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Cardiovascular Care Mark Curnow HASU UCH

Cardiovascular Care Mark Curnow HASU UCH. AIMS OF SESSION. Revision Cardiac Anatomy and physiology Electrical Conduction relating to ECG Atrial Fibrillation and stroke Management of Atrial Fibrillation Monitoring on HASU Blood Pressure Management Shock. Cardiac Anatomy and Physiology.

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Cardiovascular Care Mark Curnow HASU UCH

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  1. Cardiovascular CareMark Curnow HASU UCH

  2. AIMS OF SESSION • Revision Cardiac Anatomy and physiology • Electrical Conduction relating to ECG • Atrial Fibrillation and stroke • Management of Atrial Fibrillation • Monitoring on HASU • Blood Pressure Management • Shock

  3. Cardiac Anatomy and Physiology • The heart is essentially a sophisticated muscular pump, propelling blood through the vascular system. It is fist sized & lies in the mediastinum between 2nd & 6th ribs. • The heart consists of 4 chambers – right & left atria and right & left vent. The chambers are separated by a fibro muscular septum. • A series of 4 valves lie between the chambers; • between RA & RV - tricuspid valve • between RV & pulmonary artery - pulmonary valve • between LA & LV - mitral valve • between LV & aorta - aortic valve.

  4. HEART ANATOMY/BLOOD FLOW

  5. HEART ANATOMY/ BLOOD FLOW

  6. Cardiac Cycle

  7. BLOOD FLOW AROUND THE BODY

  8. ELECTRICAL SYSTEM OF THE HEART

  9. Normal Cardiac Conduction

  10. Cardiac Conduction- Cardiac Cycle

  11. SINUS RHYTHM

  12. Cardiac Conduction and the ECG

  13. DEFINITION OF AF: Abnormal Conduction • Most commonly sustained cardiac arrhythmia • Atrial fibrillation is a type of arrhythmia in which the upper chambers of the heart (the atria) beat erratically. This erratic beating can be extremely fast (in excess of 300 beats per minute), making it difficult for blood to circulate freely from the atria into the lower chambers of the heart, known as the ventricles. • AF is irregularly irregular, having no clear identifiable P waves. Categories: • First Episode. • Paroxysmal: AF alternating with NSR, spontaneous reversion • Persistent: AF alternates with NSR but requires treatment to convert to NSR • Permanent: Inability to convert to NSR with therapy

  14. DEFINITION OF AF: Abnormal Conduction

  15. AF: CAUSES • Most cases of AF can be attributed to diseases that affect the structure of the heart over many years. • Cardiomegaly: Chronic hypertension – causing enlargement of heart muscle, in particular enlarged atrium. • Diseases of the heart valves • Pericarditis (swelling) • Pericardial effusions (fluid around the heart ) • Myocardial Infarction (damage to heart muscle) • SSS, (diseases of conduction system) • Hyperthyroidism. • Emotional stress, Nicotine, High etoh consumption

  16. AF AND STROKE: THE PROBLEM • AF is very common • At least 1.3 % UK population (600,000) have known AF • Rising to over 4% in the over 65s and 10.2% in patients over 75 years • AF is a major predisposing factor to stroke • 16,000 strokes annually in patients with AF in England • Of these approx 12,500 are thought to be attributed to AF.

  17. AF AND STROKE: THE PROBLEM • Incidence of people with AF developing stroke is: 4-6 times higher than a person with no AF. • Anticoagulants: Warfarin is superior in stroke prevention in AF. • AF strokes tend to be more severe • Warfarin reduces stroke risk by 64% • Aspirin reduces stroke risk by 22% • NICE estimate that approximately 40% of patients in whom warfarin is indicated are not receiving it, amounting to some 166,000 patients nationally

  18. HOW AF CAN LEAD TO STROKE

  19. HOW AF CAN LEAD TO STROKEConsequence of AF- Thrombus

  20. AF: TREATMENTS • Dependant on type of AF and treatment aim. • Look at history to identify any causes, Echocardiography to look at heart structure. • Pharmacological:Digoxin, amiodarone, Flecanide, Beta blockers – Sotolol, Verapamil. • Non Pharmacological: Cardioversion, Ablation. • Anticoagulation if no contraindication: For prevention of AF related complications. INR 2.o-2.5 • People with Disabling ischemic stroke in AF, aspirin 300mg for 2 weeks, then consider warfarin.

  21. ATRIAL FLUTTER • Atrial flutter, another type of atrialarrythmia originating from a single focus within the atrium (usually the right) creating a rapid atrial rate from 250-400 beats per minute. • Due to the impulse being from a single focus, the atrial pattern on the ECG is consistent. • As with Atrial Fibrillation, there is an increased risk of stroke.

  22. ATRIAL FLUTTER

  23. MONITORING ON HASU • HASU care provides the patient with 72 hours of acute monitoring. • Key element of care for people with acute stroke is the maintenance of cerebral blood flow and oxygenation to prevent further brain damage after stroke (NICE) • Cardiac Rhythm (monitor for arrhythmia) • Blood Pressure (maintain adequate CPP, the blood pressure gradient across the brain) • Respiratory rate/ Oxygen Saturations (detect and treat hypoxia) sats>95% (NICE)

  24. Arrhythmia Detection on HASUBed side monitoring • All patients on HASU monitored. • All monitors linked to a central station with continuous recording and recall facility. • Bedside Monitor vs 24hr Holter Monitor • Study (Germany) Sample of 136 patients, 29 were newly diagnosed with PAF . 16 patients diagnosed PAF on bedside monitor prior to commencement of 24hr tape. Of the remaining 13 who were diagnosed PAF from bedside monitor, 24hr tape only picked up 3. • Therefore Continuous bedside ECG monitoring is more sensitive than 24-hour Holter ECG for PAF detection in acute stroke/TIA patients • Cerebrovasc Dis. 2010;30(4):410-7.

  25. BLOOD PRESSURE MANAGEMENT • Blood pressure monitoring is critical. • Anti-hypertensive treatment in people with acute stroke is recommended only if there is a hypertensive emergency with one of more of the following: • hypertensive encephalopathy , hypertensive nephropathy • hypertensive cardiac failure/myocardial infarction • aortic dissection. Pre-eclampsia/eclampsia • Intracerebral haemorrhage with systolic blood pressure over 200 mmHg. (NICE) • ESO (2009), Deem Hypertensive emergency as BP > systolic 220 and diastolic >120.

  26. BLOOD PRESSURE MANAGEMENT • Patients suitable for thrombolysis should have BP no higher than 185/110. (NICE) • Avoid drops in blood pressure – maintain an adequate cerebral perfusion pressure. Usually maintained by cerebral blood flow auto regulation. • An intracranial event can affect auto regulation, and an increased ICP and a decreased MAP can lower CPP which in turn cause secondary damage to brain.

  27. BLOOD PRESSURE TREATMENTS • Hypertension: • IV GTN: Mainly used in angina/ acute LVF. Causes dilation of smooth muscle within veins and arteries. Leading to reduced myocardial workload and increased myocardial perfusion. Causes hypotension. Can cause throbbing headache. • Labetolol Beta Blocker. Blocks beta adrenoreceptors within the body. Reduces blood pressure by altering baroreceptors reflex sensitivity and block peripheral adrenoreceptors. They also cause reduction in heart rate. CHHIPS (2009)

  28. SHOCK • Types: Cardiogenic: Pump Failure. Diminished cardiac output which severely impairs tissue perfusion. Causes: Myocardial Infarction / Ischemia End stage Cardiomyopathy Signs : Cold, pale clammy skin Hypotension. Tachycardia. Reduced urine output. Confusion. Treatment:Fluid challenge. Inotropes. IABP. Septic Shock Hypovoleamic.

  29. CONCLUSION Remember: • Close monitoring is essential on HASU • Familiarise yourself with the monitor (don't be scared of it) • Observe cardiac rhythm for changes, especially irregularities. • Monitor Hemodynamics, agree parameters with team and manage changes early. • Knowledge leads to empowerment. Always aim to learn from your experiences by questioning, then tell someone else!!

  30. THANK YOU

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