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MYOCARDIAL INFARCTION-MANAGEMENT
- 1. MANAGEMENT OF MYOCARDIAL INFARCTION SAMEEH SAIFUDHEEN
- 2. INTRODUCTION • Rapid development of myocardial necrosis due to a critical imbalance between O2 supply & myocardial demand. • Also known as “Heart attack”. • The most important form of IHD. • One of the major cause of mortality around the world.
- 3. CAUSES • The primary cause for MI is CORONARY ARTERY OCCLUSION. • Factors responsible are: – Coronary atherosclerosis – Vasospasm • Platelet aggregation • Cocaine abuse. – Emboli • AF • Lt. sided mural thrombus • Vegetations of inf. endocarditis
- 4. – Ischemia without detectable CA & thrombosis • Vasculitis of intramural vessels • Sickle cell disease • Amyloidosis • Vascular dissection • Low systemic BP(shock)
- 5. CLINICAL FEATURES Clinical symptoms: – May or may not present with angina pectoris. – Dyspnoea • due to pulmonary congestion caused by impaired contractility . – Diaphoresis(profuse sweating). – Rapid, weak pulse. – Anxiety.
- 6. Cardiac markers: • Enzymes – Creatine kinase(MB fraction) – Aspartate transaminase(AST) – Lactate dehydrogenase • Non-enzyme proteins – Troponin T & I – Myoglobin
- 7. Marker Abnormal activity detectable(hr) Peak value of abnormality(hr) Duration of abnormality(days) CK-MB 3-8 10-24 2-3 LD 8-12 72-144 8-14 AST 6-12 24-48 4-6 MYOGLOBIN 1-3 6-9 1 TROPONIN I TROPONIN T 3-8 3-8 24-48 72-100 3-5 5-10 CARDIAC MARKERS & TIME COURSE AFTER ONSET OF MI
- 8. WHO DIAGNOSIS OF MI Requires atleast 2 of the following criteriae: – Prolonged ischemic-type chest discomfort. – Serial ECG changes. – Elevation of cardiac markers in serum.
- 9. TREATMENT Initial treatment: 1.Morphine(2.5-5.0 mg i.v) - For sudden relief of pain & anxiety. 2.Aspirin(162-325 mg orally) - For prevention of thrombus extension, embolism, venous thrombosis. 3.O2 inhalation & assisted respiration, if needed. 4.I.V fluids - Maintain blood volume & perfusion.
- 10. Subsequent Management: – Treatment of complications: •Arrhythmias •Pump failure •Thromboembolism •Acidosis – NaHCO3 i.v infusion – Secondary prevention of further consequences & future MI.
- 11. Prevention & Treatment of Arrhythmia 1. β-blocker – Prophylactic i.v infusion • Inj. Atenolol(50 mg) – oral administration for few days • Tab. Atenolol(50 mg) – Reduce incidence of arrhythmia & mortality Note: β-blockers used early in evolving MI can reduce the infarct size & subsequent complications.
- 12. 2. Other Antiarrhythmics – Lidocaine, Procainamide for tachyarrhythmia Note: Bradycardia & Heart block may be managed with Atropine or electrical pacing.
- 13. Pump Failure – The objective is to C.O and/or filling pressure without unduly increasing cardiac work or reducing B.P. – The drugs include: • Furosemide: Reduce preload & pulm. edema. • Vasodilators: –GTN, Sod. Nitroprusside – Reduce venous return, cardiac work load. • Inotropic agents: –Dopamine, Dobutamine –Augment the pumping action of heart.
- 14. Thrombolysis & Reperfusion – First infarct patient • Inj. Streptokinase – 15,00,000 units i.v infusion over 1 hour. – Subsequent infarcts • Recombinant tissue plasminogen activator(Alteplase). • Regimen for coronary thrombolysis is 15 mg i.v followed by 0.75 mg/kg over 30 min. & 0.5mg/kg over following hour.
- 16. Adverse reactions: • Bleeding • Nausea, vomiting • Multiple micro emboli • Allergic reactions – Streptokinase is antigenic – cause anaphylaxis
- 17. Contraindications: • Haemorrhagic diathesis • Pregnancy • Recent symptoms of peptic ulcer / GI bleeding • Recent stroke (Previous 3 mths) • Recent surgery (Previous 10-14 days) • Proliferative Diabetic retinopathy • Severe uncontrolled hypertension • Aortic dissection • Acute pancreatitis
- 18. Long term Treatment The objectives include: • Prevention of remodeling & subsequent CHF. – ACE inhibitors / ARBs are of proven efficacy & afford long term survival benefit. • Prevention of future attacks. – Platelet inhibitors: – Aspirin or Clopidogrel given on long term basis are routinely prescribed.
- 19. – β blockers : – Reduces risk of reinfarction, CHF & mortality – Given for at least 2 years unless contraindicated. – Control of hyperlipidemia – Hypolipidemic drugs, especially statins. – Dietary substitution with unsaturated fats.