Chest pain with ischemic profile: chest tightness or anterior chest at rest or exercise radiating to the neck, left arm, or both during >1min with or without adrenergic manifestations.

Chest pain with non-typical ischemic profile: does not meet the criteria of pain with ischemic profile, however suggesting myocardial ischemia as tightness in lower jaw, anterior neck, epigastrium, etc.

Previous angina: chest pain with ischemic profile, characteristic or not, or equivalent prior to current index event.

Equivalent of ischemia: this kind of ischemia clinical expression has different age-related variations. Ventricular arrhythmias, first event of heart failure without a clear etiology, sudden pulmonary edema, dyspnea at rest or exercise, syncope, mental confusion, asthenia, adynamia, anorexia associated with objective evidence of ischemia, micro, macronecrosis or both (Appendix B).12

Nonspecific: ST depression <0.05mV or negative asymmetrical T wave <0.2mV, ventricular hypertrophy, pacemaker rhythm.13–15

ST depression: depression >0.05mV in two underlying leads or negative symmetrical T wave >0.2mV.13,16

Transient ST elevation: J point positive slope (>0.2mV in V1–V3 and >0.1mV in other leads) in two underlying leads with ST normalization or residual negative deep T wave, spontaneously or secondary therapeutic action.13,16

Persistent ST elevation: positive slope at J point (>0.2mV in V1–V3 and >0.1mV in other leads) in two underlying leads.13,16

According to the Mexican electrocardiography school in the context of a left bundle branch block bundle the presence of Q wave in DI, aVL, V5 or V6 leads this suggests a septal infarction; loss of QRS voltage with Q wave in V4, V5 and V6 may correspond to an anteroseptal infarction. The presence of RS or rs with negative T wave (intracavitary lead) in V4–V6 could translate a left ventricular transmural infarction. In Appendix C criteria of Sodi Pallares and Sgarbossa can be observed.14,15

J point moving in the opposite direction to the predominant QRS deflection (negative in the presence of R wave, positive in the presence of S wave) with a magnitude of displacement up to 5mm is required. The ST and T wave will show the same polarity, behaving as a single pathophysiological entity. A ST elevation in an acute myocardial infarction associated with this conduction disturbance is divided into concordant and discordant. ST elevation ≥0.1mV (1mm) in leads with R wave or ST negative slope ≥0.1mV in leads V1–V3 (with dominant S wave) is called concordant. ST elevation 0.5mV (5mm) in leads with S wave is called discordant.15

• a)

  Normal or nonspecific

• b)

  Negative ST depression

• c)

  Transient ST elevation

• d)

  Persistent ST elevation

• a)

  History of chest pain or discomfort with ischemic profile or not, ≥20min.

• a.

  Equivalent associated with persistent ST elevation and abnormal biomarkers.

• b)

  ECG with persistent ST elevation >1mm in at least two underlying leads or left bundle branch block or tall R wave (40ms) in V1 and V2 leads associated with ST depression V1–V3 and right leads.

• c)

  Elevation of cardiac biomarkers serum levels (preferably troponin) with at least one value above the upper reference limit of 99th percentile.

• d)

  Two-dimensional echocardiogram demonstrating new or presumably new abnormality of regional or global mobility.

Ischemia evidence: Demonstration and objective documentation of myocardial ischemia by echocardiography or nuclear medicine.13,16

Uncomplicated: normal blood pressure without left ventricular dysfunction signs, EF >40%, brain natriuretic peptide type-B (BNP) <100pg/dL, or both.

Complicated with left ventricular dysfunction without clinical manifestations: normal blood pressure or lower limits, no third left ventricular heart sound, EF <40%, or both, BNP >100pg/dL, or both.

Complicated with ventricular dysfunction with clinical manifestations: acute pulmonary edema or pre-cardiogenic shock suspicion (borderline blood pressure, hypotension, or both, clinical expression of -renin-angiotensin-aldosterone-vasopressin system activity, oliguria, delayed capillary refill, lower lobes crackling rales, EF <30%, BNP >600pg/dL.

• I: without left ventricular dysfunction signs

• II: left ventricular third heart sound, basal crackling rales, or both

• III: acute pulmonary edema

• IV: cardiogenic shock

Pulmonary edema: increased work of breathing with or without severe desaturation (saturation <90%), left ventricular gallop or tachycardia, crackling rales or wheezes >50% in lung fields. Chest X-ray with interstitial, alveolar, or mixed pulmonary edema.

Cardiogenic shock: (1) systolic blood pressure <90mmHg without support of vasoactive substances or 100mmHg with vasopressors use; (2) clinical, radiographic expression of pulmonary venocapillary hypertension, or both; (3) signs of peripheral vascular hypoperfusion; (4) metabolic acidosis; (5) cardiac index <2.2L/min/m2; (6) pulmonary capillary pressure >18mmHg; and (7) arteriovenous oxygen difference >5.5ml/dL.

Variables predictors of poor in-hospital outcome according to odds ratio (OR) and confidence intervals (CI) were selected from RENASICA II3 multivariate analysis: diabetes (OR 3.1, CI 1.94–5.06, and p<0.0001); ischemic chest pain >20min (OR 2.3, CI 1.43–3.69, and p 0.0006); heart failure history (OR 2.2, CI 1.16–4.23, and p 0.01); age >65 years old (OR 1.8, CI 1.27–2.67, and p 0.001); positive troponin (OR 1.7, CI 1.05–0.97, and p 0.02); and ST depression >3 leads (OR 1.6, CI 1.08–2.61, and p 0.02).

Electrocardiographic: ST decreased >70% in the most meaningful leads in an ECG taken 90min after pharmacological fibrinolysis the fibrinolytic regarding index event ECG.13

Major bleeding: Fatal bleeding, documented retroperitoneal, intracranial, or intraocular bleeding, bleeding resulting in hemodynamic compromise requiring specific treatment, bleeding requiring surgical intervention or decompression of a closed space to control the event, any transfusion >1 unit red packed cells or whole blood or a hemoglobin drop >3g/dL or more or hematocrit >10%.17

Minor bleeding: microscopic hematuria not associated with trauma by ureteral procedures. Prolonged or recurrent epistaxis requires plugging or intervention; gastrointestinal or subconjunctival bleeding or hemoptysis. Hematoma >5cm related with length in-hospital stay or new hospitalization. Bleeding decreasing hemoglobin drop <3g/dL or considering duration requires protamine sulfate.17

Fibrinolysis inducing hypotension: Blood pressure ≤90/60mmHg during or at the end of the fibrinolytic infusion without other apparent reason.

Primary angioplasty: with or without stent; without prior or concomitant fibrinolytic therapy or glycoprotein IIb/IIIa use.13

Rescue angioplasty: coronary intervention in patients after unsuccessful fibrinolytic therapy (persistent chest pain, ST elevation or decrease <70%, or both on an ECG at 90min).

Residual lesion: ≤30% and epicardial TIMI flow 3.

Suboptimal: Residual lesion: >30% and epicardial TIMI flow 2.

Failed: obstructive residual lesion ≥70% and TIMI flow 0–2 or when the guide wire fails through the atherosclerotic lesion.13

• TIMI 0: total absence of flow

• TIMI 1: slight penetration of the contrast medium without reaching the obstructive lesion or the terminal portion of the vessel

• TIMI 2: penetration of the contrast medium reaches the obstructive lesion but not exceeded or the entire artery and typically presents with low flow

• TIMI 3: normal coronary flow.13

• TIMI 0: total absence of flow

• TIMI 1: slight penetration of the contrast medium without reaching the obstructive lesion or the terminal portion of the vessel

• TIMI 2: penetration of the contrast medium reaches the obstructive lesion but not exceeded or the entire artery and typically presents with low flow

• TIMI 3: normal coronary flow.13

• TMPG 0: No or minimal blush

• TMPG 1: Stain present. Blush persists on next injection

• TMPG 2: Dye strongly persistent at end of washout. Gone by next injection

• TMPG 3: Normal ground glass appearance of blush. Dye mildly persistent at end of washout.18

• TMPG 0: No or minimal blush

• TMPG 1: Stain present. Blush persists on next injection

• TMPG 2: Dye strongly persistent at end of washout. Gone by next injection

• TMPG 3: Normal ground glass appearance of blush. Dye mildly persistent at end of washout.18

Recurrent ischemia: new chest pain episode with ischemic profile (treatment with two antiischemic drugs at least) >5min, with ST dynamic ECG changes, and without myocardial necrosis.

Reinfarction: Two or more of the following criteria: (1) chest pain with ischemic profile ≥20min; (2) new ST elevation (>0.1mV) in two underlying leads or new Q wave; (3) CK–MB new elevation ≥50% normal high upper limit or ≥50% of baseline.

Cardiogenic shock: (1) systolic blood pressure <90mmHg without support of vasoactive substances, or 100mmHg with vasopressors; (2) clinical, chest X-ray expression of pulmonary venocapillary hypertension, or both; (3) signs of peripheral vascular hypoperfusion manifested by oligoanuria <1ml/kg/h; (4) metabolic acidosis; (5) cardiac index <2.2L/min/m2; (6) pulmonary capillary pressure >18mmHg; and (7) arteriovenous oxygen difference >5.5ml/dL.

Cardiovascular death: Secondary to acute coronary ischemic event index or new in-hospital event or during follow-up.

Acute cerebrovascular disease: Loss of neurological function secondary to an ischemic, embolic or bleeding event. Ideally, objective evidence through computerized axial tomography or magnetic resonance must be obtained.

Ventricular fibrillation: Chaotic rhythm with total absence of isoelectric line and total absence of atrial contraction.

Ventricular tachycardia: Four or more consecutive ventricular extrasystoles; is considered as not sustained <30s or sustained >30s.

Hyperlipidemia: Cholesterol >200mg/dL or normal levels with treatment.

Previous infarction: Necrosis demonstration by ECG, echocardiography, nuclear medicine or nuclear magnetic resonance.

Mitral insufficiency: Regurgitation murmur radiating to the axilla and objective demonstration by echocardiography and ventriculography.

Renal failure: Serum creatinine >2.0mg/dL.

Renal dysfunction

Moderate: 50–30mL/min

Severe: <30mL/min

Cocroft Gault formula

Serum creatinine clearance=(140−Age expressed in years)×(Weight expressed in kilograms)

Serum creatinine (mg/dL)×72

Cardiac arrest: Electromechanical or asystole dissociation.

Pericarditis: Suggestive chest pain with or without pericardial rub and suggestive ECG changes.

Sepsis: Toxi-infectious medical condition characterized by multiple organ failure, incipient or advanced hematological alterations and clinical data of tisular hypoperfusion.

Pulmonary embolism: High risk: sudden dyspnea associated with chest pain or syncope with echocardiographic right ventricular dysfunction, BNP >100pg/d, or both, dimer D >500, and objective demonstration by radionuclide lung scintigraphy V/P, or pulmonary angiography, or CT angiogram, or magnetic resonance.19

Pulmonary embolism: common risk: sudden dyspnea, tachycardia, pleural pain, without right ventricular dysfunction by ECHO, BNP <100pg/dL, or both, dimer D >500, and objective demonstration by radionuclide lung scintigraphy V/P, or pulmonary angiography, or CT angiogram, or magnetic resonance.19