Chapter 3 ST-Elevation Myocardial Infarctioninitial dose should be 162 mg (Level of Evidence: A)
to 325 mg (Level of Evidence: C). Although some
trials have used enteric-coated aspirin for initial
dosing, more rapid buccal absorption occurs with
non-enteric-coated aspirin formulations.
e. Beta-blockers [2]
Class I
1 Oral beta-blocker therapy should be initiated in
the fi rst 24 hours for patients who do not have any
of the following: (1) signs of heart failure; (2) evi-
dence of a low output state; (3) increased risk* for
cardiogenic shock; or (4) other relative contraindi-
cations to beta blockade (PR interval greater than
0.24 seconds, second- or third-degree heart block,
active asthma, or reactive airway disease). (Level of
Evidence: B)
2 Patients with early contraindications within the
fi rst 24 hours of STEMI should be reevaluated for
candidacy for beta-blocker therapy as secondary
prevention. (Level of Evidence: C)
3 Patients with moderate or severe LV failure should
receive beta-blocker therapy as secondary preven-
tion with a gradual titration scheme. (Level of Evi-
dence: B)
Class IIa
It is reasonable to administer an intravenous beta
blocker at the time of presentation to STEMI patients
who are hypertensive and who do not have any of
the following: (1) signs of heart failure; (2) evidence
of a low output state; (3) increased risk* for cardio-
genic shock; or (4) other relative contraindications
to beta blockade (PR interval greater than 0.24
seconds, second or third degree heart block, active
asthma or reactive airway disease). (Level of Evi-
dence: B)
Class III
Intravenous beta-blockers should not be adminis-
tered to STEMI patients who have any of the follow-
ing: (1) signs of heart failure; (2) evidence of a low
output state; (3) increased risk* for cardiogenic
shock; or (4) other relative contraindications to beta
blockade (PR interval greater than 0.24 seconds,
second or third degree heart block, active asthma or
reactive airway disease). (Level of Evidence: A)f. Reperfusion
General concepts
See Table 3.2 for selection of reperfusion therapy.Class I
1 STEMI patients presenting to a hospital with PCI
capability should be treated with primary PCI within
90 minutes of fi rst medical contact (see Figure 3.4)
as a systems goal. (Level of Evidence: A)
2 STEMI patients presenting to a hospital without
PCI capability and who cannot be transferred to a
PCI center and undergo PCI within 90 minutes of
fi rst medical contact (see Figure 3.1) should be
treated with fi brinolytic therapy within 30 minutes
of hospital presentation as a systems goal unless
fi brinolytic therapy is contraindicated. (Level of Evi-
dence: B)Pharmacological reperfusion
See Figure 3.4 [12,13].Indications for fi brinolytic therapy
Class I
1 In the absence of contraindications, fi brinolytic
therapy should be administered to STEMI patients
with symptom onset within the prior 12 hours and
ST elevation greater than 0.1 mV in at least two con-
tiguous precordial leads or at least 2 adjacent limb
leads. (Level of Evidence: A)
2 In the absence of contraindications, fi brinolytic
therapy should be administered to STEMI patients
with symptom onset within the prior 12 hours and new
or presumably new LBBB. (Level of Evidence: A)Class IIa
1 In the absence of contraindications, it is reason-
able to administer fi brinolytic therapy to STEMI
patients with symptom onset within the prior 12- Risk factors for cardiogenic shock (the greater the number of
risk factors present, the higher the risk of developing cardio-
genic shock) are age greater than 70 years, systolic blood pres-
sure less than 120 mm Hg, sinus tachycardia greater than
110 bpm or heart rate less than 60 bpm, and increased time
since onset of symptoms of STEMI. IV indicates intravenous;
LOE, level of evidence; LV, left ventricular; PCI, percutaneous
coronary intervention; and STEMI, ST-elevation myocardial
infarction.