Abstract
In 2012, Oman Heart Association (OHA) published its own guidelines for the management of patients with unstable angina/non–ST-elevation myocardial infarction, the aim was not to be comprehensive but rather simplified and practical in order to reduce the gap between the long comprehensive guidelines and our actual practice. However, we still feel that the busy registrars and residents need simpler and direct clinical pathways or protocol to be used in the emergency departments, coronary care units and in the wards. Clinical pathways are now one of the main tools used to manage the quality in healthcare concerning the standardization of care processes. It has been shown that their implementation reduces the variability in clinical practice and improves outcomes in acute care.
Keywords: Acute coronary syndrome; Non-ST elevation; Unstable angina; Myocardial infarction; Oman Heart Association.
Introduction
Oman Heart Association has recently published the 2012 Simplified Guidelines for the Management of Patients with Unstable Angina/Non-ST Elevation Myocardial Infarction.1 The recommendations are similar to published international guidelines,2-9 but suited for local physicians in a simplified manner. Here we publish the clinical pathways which are exclusively based on these guidelines. The aim of these clinical pathways is to provide the busy physicians in Oman with even more simple and direct approach towards implementing these guidelines into clinical practice. The emphasis is on the balance of patient's risk between ischemia and bleeding and on the optimum usage of the available medications and facilities. An attempt was made to best include all the medications available in the different health organizations all over the country to really represent a national reference.
I. Risk Stratification
A. Ischemic Risk: Indicators of Early Significant Risk in Patients with Non-ST Elevation Acute Coronary Syndrome.
B. Bleeding Risk: Clinical Features Associated with Increased Bleeding Risk
1. Age ≥75 years
2. History of stroke or a transient ischemic attack
3. Prior vascular disease
4. History of bleeding
5. Renal insufficiency (CrCl <60 mL/min)
6. Hemodynamic instability
7. Anemia
8. Female gender
9. Body weight ≤60 kg
10. Hypertension
11. Diabetes mellitus
12. Use of Glycoprotein IIb/IIIa inhibitor
13. Procedural factors: Femoral artery access, Prolonged procedure,intra-aortic balloon pump, right heart catheterization.
II. Medical Therapy
A. Anti-Ischemic Therapy
1. Bed rest in coronary care unit (CCU) or monitored bed.
2. Oxygen: 2 L/min nasal cannula (titrate to keep arterial saturation >90%).
3. Nitroglycerin (NTG): 0.4 mg sublingually (SL) every 5 min for a total of 3 doses; afterwards, assess need for intravenous (IV). NTG IV – start infusion at 5 -10 μg/min, then titrate up by 10 μg/min every 5-10 min until relief of symptoms or SBP ≤100 mm Hg or maximum of 400 μg/min.
4. Morphine: If pain is not relieved. Give IV bolus 2 - 5 mg, with careful BP monitoring, repeated doses can be administered every 5 to 30 minutes. If respiratory depression develops, naloxone (0.4 to 2.0 mg IV).
5. Beta-blockers: A. Oral beta-blocker: should be initiated within the first 24 hours. Hold if: signs of HF, evidence of a low-output state, increased risk for cardiogenic shock (age >70 years, SBP <120 mm Hg, heart rate (HR) >110 bpm or HR <60 bpm, increased time since onset of NSTE ACS symptoms), or other relative contraindications to β-blockade (PR interval >0.24 s, second- or third-degree heart block, active asthma, or reactive airway disease).
Choose one:
B. IV β-Blocker (optional; reserved for patients with refractory tachycardia or refractory hypertension; otherwise, oral β-blockade is sufficient)
Choose one:
Esmolol: 3-6 mg over 1 min, then 1-5 mg/min
Propranolol: 1 mg at a rate of 0.5 mg/min, repeated if necessary at 2-5-min intervals to a maximum of 5 mg (rarely 10 mg): 0.1 mg/kg.
6. Calcium channel blockers (CCB): CCBs may be used to control ongoing or recurring ischemia-related symptoms in: (1) patients who are already receiving adequate doses of nitrates and β-blockers, (2) patients unable to tolerate adequate doses of 1 or both of these agents, (3) patients with variant angina, (4) management of hypertension in patients with recurrent unstable angina.
Choose one: (according to LV function, HR or BP)
Diltiazem: 120-360 mg daily in 3 or 4 doses
Verapamil: SR 120-240 mg once daily
Amlodipine: 5 mg daily; max. 10 mg
B. Antiplatelet Therapy
1. Aspirin: Initial Dose: 300 mg; Maintenance Dose: 75 mg PO daily for all patients lifelong, including after-stenting.
2. Clopidogrel:
Loading Dose: 600 mg;
Conservative strategy: 75 mg daily for one year.
After PCI [bare metal stent (BMS) or drug eluting stent (DES)]: 75 mg daily for one year. Higher maintenance dose of 150 mg daily for 6 days, then 75 mg daily for 1 year may be reasonable in patients not considered at high risk for bleeding.
3. Glycoprotein IIb/IIIa receptor inhibitors:
Upstream Use: Patients with ongoing and/or recurrent ischemia despite dual antiplatelet therapy (DAPT) and an anticoagulant.
During PCI: Patients having thrombotic complications or large side branch closure or unsealed dissection and patients undergoing PCI and not adequately pre-loaded with Clopidogrel.
Choose: Tirofiban Dose: Bolus-Only Strategy: 0.25 mcg/kg, or Standard regimen: IV infusion of 0.4 μg/kg/min for 30 min (reduce to 0.2 μg/kg/min for CrCl <30 mL/min), followed by IV infusion of 0.1 μg/kg/min for 18-24 hours (reduce to 0.05 μg/kg/min if CrCl <30 mL/min).
C. Anticoagulant Agents
Currently available agents in Oman are unfractionated heparin, enoxaparin and fondaparinux. Choice of anticoagulant agents depends upon the balance between the ischemic and bleeding risk.
I. Enoxaparin: Indications: For ALL patients WITHOUT the following precautions/contraindications:
1. Patients with an increased risk for bleeding, mainly:
a. Patients with a history of stroke or a transient ischemic attack
b. Renal insufficiency (CrCl <60 mL/min)
c. Age ≥75 years
d. Hemodynamic instability
2. When immediate or urgent CAG is indicated, especially if the patient will most likely undergo CABG (diabetic with widespread ST-depression and/or ST-elevation [>1 mm] in lead aVR or multiple wall motion abnormalities).
Dose: 1 mg/kg subcutaneous (SC) every 12 hours
Duration: For the duration of hospitalization or until PCI or CABG is performed.
II. Fondaparinux: Indications:
a. Patients most likely will need prolonged anticoagulation (including patients admitted to hospitals without catheterization laboratory facilities)
b. Patients with an increased risk for bleeding
c. Patients with GFR between 30 and 60 ml/min. Avoid using if CrCl <30 ml/min.
Dose: 2.5 mg SC once daily.
Duration: For the duration of hospitalization or until PCI or CABG is performed.
III. Unfractionated Heparin: Indications:
a. Severe renal insufficiency (CrCl ≤30 mL/min)
b. When immediate or urgent coronary angiography is indicated, especially if the patient will most likely undergo CABG
c. Patients with an increased risk for bleeding, if fondaparinux is not available.
Dose: 60 U/kg IV bolus (not to exceed 4000 U), followed by IV infusion of 12 U/kg/h (not to exceed 1000 U/h) to achieve goal aPTT 1.5 to 2.0 times control (approximately 50 to 70 s); check aPTT in 6 hrs and adjust heparin as indicated.
Duration: For 48 hours.
D. Anti-Remodeling Therapy
1. Angiotensin-Converting Enzyme Inhibitors: Indications:
A. ACE inhibitors SHOULD be given-unless contraindicated- within the first day of admission and continued indefinitely for NSTE ACS patients with: 1. HF, 2. LV dysfunction (LVEF <40%), 3. Hypertension, 4. Diabetes mellitus, 5. Chronic kidney disease.
B. ACE inhibitors MAY be given-unless contraindicated-during the course of hospitalization and continued indefinitely for ALL the other patients with NSTE ACS.
C. An angiotensin receptor blocker should be prescribed to those NSTE ACS patients who are intolerant of an ACE inhibitor.
2. Aldosterone Receptor Antagonist: Indications: Patients without significant renal dysfunction (estimated creatinine clearance should be >30 mL/min) or hyperkalemia (potassium should be ≤5 meq/L) who are already receiving therapeutic doses of an ACE inhibitor, have an LVEF ≤40%, and have either symptomatic HF or diabetes mellitus.
E. Antilipid Agents
Statins, in the absence of contraindications, should be given to all NSTE ACS patients regardless of baseline LDL-Cholesterol and diet modification. Therapy should be initiated or intensified to achieve an LDL-C <2.6 mmol/L or <100 mg/dL. Further titration to <1.8 mmol/L or <70 mg/dL is reasonable.
Choose: Atorvastatin 80 mg/day OD.
If triglycerides are ≥5.6 mmol/L or 500 mg/dL, Fenofibrate 150 or 300 mg OD should be started to prevent pancreatitis before LDL-lowering therapy is recommended.
III. Coronary Revascularization
In high-risk patients, a routine invasive strategy is generally preferred if there are no contraindications to coronary angiography. Among intermediate-risk patients, the benefits of an invasive approach are attenuated but still present; among low-risk patients, no benefit exists for the routine invasive approach.
A. Urgent coronary angiography/PCI: (<2 h)
1. Hemodynamic instability or cardiogenic shock.
2. Severe HF.
3. Life-threatening ventricular arrhythmias.
4. Recurrent or persistent rest angina despite intensive medical therapy.
5. New or worsening MR or new VSD.
B. Early angiography: (within 24 to 48 hours of admission)
1. Prior PCI within six months or prior CABG.
2. New or presumably new ST segment depression.
3. Elevated serum troponins.
4. Recurrent angina or ischemia at rest or with low level activity.
5. LVEF <40%.
Conclusion
Cardiovascular diseases are currently the leading cause of death in Oman, compared to western patients, our patients have a higher prevalence of cardiovascular risk factors mainly diabetes, hypertension and overweight. Although our in-hospital mortality rates are similar to the western registries, this may be misleading since our patients are about a decade younger than patients in the Western registries. We hope that these clinical pathways will help cardiac caregivers in the front lines to improve outcomes of our NSTE ACS patients.
Acknowledgements
The authors reported no conflict of interests and no funding was received for this work.
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