of Modern Management for Acute Stroke.
14. APPENDIX II
Stroke Scales
I. Glasgow Coma Scale
Category Score
Eye Opening
Spontaneous
To speech
To pain
None
4
3
2
1
Best Motor Response
Obeys
Localizes
Withdraws
Abnormal flexion (decorticate)
Abnormal extension (decerebrate)
None
6
5
4
3
2
1
Best Verbal response
Oriented
Confused
Inappropriate words
Incomprehensible sounds
None
5
4
3
2
1
Total score=15
II. National Institutes of Health (NIH) Stroke Scale
Items Scale Definition
Ia. Level of
Consciousness
(LOC)
0 = Alert, keenly responsive
1 = Not alert, but arousable by minor stimulation to
obey, answer or respond
2 = Not alert, requires repeated stimulation to attend, or
is obtunded and requires strong or painful stimulation
to make movements (not stereotyped)
3 = Responds only with reflex motor or autonomic
effects or totally unresponsive, or totally unresponsive,
flaccid, areflexic
Ib. LOC
Questions
0 = Answers both questions correctly
1 = Answers one question correctly
2 = Answers neither question correctly
Ic. LOC
Commands
0 = Performs both tasks correctly
1 = Performs one task correctly
2 = Performs neither task correctly
15. 2. Best gaze 0 = Normal
1= Partial gaze palsy. Gaze is abnormal in one or both
eyes but forced deviation or total gaze paresis is not
present
2 = Forced deviation, or total gaze paresis is not
overcome by oculocephalic maneuver
3. Visual 0 = No visual loss
1 = Partial hemianopia
2 = Complete hemianopia
3 = Bilateral hemianopia (blind, including cortical
blindness)
4. Facial palsy 0 = Normal symmetrical movement
1 = Minor paralysis (flattened nasolabial fold,
asymmetry on smiling)
5. Motor (Arm)
5 a. Left arm
5 b. Right
arm
0 = No drift; limb holds 90 (or 45) degrees for full 10
seconds
1 = Drifts; limb holds 90 (or 45) degrees but drifts down
before full 10 seconds; does not hit bed or other
support
2 = Some effort against gravity, limb cannot get up to or
maintain (if cued) 90 (or 45) degrees; drifts down to
bed, but has some effort against gravity
3 = No effort against gravity; limb falls
4 = No movement
9 = Amputation or joint fusion; explain
6. Motor (Leg)
6 a. Right leg
6 b. Left leg
0 = No drift; leg holds 30-degree position for full 5
seconds
1 = Driftd; leg falls by the end of the 5-second period
but does not hit bed
2 = Some effort against gravity; leg falls to bed by 5
seconds but has some effort against gravity
3 = No effort against gravity; leg falls to bed
immediately
4 = No movement
9 = Amputation or joint fusion; explain
7. Limb ataxia 0 = absent
1 = Present in one limb
2 = Present in two limbs
9 = Amputation or joint fusion; explain
8. Sensory 0 = Normal; no sensory loss
1 = Mild to moderate sensory loss; patient feels
pinprick is less sharp or dull on the affected side; or
there is a loss of superficial pain with pinprick, but
patient is aware he/she is being touched
2 = Severe or total sensory loss; patient is not aware of
being touched in the face, arm or leg
16. 9. Best
Language
0 = No aphasia
1 = Mild to moderate aphasia; some obvious loss of
fluency or facility of comprehension, without significant
limitation on ideas expressed or form of expression.
Reduction of speech and/or comprehension, however,
makes conversation on provided material difficult
2 = Severe aphasia; all communication is through
fragmentary expression; great need for inference,
questioning and guessing by the listener. Range of
information that can be exchanged is limited; listener
carries the burden of communication
3 = Mute, global aphasia; no usable speech or auditory
comprehension
10. Dysarthria 0 = Normal
1 = Mild to moderate; patient slurs at least some words
and at worst, can be understood with some difficulty
2 = Severe; patient’s speech is so slurred as to be
unintelligible in the absence of or out of proportion to
any dysphasia, or is mute/anarthric
9 = intubated or other physical barrier; explain
11. Extinction &
Inattention
0 = No abnormality
1 = Visual, tactile, auditory, spatial or personal
inattention or extinction to bilateral simultaneous
stimulation in one of the sensory modalities
2 = Profound hemiattention or hemi-inattention to more
than one modality. Does not recognize own hand or
orients to only one side of space
Total score=42
III. Modified Rankin Scale
Score
No symptoms at all 0
No significant disability despite symptoms; able to
carry out all usual duties and activities
1
Slight disability; unable to carry out all previous
activities but able to look after own affairs without
assistance
2
Moderate disability; requiring some help but able to
walk without assistance
3
Moderately severe disability; unable to walk without
assistance and unable to attend to own bodily needs
without assistance
4
Severe disability; bedridden, incontinent and requiring
constant nursing care and attention
5
17. Bibliography
Brott T, Adams H. Olinger CP, et al. Measurements of acute cerebral infarction: a clinical examination scale.
Stroke 1989;20:864-870.
Goldstein LB, Bartels C. Davis JN. Interrater reliability of the NIH Stroke Scale. Arch Neurol 1989;46:660-
662.
Rankin J. Cerebral vascular accidents in patients over the age of 60. Scot Med J 1957;2:200-215.
Van Swieten JC, Koudstaal JP, Visser MC, et al. Interobserver agreement for the assessment of handicap in
stroke patients. Stroke 1988;19:604-607.
The Brain Matters Stroke Initiative. Acute Stroke Management Workshop Syllabus. Basic Principles of
Modern Management for Acute Stroke.
18. APPENDIX III
Blood Pressure Management
A. BP management in Acute Ischemic Stroke
1. Use the following definitions:
Cerebral Perfusion Pressure (CPP) = MAP – ICP
MAP = 2 (diastolic) + systolic
3
2. Check if patient is in any condition that may increase BP such as pain, stress,
bladder distention or constipation, which should be addressed accordingly.
3. Allow “permissive hypertension” during the first week to ensure adequate CPP
but ascertain cardiac and renal protection
a. Treat if SBP>220 or DBP>120 or MAP>130
b. Defer emergency BP therapy if MAP is within 110-130 or SBP=185-220
mmHg or DBP=105-120 mmHg, unless in the presence of:
Acute MI
Congestive heart failure
Aortic dissection
Acute pulmonary edema
Acute renal failure
Hypertensive encephalopathy
4. Treat with small doses of IV antihypertensives patients who are potential
candidates for rtPA therapy who have persistent elevations in SBP >185 mmHg
or DBP >110 mmHg. Maintain BP just below these limits.
5. Use the following locally available intravenous anti-hypertensives in acute
stroke:
Drug Dose Onset of
Action
Duration
of
Action
Availability
/Dilution
Stability Adverse
Reactions
Action
Nicardipine
1-15
mg/hour
5-10
mins
1-4
hours
(10 mg/ 10
ml amp );
10 mg in
90 ml
NSS/D5W
1 to 4
hours
Tachycardia,
headache,
flushing,
dizziness,
somnolence,
nausea
Inhibits calcium
ion from
entering slow
channel,
producing
coronary,
vascular,
smooth muscle
relaxation &
vasodilatation
19. Hydralazine
IV push 10-
20 mg/dose
q 4-6 hours
as needed,
may
increase to
40 mg/dose
10-20
mins
3-8
hours
25 mg/mL
amp; 25
mg/tab
4 days Tachycardia,
flushing,
headache,
vomiting,
increased
angina
Direct
vasodilatation
of arterioles &
decreased
systemic
resistance
Labetalol
5 mg IV
push over 2
mins,
repeat with
incremental
dose of 10,
20, 40, 80
mg until
desired BP
is achieved
or a total
dose of 300
mg has been
administered
2-5
mins
2-4
hours
5 mg/ml in
40 ml vial;
250 mg in
250 mL
NSS/D5W
72
hours
Orthostatic
hypotension,
drowsiness,
dizziness,
lightheadednes
s, dyspnea,
wheezing &
bronchospasm
Alpha- & beta-
blocker. Beta-
adrenergic
blocking activity
is 7x > than
alpha-
adrenergic
blockers.
Produces dose-
dependent ↓ in
BP without
significant ↓ in
HR or cardiac
output
Esmolol
0.25-0.5 mg/
kg IV push
1-2 mins
followed by
infusion of
0.05
mg/kg/min.
If there is no
response,
repeat 0.5
mg/kg bolus
dose & ↑
infusion to
0.10
mg/kg/min.
Maximum
infusion
rate=0.30
mg/kg/min
2-10
mins
10-30
mins
100 mg/
10 ml vial;
2,500 mg
in 250 mL
D5W/NSS
48
hours
Hypotension,
bradycardia,
AV block,
agitation,
confusion,
wheezing /
bronchoconstric
tion, phlebitis
Short-acting
beta-adrenergic
blocking agent.
At low doses,
has little effect
on beta2
receptors of
bronchial &
vascular
smooth muscle
B. Blood pressure management in Acute Hypertensive ICH
Maintain MAP<130, but not lower than 110 mmHg
• Sustained hypertension may alter cerebral autoregulation, promote
progression of bleed and increase edema
• Hypotension may result in cerebral hypoperfusion especially in the setting of
increased intracranial pressure (ICP)
• Absence of penumbra allows for more aggressive BP management
Bibliography
Adams H, Adams R, del Zoppo G, Goldstein L. Guidelines for the early management of patients with
ischemic stroke. 2005 Guidelines update, a scientific statement from the Stroke Council of the American
Heart Association. Stroke 2005;36:916-923.
20. Broderick JP, Adams HP, Barsan W, et al. Guidelines for the management of spontaneous intracerebral
hemorrhage: a statement for healthcare professionals from a special writing group of the Stroke Council of
the American Heart Association. Stroke 1999;30:905-915.
Fogelholm R, Avikainen S and Murros K. Prognostic value and determinants of first day mean arterial
pressure in spontaneous supratentorial intracerebral hemorrhage. Stroke 1997;28:1396-1400.
Guyton A and Hall J. Guyton and Hall’s Textbook of Medical Physiology, 11
th
ed. USA: WB Saunders; 2005.
Kidwell CS, Saver JL, Mattiello J, et al. Diffusion perfusion MR evaluation of perihematomal injury in
hyperacute intracebral hemorrhage. Neurology 2001;57:1611-1617.
Powers WJ, Zazulia AR, Videen TO, et al. Autoregulation of cerebral blood flow surrounding acute (6-
22hours) intracerebral hemorrhage. Neurology 2001;57:18-24.
Qureshi A, Wilson D, Hanley D, Traystman R. No evidence for an ischemic penumbra in massive
experimental intracerebral hemorrhage. Neurology 1999;52:266-272.
Schellinger P, Fiebach J, Hoffman K, et al. Stroke MRI in intracerebral hemorrhage: is there a
perihemorrhagic penumbra? Stroke 2003;34:1647-1680.
The Brain Matters Stroke Initiative. Acute Stroke Management Workshop Syllabus. Basic Principles of
Modern Management for Acute Stroke.
21. APPENDIX IV
Neuroimaging (CT and MRI)
A. Hyperacute or Acute Ischemic Stroke
• Plain CT scan of the head is the initial neuroimaging study of choice in
acute stroke. The main objective is to exclude hemorrhagic stroke and
stroke mimickers. A plain study obviates the need to wait for creatinine
result.
• CT scan is 100% sensitive in documenting intracranial hemorrhage (ICH)
and 96% sensitive in documenting subarachnoid hemorrhage (SAH).
• Cerebral infarcts are often not documented within 3 hours from stroke
onset. However, 60% have “early” infarct signs when viewed very closely:
1. Dense MCA sign
2. Obscuration of the lentiform nucleus
3. Loss of the gray-white interphase along the lateral insula
(Insular ribbon sign)
4. Effacement of the sulci
• In cases of neurologic deterioration, large infarcts or suspected
hemorrhagic conversion, a follow-up plain CT of the head is
recommended.
• MRI has the technical advantage of documenting small lesions or those
located in the brainstem or posterior fossa.
• MRI can detect early infarction as early as 90 minutes using Diffusion
Weighted Imaging (DWI).
• Despite the superior diagnostic yield of MRI over CT, MRI is not
recommended as routine evaluation of patients with acute ischemic
stroke. It is more expensive, time-consuming and less readily available.
B. Intracerebral Hemorrhage
• CT can accurately document the exact location of the hemorrhage and the
presence of mass effect, ventricular extension and hydrocephalus.
• In hypertensive ICH, a repeat plain CT scan after 24 hours of ictus is
recommended especially in cases showing clinical deterioration to
document hematoma enlargement and/or development of hydrocephalus.
Computation of Hematoma Volume (Kothari method)
Hematoma volume (in cc) = A x B x C
2
where: A= Largest diameter of hematoma (in cm)
B= Diameter perpendicular to A (in cm)
C= Number of slices on CT scan with hemorrhage X slice
thickness (in cm)
22. − Count slice as 1 if size of hematoma is >75% of largest diameter
− Count slice as 0.5 if size of hematoma is 25-75% of largest
diameter
− Disregard slice if size of hematoma is <25% of largest diameter
• In suspected cases of AV malformation, aneurysm or tumor bleed, a
contrast CT of the head may be warranted
C. Subarachnoid Hemorrhage
• Plain CT of the head is strongly recommended as the initial procedure for
diagnosis.
• The diagnostic yield of CT goes down from 92% within the first 24 hours
to 50% within 7 days of onset.
Bibliography
Brott T, Broderick J, Kothari R, et al. Early Hemorrhage growth in patients with intracerebral hemorrhage.
Stroke 1997;28:1-5.
Culebras A, Kase C, Masdeu J, et al. Practice guidelines for the use of imaging in transient ischemic attacks
and acute stroke. Stroke 1997;28:1480-1497.
Kothari RU, Brott T, Broderick JP, et al. The ABCs of measuring intracerebral hemorrhage volumes. Stroke
1996;27:1304-1309.
Osborne A. Diagnostic Neuroradiology, 1
st
edition. USA: Mosby; 1994.
23. APPENDIX V
Early Specific Treatment For Ischemic Stroke
A. Thrombolytic therapy
- Patients treated with IV recombinant tissue plasminogen activator (rtPA)
within 3 hours of stroke onset are at least 30% more likely to have minimal or
no disability at 3 months.
- Streptokinase has no role in acute thrombolysis for ischemic stroke .
National Institute of Neurological Disorders and Stroke (NINDS) rTPA
guidelines
1. Dose of rtPA is 0.9 mg/kg (maximum 90 mg). Ten percent of total dose
is given as IV bolus, the rest as infusion over 60 minutes.
2. rtPA is recommended within 3 hours of onset of ischemic stroke. The
benefit of IV rtPA for acute ischemic stroke beyond 3 hours from onset
of symptoms is not established. IV rtPA is not recommended when the
time of onset of stroke cannot be ascertained reliably, including strokes
recognized upon awakening.
3. Thrombolytic therapy is not recommended unless the diagnosis is
established by a physician with expertise in diagnosing stroke and CT
of the brain is assessed by physicians with expertise in reading this
imaging study. If CT demonstrates early changes of a recent major
infarction such as sulcal effacement, mass effect, edema or possible
hemorrhage, thrombolytic therapy should be avoided.
4. Thrombolytic therapy cannot be recommended for patients with any of
the following (NINDS Study):
a. Current use of oral anticoagulants or PT>15 seconds (INR>1.7)
b. Use of heparin in the previous 48 hours or prolonged PTT>1.5x
normal
c. Platelet count <100,000 mm3
d. Another stroke or a serious head injury within the previous 3
months
e. Major surgery within the preceding 14 days
f. Sustained pretreatment SBP>185 mmHg or DBP>110 mmHg
(when aggressive treatment necessary to lower BP)
g. Rapidly improving neurological signs
h. Mild, isolated neurological deficits, such as ataxia alone,
sensory loss alone, dysarthria alone, or minimal weakness
i. Prior ICH
j. Blood glucose <50 mg/dL or > 400 mg/dL
k. Seizure at onset of stroke
l. Gastrointestinal or urinary bleeding within preceding 21 days
m. Recent myocardial infarction (within the previous 3 months)
24. 5. Thrombolytic therapy should not be given unless emergent ancillary
care and the facilities to handle bleeding complications are readily
available.
6. Caution is advised before giving rtPA to persons with severe stroke
(NIH Stroke Scale Score >22)
7. Because the use of thrombolytic drugs carries the real risk of major
bleeding, whenever possible the risks and potential benefits of rtPA
should be discussed with the patient and his or her family before
treatment is initiated.
8. Patients given rtPA should not receive antiplatelets or anticoagulants
within 24 hours of treatment.
B. Antithrombotic therapy
1. International Stroke Trial (IST)
- Multicenter randomized clinical trial of 19,435 patients
- Regimen: Aspirin 300-325 mg/day vs. no aspirin
Heparin SC vs. no heparin
5,000 units bid or 12,500 units bid
- Started within 48 hours of stroke onset for 14 days or until
discharge
- Results:
Aspirin
- Fewer recurrent stroke within 14 days
- Fewer deaths and dependency at 6 months
Heparin
- No benefit even at 6 months
- If used should not exceed 5,000 units bid
2. Chinese Acute Stroke Trial (CAST)
- 21,106 patients randomized
- Aspirin 160 mg/day vs. placebo
- Started within 48 hours of stroke onset
- Results:
Risk of recurrent stroke or vascular death:
Aspirin 5.3%
Placebo 5.9% (p=0.03)
3. Meta-analysis on low molecular-weight heparin (LMWH) and
heparinoids in acute ischemic stroke involving 2,855 patients has
shown that treatment was associated with significant reduction in
venous thromboembolism (DVT and pulmonary embolism). LMWH has
no significant effect on reducing death and disability at 6 months.
Symptomatic ICH was not significantly increased.
25. C. Neuroprotection
1. Neuroprotective Interventions: The 5 “H” Principle
Avoid hypotension, hypoxemia, hyperglycemia or hypoglycemia
and hyperthermia (fever) during acute stroke in an effort to "salvage"
the ischemic penumbra
Avoid Hypotension
• Aggressive BP lowering is detrimental in acute stroke.
Manage hypertension as per recommendation (Appendix III)
Avoid Hypoxemia
• Routine oxygenation in all stroke patients is not warranted
• Maintain adequate tissue oxygenation (target O2 saturation
>95%)
• Do arterial blood gases (ABG) determination or monitor
oxygenation via pulse oximeter
• Give supplemental oxygen if there is evidence of hypoxemia
or desaturation
• Provide ventilatory support if upper airway is threatened or
sensorium is impaired or ICP increased.
Avoid hypoglycemia or hyperglycemia
• Hyperglycemia can increase the severity of ischemic injury
(causes lactic acidosis, increases production of free radicals,
worsens cerebral edema and weakens blood vessels),
whereas hypoglycemia can mimic a stroke
• Prompt determination of blood glucose should be done in all
stroke patients
• Ensure tight glycemic control at 80-110 mg/dL
• Avoid glucose-containing (D5) IV fluids. Use isotonic saline
(0.9% NaCl)
Avoid Hyperthermia
• Fever in acute stroke is associated with poor outcome
possibly related to increased metabolic demand, increased
free radical production and enhanced neurotransmitter
release.
• For every 1°C increase in body temperature, the relative risk
of death or disability increases by 2.2.
• Search for the source of fever.
• Treat fever with antipyretics and cooling blankets.
• Maintain normothermia.
D. Neuroprotectants
26. Neuroprotectants are drugs that:
o Protect against excitotoxins and prolong neuronal survival
o Block the release of glutamate, free radicals, inflammatory cytokines,
and the accumulation of intracellular calcium cations.
Several neuroprotective drugs have reached phase III clinical trials, but
most had negative or disappointing results except for citicoline. Data-pooling
analysis on four trials involving 1,652 patients with ischemic stroke show that
treatment with citicoline within the first 24 hours increases the probability of
global recovery (NIHSS, mRS, BI) by 30% at 3 months.
CDP–choline helps increase phosphatidylcholine synthesis and inhibition
of phospholipase A2 within the injured brain during ischemia
Several phase III clinical trials (e.g. SAINT II, FAST-MAG) are currently
underway
Bibliography
Adams H, Adams R, del Zoppo G, Goldstein L. Guidelines for the early management of patients with
ischemic stroke. 2005 Guidelines update, a scientific statement from the Stroke Council of the American
Heart Association. Stroke 2005;36:916-923.
Adams H, Brott T, Furlan A, et al. Guidelines for thrombolytic therapy for acute stroke: supplement to the
guidelines for the management of patients in acute ischemic stroke. Circulation 1996;94:1167-1174.
Adams H. Emergent use of anticoagulation for treatment of patients with ischemic stroke. Stroke
2002;33:856-861.
Albers GW, Amarenco P, Easton JD, et al. Antithrombotic and thrombolytic therapy for ischemic stroke The
Seventh ACCP Conference on Antithrombotic and Thrombolytic Therapy. Chest 2004;126(3 Suppl):483S-
512S.
Bath P, Iddenden R, Bath, F. Low Molecular weight heparins and heparinoids in acute ischemic stroke. a
meta-analysis of randomized controlled trials. Stroke 2000;31:1770-1778.
Chen Z, Sandercock P, Pan H, et al. Indications for early aspirin use in acute ischemic stroke: a combined
analysis of 40,000 randomized patients from the CAST and IST. Stroke 2000;31:1240-1249.
Chinese Acute Stroke Trial Collaborative Group. CAST: randomised placebo-controlled trial of early aspirin
use in 20,000 patients with acute ischaemic stroke. Lancet 1997;349:1641-1649.
Clark WM, Warachi SJ, Pettigrew LC, et al; for the Citicoline Stroke Study Group. A randomized dose
response trial of citicoline in acute ischemic stroke patients. Neurology 1997;29:671-678.
Coull BM , Willliam LS, Goldstein LB. et al. Anticoagulants and antiplatelets in acute ischemic stroke. Report
of the Joint Stroke Guideline Development Committee of the American Academy of Neurology and the
American Stroke Association. Neurology 2002;59:13-22.
Davalos A, Castillo J, Alvarez-Sabin J, et al. Oral citicoline in acute ischemic stroke: an individual patient
data pooling analysis of clinical trials. Stroke 2002;33:2850-2857.
International Stroke Trial Collaborative Group. The International Stroke Trial: a randomised trial of aspirin,
subcutaneous heparin, both or neither among 19,435 patients with acute ischemic stroke. Lancet
1997;349:1569-1581.
Labiche LA, Grotta JC. Clinical trials for cytoprotection in stroke. NeuroRx 2004;1:46-70.
27. Lyden P, Wahlgren N. Mechanism of action of neuroprotectants in stroke. Journal of stroke and
cerebrovascular diseases.2000; 9(6): 9 – 14.
NINDS rt-PA Stroke Study Group. Tissue plasminogen activator for acute ischemic stroke. N Engl J Med
1995;333:1581-1587.
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.
28. APPENDIX VI
Anticoagulation In Acute Cardioembolic Stroke
A. Cardioembolic sources
High Risk Low or Uncertain Risk
AF (valvular or non-valvular) Mitral valve Prolapse
Rheumatic mitral stenosis Mitral annular calcification
Prosthetic heart valves Patent foramen ovale (PFO)
Recent MI Atrial septal aneurysm
LV/LA thrombus Calcific aortic stenosis
Atrial myxoma Mitral valve strands
Infective Endocarditis
Dilated cardiomyopathy
Marantic endocarditis
B. Indications and contraindications for anticoagulation in patients with
cardioembolic stroke
Probably Indicated Contraindicated
Intracardiac thrombus Bleeding diathesis
Mechanical prosthetic valve Non-petechial intracranial
hemorrhage
Recent MI Recent major surgery or trauma
CHF Infective endocarditis
Bridging measure for long term
anticoagulation
C. When considering anticoagulation in acute cardioembolic stroke, the benefits
of anticoagulation in reducing early stroke recurrence should be weighed against
the risk of hemorrhagic transformation. The latter is higher in patients with large
infarction, severe strokes or neurological deficits and uncontrolled hypertension.
D. How to anticoagulate
1. Requirements for IV anticoagulation of patients with cardiogenic source of
embolism:
a. Heparin sodium in D5W
b. Infusion pump, if available
c. Activated partial thromboplastin time (aPTT) or clotting time
2. Procedure:
a. Start intravenous infusion at 800 units heparin/hour ideally using
infusion pump. IV heparin bolus is not recommended.
29. b. Perform aPTT as often as necessary, every 6 hours if need, to keep
aPTT at 1.5-2.5x the control. Risk for major hemorrhage, including
intracranial bleed, progressively increases as aPTT exceeds 80
seconds.
c. Infusion may be discontinued once oral anticoagulation with coumadin
has reached therapeutic levels or once antiplatelet medication is
started for secondary prevention.
To date, there has been no trial directly comparing efficacy of unfractionated
heparin vs LMWH in patients with acute cardioembolic stroke. LMWH has the
advantage of ease of administration and does not require aPTT monitoring.
Bibliography
Adams H. Emergent use of anticoagulation for treatment of patients with ischemic stroke. Stroke
2002;33:856-861.
Hart R, Palacio S, Pearce L. Atrial fibrillation, stroke and acute antithrombotic therapy. Stroke 2002;33:2722-
2727.
Moonis, M, Fisher M. Considering the role of heparin and low-molecular weight heparin in acute ischemic
stroke. Stroke 2002;33:1927-1933.
30. APPENDIX VI
Early Specific Treatment of Hypertensive Intracerebral Hemorrhage
A. Medical Treatment for all ICH:
The goals are to prevent complications and careful manage BP.
a. Maintain MAP <130, but not lower than 110 mmHg
b. Manage increased ICP accordingly (see Appendix IX)
c. Start anticonvulsants only if with seizures
• The incidence of seizures is higher in ICH, especially in lobar
hematomas.
• The role of prophylactic anticonvulsants in deep
hemorrhages is unclear. It is justified to withhold
anticonvulsants until clinically indicated.
d. Prevent and treat respiratory complications. Endotracheal
intubation is performed in patients to provide airway protection
and in those in coma or with respiratory failure.
e. Prevent and treat infections.
f. Maintain adequate nutrition.
g. Ensure proper fluid and electrolyte balance; maintain
normothermia and normoglycemia.
h. Rehabilitate early once stable.
i. Practice bedsore precautions.
j. Deep-vein thrombosis and pulmonary embolism prophylaxis
should be instituted (use antiembolic stockings or intermittent
pneumatic compression devices)
B. Surgical Treatment
Its role depends on the size, extent and location of the hematoma, and
patient factors.
a. There is evidence of increase in hematoma size by 33% within
24 hours of stroke onset in 38% of cases.
b. Considerations for surgical intervention:
Non-surgical candidates
• Patients with small hemorrhages (<10 mL) or minimal
neurological deficits
• Patients with GCS<5 except those who have cerebellar
hemorrhage and brainstem compression
• Patients with hematoma volume > 85 mL
Candidates for immediate surgery
• Patients with cerebellar hemorrhage >3 cm who are
neurologically deteriorating or have brainstem compression
and hydrocephalus from ventricular obstruction
31. • Patients with bleed associated with a structural lesion such
as an aneurysm, AV malformation or cavernous angioma if
there is a chance for good outcome and the vascular lesion
is surgically accessible
• Clinically deteriorating young patients with moderate or large
lobar hemorrhage.
• Ventricular drainage for patients with intraventricular
hemorrhage with moderate to severe hydrocephalus.
All other patients may benefit from surgery
• Patients with basal ganglia or thalamic hemorrhage
• Patients with GCS >4
• Patients with supratentorial hematoma with volume >30 cc
Bibliography
Academy of Filipino Neurosurgeons Guidelines on the Management of Hypertensive ICH
Broderick JP, Brott TG, Tomsick T, et al. Ultra-early evaluation of intracerebral hemorrhage. J Neurosurg
1990;72:195-199.
Broderick JP, Adams HP, Barsan W, et al. Guidelines for the management of spontaneous intracerebral
hemorrhage: a statement for healthcare professionals from a special writing group of the Stroke Council of
the American Heart Association. Stroke 1999;30:905-915.
Brott T, Broderick J, Kothari R, et al. Early hemorrhage growth in patients with intracerebral hemorrhage.
Stroke 1997;28:1-5.
Fujii Y, Tanaka R, Takeuchi S, et al. Hematoma enlargement in spontaneous intracerebral hemorrhage. J
Neurosurg 1994;80:51-57.
Juvela S, Heiskanen O, Poranen A, et al. The treatment of spontaneous intracerebral hemorrhage. A
prospective randomized trial of surgical and conservative treatment. J Neurosurg 1989;70:755-758.
Kazui S, Naritomi H, Yamamoto H, et al. Enlargement of spontaneous intracerebral hemorrhage. Incidence
and time course. Stroke 1996;27:1783-1787.
Kothari RU, Brott T, Broderick JP, et al. The ABCs of measuring intracerebral hemorrhage volumes. Stroke
1996;27:1304-1309.
32. APPENDIX VIII
Antiplatelets for Secondary Stroke Prevention
A. Aspirin
1. Antiplatelet Trialist’s Collaboration
65 trials involving 60,196 patients with symptomatic atherosclerosis
(e.g., unstable angina, MI, TIA, stroke)
Aspirin 50-1,500 mg/day vs control
23% odds reduction on composite outcome of MI, stroke or vascular
death
Highest RRR was seen in the low (75-150 mg) and medium dose (160-
325 mg) groups
2. Mini-meta-analysis on aspirin among patient with prior stroke or TIA
10 trials involving 6,171 patients with prior TIA or non-disabling stroke
Aspirin reduced the odds for the cluster of stroke, MI or vascular death
by 16%
No difference in RRR for low (<100 mg), medium (300-325 mg) and
high doses (>900 mg) of aspirin
B. Ticlopidine
1. Canadian American Ticlopidine Study (CATS)
1,072 patients with recent thromboembolic stroke
Ticlopidine 250 mg bid vs placebo
30.2% risk reduction on composite outcome of MI, stroke, vascular
death over placebo
2. Ticlopidine Aspirin Stroke Study (TASS)
3,069 patients with recent TIA/cerebral infarction
Ticlopidine 250 mg bid vs aspirin 1,300 mg od
12% risk reduction vs aspirin for stroke or death at 3 years
C. Clopidogrel
1. Clopidogrel vs Aspirin in Patients at Risk of Ischemic Events (CAPRIE)
19,185 patients with prior stroke, MI or PAD
Clopidogrel 75 mg/day vs aspirin 325 mg/day
8.7% RRR vs aspirin for combined endpoint of stroke, MI and vascular
death
2. Clopidogrel and Aspirin combination (Management of Atherothrombosis
with Clopidogrel in High-Risk Patients with TIA or Stroke [MATCH])
7,599 patients with prior stroke or TIA and additional risk factors
Clopidogrel-aspirin 75 mg/75 mg vs clopidogrel 75 mg
No significant difference in composite outcome of ischemic stroke, MI,
vascular death or rehospitalization secondary to ischemic events
33. 3. Clopidogrel for High Atherothrobotic Risk and Ischemic Stabilization,
Management and Avoidance (CHARISMA)
15,603 patients with either clinically evident cardiovascular disease or
multiple risk factors
Clopidogrel 75 mg with low-dose aspirin (75-162 mg) vs low-dose
aspirin only
Overall, clopidogrel/aspirin combination was not significantly more
effective than aspirin alone in reducing rate of MI, stroke or vascular
death
Suggestion of benefit with combination treatment in patients with
symptomatic atherothrombosis
D. Cilostazol
Cilostazol Stroke Prevention Study (CSPS)
1,095 patients with cerebral infarction in the past 6 months
Cilostazol 100 mg bid vs placebo
41.7% RRR for recurrent stroke
E. Dipyridamole and asprin combination
1. European Stroke Prevention Study (ESPS 2)
6,602 patients with recent TIA or stroke randomized to placebo, aspirin
25 mg bid, extended-release dipyridamole 200 mg bid, or aspirin 25
mg + ER-dipyridamole 200 mg bid
Aspirin better than placebo; dipyridamole better than placebo;
combination treatment better than either agent alone.
37.8% risk reduction for stroke with combination therapy over placebo
No increased risk of major bleeding with combination treatment
2. European/Australasian Stroke Prevention in Reversible Ischemia Trial
(ESPRIT Trial)
2,739 patients with recent TIA or minor stroke of arterial origin
randomized to aspirin 30-325 mg/day or aspirin 30-325 mg od +
dipyridamole 200 mg bid
20% risk reduction for composite outcome of stroke, MI, vascular death
with combination therapy
No increased risk of major bleeding with combination treatment
Bibliography
Albers GW, Amarenco P, Easton JD, et al. Antithrombotic and thrombolytic therapy for ischemic stroke The
Seventh ACCP Conference on Antithrombotic and Thrombolytic Therapy. Chest 2004;126 (3 suppl):483S-
512S
Algra A, van Gijn J. Aspirin at any dose above 30 mg offers only modest protection after cerebral ischemia. J
Neurol Neurosurg Psychiatry 1996;60:197-199.
Antithrombotic Trialist Collaboration, Collaborative meta-analysis of randomized trials of antiplatelet therapy
for prevention of death, myocardial infarction and stroke in high-risk patients. BMJ 2002;324:71-86.
34. Bhatt D, Fox K, Hacke W, et al; for the CHARISMA Investigators. Clopidogrel and aspirin alone for the
prevention of atherothrombotic events. N Eng J Med 2006;354:1-12.
CAPRIE Steering Committee. A randomized, blinded trial of clopidogrel vs aspirin in patients at risk of
ischemic events. Lancet 1996:348:1329-1339.
Diener HC, Cunha L, Forbes C, et al. European Stroke Prevention Study 2. Dipyridamole and Aspirin in the
secondary prevention of stroke. J Neurol Sci 1996;143:1-13.
Diener HC, Bogousslavsky J, Brass LM, et al; for the MATCH Investigators. Aspirin and clopidogrel
compared with clopidogrel alone after recent ischemic stroke or TIA in high risk patients (MATCH): a
randomized, double- blind, placebo- controlled trial. Lancet 2004;364:331-337.
Gent M, Blakely JA, Easton JD, et al. The Canadian American Ticlopidine Study (CATS) in Thromboembolic
Stroke. Lancet 1989;1:1215-1220.
Gotoh F, Tohgi H, Hirai S, et al. Cilostazol Stroke Prevention Study: a placebo controlled trial double-blind
trial for secondary prevention of cerebral infarction. J Stroke Cerebrovasc Dis 2000;9:147-157.
Halkes PH, van Gijn J, Kappelle LJ, et al; for the ESPRIT Study Group. Aspirin plus dipyridamole versus
aspirin alone after cerebral ischemia of arterial origin. Lancet 2006;367:1665-1673.
Hass WK, Easton JD, Adams HP, et al. A randomized trial comparing ticlopidine hydrochloride with aspirin
for the prevention of stroke in high-risk patients. N Eng J Med 1989;321:501-507.
35. APPENDIX IX
Management of Increased Intracranial Pressure
A. Signs and symptoms of increased ICP
1. Deteriorating level of sensorium
2. Cushing’s triad
i. Hypertension
ii. Bradycardia
iii. Irregular respiration
3. Anisocoria
B. Management options for increased ICP
General
1. Control agitation and pain with short-acting medications, such as NSAIDS
and opioids.
2. Control fever. Avoid hyperthermia.
3. Control seizures if present. May treat with phenytoin with a loading dose of
18-20 mg/kg IV then maintained at 3-5 mg/kg. Status epilepticus should
be managed accordingly.
4. Strict glucose control between 80-110 mg/dL
5. No dextrose-containing IVF. Hyperglycemia may extend ischemic zone
(penumbra) and further cause cerebral edema
6. Use stool softeners to prevent straining.
Specific
1. Elevate the head at 30 to 45 degrees to assist venous drainage.
2. Give osmotic diuretics: Mannitol 20% loading dose at 1 g/kg, maintenance
dose at 0.5-0.75 mg/kg) to decrease intravascular volume and free water.
3. Lost fluids must be replaced. Hypertonic saline is an option and has the
advantage of maintaining an effective serum gradient for a prolonged
period with lower incidence of rebound intracranial hypertension. Aim for
serum osmolarity=310 mOsm/L. (Serum osmolarity = 2 (Na) + Glucose/18
+ BUN /2.8)
4. Hyperventilate only in impending herniation by adjusting tidal volume and
pCO2 between 25 to 30. This maneuver is usually effective only for
approximately 6 hours. Otherwise maintain normal pCO2 between 35 and
40.
5. Carefully intubate patients with GCS 8 or less, or those unable to protect
the airway.
6. Do CSF drainage in patients with intraventricular hemorrhage (IVH) or
hydrocephalus.
7. Use barbiturates if all other measures fail. Available locally is thiopental
(loading dose=10 mg/kg, maintenance dose titrated at 1-12 mg/kg/hour
continuous infusion to achieve burst suppression pattern in EEG)
36. 8. Consider surgical evacuation for mass lesions.
9. Consider decompressive hemicraniectomy in cases of malignant middle
cerebral artery infarcts
C. Sedatives and Narcotics Available Locally
Drugs Usual
Dose
Onset of
Action
Duration
of Effect
Comments Availability/Dilution
Midazolam 0.025-0.35
mg/kg
1 to 5 min 2 hours Unpredictable sedation 15 mg/3 mL amp;
5 mg/5 mL amp;
50 mg in 100 mL
NSS/D5W
Diazepam 0.1-0.2
mg/kg
Immediate 20 to 30
minutes
Sedation can be reversed with
flumazenil (0.2-1 mg at 0.2
mg/min at 20 min interval, max
dose 3 mg in one hour)
10 mg/2 mL amp;
50 mg in 250 mL
NSS/D5W
Propofol 5-50
ug/kg/min
<40 secs 10 to 15
min
Expensive (10 mg/mL) 100 mL
vial (premixed)
Ketorolac 50-100 mg
IV
1 hour 6 to 8
hours
NSAID 30 mg/mL amp
Tramadol 50-100 mg
IV
1 hour 9 hours Centrally acting synthetic
analgesic compound not
chemically related to opiates
but thought to bind to opioid
receptors and inhibit reuptake
of NE and serotonin
50 mg/ 2 mL amp;
100 mg/2 mL amp
Fentanyl 50-100
ug/hour
1-2 mins >60 min Can be easily reversed with
naloxone (0.4-2 mg IVP;
repeat at 2-3 min intervals,
max dose 10 mg)
* 110x more potent than
morphine
100 ug/2 mL;
2,500 ug in 250 mL
NSS/D5W
Morphine 2-5
mg/hour
5 mins >60 min Opioid 10 mg/mL gr 1/6;
16 mg/ mL gr 1/4
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