Acute Coronary Syndromes Chapter 28

About This Presentation

Title:

Acute Coronary Syndromes Chapter 28

Description:

ST-elevation myocardial infarction: A report of the ACC/AHA Task Force on ... However, only a small fraction of these abnormalities cause symptomatic ischemia. ... – PowerPoint PPT presentation

Number of Views:207

Avg rating:3.0/5.0

Slides: 103

Provided by: mandy6

Category:

more less

Transcript and Presenter's Notes

Title: Acute Coronary Syndromes Chapter 28

1
Acute Coronary SyndromesChapter 28
Chapter 18

Pharmacotherapy A Pathophysiologic Approach
The McGraw-Hill Companies

2
Abbreviations

ACC American College of Cardiology
ACE angiotensin-converting enzyme
ACS acute coronary syndrome
ACUITY Acute Catheterization and Urgent
Intervention Triage
Strategy
ADP adenosine diphosphate
AHA American Heart Association
ARB angiotensin receptor blocker
ASPECT Antithrombotics in Secondary Prevention
of
Events in Coronary Thrombosis
CK creatine kinase

3
Abbreviations

CABG coronary artery bypass graft
CHD coronary heart disease
CVD cardiovascular disease
DHA docosahexaenoic acid
ECG electrocardiogram
EF ejection fraction
EPA eicosapentaenoic acid
EPHESUS Eplerenone Post-Acute Myocardial
Infarction
Heart Failure Efficacy and Survival Study
ExTRACT Enoxaparin versus Unfractionated Heparin
with
Fibrinolysis for ST-elevation Myocardial
Infarction

4
Abbreviations

HIT Heparin induced thrombocytopenia
ICH intracranial hemorrhage
INR international normalized ratio
IV intravenous
LDL low-density lipoprotein
LMWH low-molecular-weight heparin
LV left ventricular
LVEF left ventricular ejection fraction
MADIT Multicenter Automatic Defibrillator
Implantation Trial
MB myocardial band
MI myocardial infarction

5
Abbreviations

NCEP National Cholesterol Education Program
NICE-SUGAR Intensive Versus Conventional Glucose
Control
in Critically Ill Patients Trial
NRMI National Registry of Myocardial Infarction
NSAID nonsteroidal antiinflammatory drug
NSTE nonST-segment elevation
OASIS Organization for the Assessment of
Strategies for
Ischemic Syndromes
OAT Occluded Artery Trial
PCI percutaneous coronary intervention
TIMI Thrombolysis in Myocardial Infarction
UFH unfractionated heparin
WARIS Warfarin Re-Infarction Study

6
Recommendations Evidence

Strength of recommendations
A good, B moderate, C poor
Quality of evidence
1 more than 1 properly randomized, controlled
trial
2 at least 1 well-designed clinical trial with
randomization from cohort or case-controlled
analytic studies or dramatic results from
uncontrolled experiments or subgroup analyses
3 opinions of respected authorities, based on
clinical experience, descriptive studies, or
reports of expert communities

7
Key Concepts

Acute coronary syndromes (ACS) typically caused
by atherosclerotic plaque rupture subsequent
clot formation
Risk-stratify patients with suspected ACS based
on ECG, symptoms lab tests
Early reperfusion with PCI or fibrinolytic
recommended for patients with ST-segment
elevation myocardial infarction (STEMI)

8
Key Concepts

High-risk NSTE (non ST-segment elevation) ACS
patients should have early coronary angiography
revascularization
ACS patients should also receive early therapy
with intranasal oxygen, aspirin, clopidogrel,
nitroglycerin, ß-blocker an anticoagulant
MI patients should receive indefinite therapy
with ASA, ß-blocker, ACE inhibitor or ARB
Selected patients should receive statin,
clopidogrel or anticoagulation

9
Epidemiology

1.5 million American experience an ACS every year
220,000 of those will die of an MI
Chest discomfort 2nd most frequent reason for ED
visits
CHD leading cause of premature disability in the
US
2007 cost of CHD 151.6 billion

Anderson JL, Adams CD, Antman EM, et al. ACC/AHA
2007, Guidelines for the management of patients
with unstable angina/non ST-elevation myocardial
infarction A report of the ACC/AHA Task Force on
Practice Guidelines Circulation
2007116803877.
American Heart Association. Heart Disease and
Stroke Statistics2007, Update. Dallas, TX
American Heart Association, 2007.
10
Epidemiology

In hospital death rates
STE ACS 4.6
NSTE ACS 2.2
Lower mortality rates for patients treated with
reperfusion therapy (fibrinolytics or PCI)
Mortality rates higher in women elderly patients

American Heart Association. Heart Disease and
Stroke Statistics2007, Update. Dallas, TX
American Heart Association, 2007.
11
Etiology

Atherosclerosis starts early in life
Inflammation plays key role
Several factors contribute to evolution of
endothelial dysfunction formation of fatty
streaks arteries that lead to atherosclerotic
plaques

HTN
age
male gender
tobacco use

DM
obesity
dyslipidemias

12
Pathophysiology

ACSs result from myocardial ischemia due to
imbalance between myocardial O2 demand supply
usually due to occluded coronary artery thrombus
STEMI, NSTEMI, unstable angina fall under this
heading
unstable angina does not produce detectable
biochemical marker levels

13
Comparison of ACSs
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
14
CAD Causes
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
15
Plaque Rupture Clot Formation

gt 90 of ACSs caused by rupture or erosion of an
atherosclerotic plaque
Plaques likely to rupture
those that occlude lt 50 of the lumen
eccentric shape
thin fibrous cap with large fatty core
Clots form on top of ruptured plaques partially
or fully occlude the artery lumen
Exposure of collagen tissue factor from the
plaque induces platelet adhesion activation
promotes release of vasoactive substances

16
Atheroma Production
A normal muscular artery. The adventitia, or
outermost layer of the artery, consists
principally of recognizable fibroblasts
intermixed with smooth muscle cells loosely
arranged between bundles of collagen and
surrounded by proteoglycans. It is usually
separated from the media by a discontinuous sheet
of elastic tissue, the external elastic lamina.
B platelet aggregates, or microthrombi, form as
a result of adherence of the platelets to the
exposed subendothelial connective tissue.
Platelets that adhere to the connective tissue
release granules whose constituents may gain
entry into the arterial wall. Platelet factors
thus interact with plasma constituents in the
artery wall and may stimulate events shown in the
next illustration C smooth muscle cells migrate
from the media into the intima and actively
multiply within the intima. Endothelial cells
regenerate in an attempt to re-cover the exposed
intima, which thickens rapidly owing to smooth
muscle proliferation and formation of new
connective tissue.
17
Plaque Rupture Clot Formation

Platelet activation changes on platelet GP
IIb/IIIa receptors lead to formation of fibrin
bridges
inclusion of many platelets creates white clots
more common in NTSE ACS
incomplete artery occlusion
Coagulation cascade activated fibrin traps RBCs
clots have red appearance
more common in STE ACS
more likely to completely occlude vessels
Myocardial ischemia can result from microthrombi
embolization lead to necrosis

18
Ventricular Remodeling

Changes in size, shape function of the left
ventricle (LV)
results in HF
ACE inhibitors, ARBs, ß-blockers, aldosterone
antagonists
slow down or reverse remodeling
improve chance of survival

19
Complications

Cardiogenic shock
5 to 6 of STEMI patients
2 of NSTE ACS
mortality rate 60
Others
heart failure
valve dysfunction
arrhythmias
heart block

pericardititis
stroke
venous thromboembolism
LV free-wall rupture

20
Symptoms

Midline anterior anginal chest pain
Severe new-onset angina
Increasing angina gt 20 minutes
Pain may radiate
left arm
jaw
back
Nausea, vomiting, diaphoresis, shortness of
breath
Women, diabetics, elderly patients may have
atypical or no symptoms

21
Electrocardiogram

12-lead ECG should be done within 10 min of ED
arrival
Key findings indicating myocardial damage
ST-segment elevation
ST-segment depression
T-wave inversion

22
Biochemical Markers

Evaluate troponin CK MB to confirm MI
released in response to myocardial necrosis
3 measurements taken over the 1st 12 to 24 hrs
MI diagnosis
gt 1 one troponin value greater than MI decision
limit set by lab
or
2 CK MB values greater than MI decision limit set
by lab

23
NSTEMI
STEMI
24
STEMI
25
(No Transcript)
26
(No Transcript)
27
Risk Stratification

Treat STEMI patients as fast as possible
NST ACS patients stratified based on clinical
presentation, lab findings
Risk categories
high
medium
low
TIMI Thrombolysis In Myocardial Infarction
Treatment based on TIMI score

28
aTroponin I, troponin T,
or creatinine kinase MB greater than the MI
detection limit.
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
29
Treatment Goals

Restore blood flow to prevent infarct expansion
MI
Prevent death, complications
Prevent coronary artery reocclusion
Relieve ischemic chest discomfort
Maintain normoglycemia

30
2006 American College of Cardiology/American
Heart Association STE and NSTE MI Performance
Measures
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
31
2006 American College of Cardiology/American
Heart Association STE and NSTE MI Performance
Measures
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
32
Nonpharmacologic Therapy

STEMI patients should receive either fibrinolysis
or primary PCI within 3 hrs of symptom onset
PCI preferred treatment in capable centers
High risk NST ACS patients may undergo PCI or
CABG
early invasive strategy

33
Primary PCI

A meta-analysis comparing fibrinolysis with PCI
indicated lower mortality rate in PCI patients
PCI opens arteries better than fibrinolytics
reduces risk of major bleeding, intracranial
hemorrhage (ICH)
better side effect profile
Door-to-balloon time
time of hospital presentation to time occluded
artery is opened should be lt 90 min

34
Additional Testing

Echocardiogram to determine LV function
LV function best predictor of mortality after MI
LVEF lt 40 higher risk of death
Implantable cardioverter defibrillator (ICD) may
be placed in patients with ventricular
tachycardias
May perform stress testing in moderate or low
risk patients to diagnose CAD
Draw fasting lipid panel

35
Early Pharmacotherapy for ACS

Intranasal oxygen (if O2 saturation lt 90)
Sublingual NTG (IV if indicated)
ß-blocker (PO)
Anticoagulation
UFH, enoxaparin, etc.
Morphine can be given for refractory anginal pain
Fibrinolytics in STE ACS only

36
(ACE, angiotensin-converting enzyme ACS, acute
coronary syndrome ARB, angiotensin receptor
blocker CABG, coronary artery bypass graft
surgery IV, intravenous NTG, nitroglycerin
PCI, percutaneous coronary intervention SC,
subcutaneous SL, sublingual UFH, unfractionated
heparin.) aAlthough recommended by the 2004
American College of Cardiology and American Heart
Association practice guidelines, no dose
recommendation is given. bSee Table 184 for
dosing and specific types of patients who should
not receive enoxaparin or IV NTG.)
37
Pharmacotherapy for STE ACS

In the ED
sublingual or IV NTG
ASA
ß-blocker
unfractionated heparin (UFH) or enoxaparin
morphine PRN
fibrinolysis

38
Pharmacotherapy for STE ACS

All patients at discharge
ASA
ß-blocker
statin/lipid lowering therapy
ACE inhibitor or ARB
Select patients
aldosterone antagonists
clopidogrel
warfarin

39
(No Transcript)
40
Pharmacotherapy for NSTE ACS

Similar to STE ACS treatment with a few
exceptions
fibrinolytic therapy contraindicated
GP IIb/IIIa receptor blockers administered to
high-risk patients
no established quality performance measures for
STE ACS patients with unstable angina

41
Fibrinolytics

Indicated in STEMI patients who present within 12
hours of symptom onset have gt 1 mm of STE on
EKG (Class 1)
not indicated in NSTE ACS
CI in patients with high bleeding risk
Fibrinolytic therapy controversial in patients gt
75 yr

42
Contraindications to Fibrinolysis

Absolute contraindications
active internal bleeding (not including menses)
previous intracranial hemorrhage at any time
ischemic stroke within 3 months
intracranial neoplasm
structural vascular lesion (e.g., arteriovenous
malformation)
suspected aortic dissection
significant closed head or facial trauma within 3
months

43
Contraindications to Fibrinolysis

Relative contraindications
uncontrolled HTN (BP gt 180/110 mm Hg)
ischemic stroke gt 3 months
dementia
intracranial pathology
current anticoagulant use
bleeding diathesis
traumatic or prolonged CPR (gt 10 min)
major surgery (lt 3 wks)

44
Contraindications to Fibrinolysis

Relative contraindications
noncompressible vascular puncture
recent liver biopsy
carotid artery puncture
recent internal bleeding (within 2 to 4 wks)
for streptokinase administration, previous
streptokinase use (gt 5 days) or prior allergic
reaction
pregnancy
active peptic ulcer
history of severe, chronic, poorly controlled HTN

45
Comparison of Fibrinolytic Agents
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
46
Fibrinolytics

Fibrin specific agents (alteplase, tenecteplase,
reteplase) preferred over non-fibrin specific
agents (streptokinase)
studies show lower mortality for fibrin specific
agents
Alteplase most indications difficult to dose
bolus followed by weight based infusion
Tenecteplase single weight-based dose
Reteplase 2 fixed doses (no weight adjustment)

47
Fibrinolytics

ICH major bleeding most serious side effects
ICH rates higher in fibrin specific agents
systemic bleeding other than ICH higher with
streptokinase
Door-to-needle time lt 30 min
quality performance measure

48
Anti-platelet Agents

ASA
Thienopyridines
clopidogrel preferred agent
ticlopidine associated with neutropenia
requires close CBC monitoring during 1st 3 months
of treatment
GP IIa/IIIa Receptor Inhibitors
abciximab
eptifibatide
tirofiban

49
Aspirin (ASA)

Preferred anti-platelet agent for treatment for
all ACSs (Class I)
Start during 1st 24 hrs of hospitalization
Studies show lower 35-day vascular mortality
compared to placebo
Dosing 162 to 325 mg PO loading dose, then 75
to 162 mg PO daily
maintenance dose should be higher in patients
with intracoronary stent for the 1st 1 to 6
months depending on type of stent
Continue indefinitely

50
Aspirin (ASA)

Irreversible inhibition of platelet
cycloxygenase-1 (COX-1)
may have anti-inflammatory effects
Monitor for bleeding
Contraindications
hypersensitivity
active bleeding
severe bleeding risk

51
Clopidogrel

Alternative for patients with ASA allergy (Class
1)
STE ACS
added to ASA in patients undergoing primary PCI
(Class 1)
based on current data, clopidogrel should be
given to patients treated by fibrinolytics or
those receiving no revascularization with
PCI/CABG (Class 1)
NSTE ACS
recommended for most patients in combination with
ASA for up to 12 months (Class 1)

52
Clopidogrel

Blocks ADP2Y12 receptors on platelets
prevents fibrin binding
Dosing
300 to 600 mg PO loading dose
followed by 75 mg PO daily
Duration of therapy depends on type of stent

53
Clopidogrel

Contraindications
hypersensitivity
active bleeding
severe bleeding risk
Adverse effects
bleeding
nausea
vomiting
diarrhea

54
GP IIb/IIIa Receptor Inhibitors

STE ACS
abciximab indicated for patients undergoing 1
PCI in combination with ASA, clopidogrel, UFH
(Class 2a)
eptifibatide also FDA approved for this
indication (Class 2b)
use in patients not undergoing PCI not
recommended

55
GP IIb/IIIa Receptor Inhibitors

NSTE ACS
tirofiban or eptifibatide recommended for
high-risk patients not undergoing
revascularization or patients with continued
ischemia despite treatment with ASA, clopidogrel
an anticoagulant (Class 2a)
abcixicmab or eptifibatide recommended for
patients undergoing PCI (Class 1)

56
GP IIb/IIIa Receptor Inhibitors

Prevents cross linking of platelets through
inhibition of GP IIb/IIIa receptors
May help with early opening of coronary arteries
Contraindications
active bleeding
thrombocytopenia
history of stroke
Adverse effects
bleeding
immune mediated thrombocytopenia

57
(No Transcript)
58
(No Transcript)
59
(No Transcript)
60
Clinical Controversies

Early up stream administration of a GP IIb/IIIa
inhibitor vs delayed selective therapy at time of
PCI in NSTE ACS patients
A recent study showed no statistical difference
in ischemic events but more bleeding events when
the drug was given prior to angiography
short administration times
statistical power may not have been sufficient
Timing of GP IIb/IIIa administration in NSTE ACS
patients undergoing angiography remains
controversial

Stone GW, Bertrand ME, Moses JW, et al. Routine
upstream initiation vs. deferred selective use of
glycoprotein IIb/IIa inhibitors in acute coronary
syndromes The ACUITY Timing Trial.
JAMA.2007297591-602.
61
Anticoagulants

Heparins
unfractionated heparin (UFH)
low molecular weight heparin (LMWH)
enoxaparin, dalteparin
Factor X-A Inhibitor
fondaparinux
Direct Thrombin Inhibitors
bivalirudin reversible binding
lepirudin irreversible binding
argatroban reversible binding

62
Unfractionated Heparin (UFH)

1st line anticoagulant for STE ACS PCI
administered with a fibrin selective fibrinolytic
(Class 1)
NSTE ACS
preferred anticoagulant following angiography in
patients undergoing CABG (Class 1)
option for patients undergoing planned early
angiography revascularization (Class 1)
may be used in patients in whom an initial
conservative strategy is planned (Class 1)

63
Unfractionated Heparin (UFH)

Binds antithrombin inhibits clotting factors Xa
IIa (thrombin)
IV bolus followed by infusion, adjust according
to aPTT or antifactor Xa levels
Can be used in patients with renal dysfunction
Continue 48 hrs in patients who will be on
warfarin, otherwise discontinue immediately after
PCI

64
Heparin
65
Unfractionated Heparin (UFH)

Contraindications
history of heparin induced thrombocytopenia (HIT)
active bleeding
severe bleeding risk
recent stroke
Adverse effects
bleeding
HIT

66
Enoxaparin

STEMI
not studied in primary PCI (Class 2b as
alternative to UFH)
NSTEMI ACS
option for patients undergoing planned early
angiography and revascularization (Class 2a)
UFH recommended over enoxaparin or fondaparinux
(Class 1b)
may be used in patients in whom an initial
conservative strategy is planned (Class 1)
fondaparinux recommended over enoxaparin (Class
1a)
enoxaparin recommended over UFH (Class 1b)

Schünemann HJ, Hirsh J, Guyatt G, et al.
Executive Summary American College of Chest
Physicians Evidence-Based Clinical Practice
Guidelines (8th Edition). Chest. 200813371-109.
67
Enoxaparin

Binds antithrombin, inhibits factors Xa IIa
ExTRACT trial (Enoxaparin versus Unfractionated
Heparin with Fibrinolysis for ST-Elevation MI)
n20,506
enoxaparin 30 mg IV bolus, 1 mg/kg SQ 15 min
later then every 12 hr (dose ? for age gt 75 yr,
renal dysfunction)
UFH 60 units/kg IV bolus (maximum 4000 units)
followed by 12 units/kg/hr infusion with
adjustments to maintain aPPT 1.5 to 2.0 times the
control value
17 risk reduction for death or nonfatal MI in
patients on enoxaparin compared to UFH

Antman EM, Morrow DA, McCabe CH, et al.
Enoxaparin versus unfractionated heparin with
fibrinolysis for ST-elevation myocardial
infarction. N Engl J Med 200635414771488.
68
Enoxaparin

Shorter chain length compared to UFH
more predictable effects
Contraindications
active bleeding, severe bleeding risk
history of HIT
recent stroke
CrCl lt 15 ml/min
avoid in CABG patients
Dose 1 mg/kg every 12 hrs (renal adjustment
required)
Adverse effects bleeding HIT (lesser extent
than UFH)

69
Fondaparinux

Inhibits factor Xa
less likely to cause HIT than UFH, LMWH
STE ACS
alternative to UFH in patients not undergoing
reperfusion (Class 1) or receiving fibrinolytics
(Class 2b)
not recommended for use alone in 1 PCI (Class 1a)

Schünemann HJ, Hirsh J, Guyatt G, et al.
Executive Summary American College of Chest
Physicians Evidence-Based Clinical Practice
Guidelines (8th Edition). Chest. 200813371-109.
70
Fondaparinux

NSTE ACS
option for patients undergoing planned early
angiography revascularization with PCI
option for patients in whom an initial
conservative strategy is planned
preferred agent for patients with high risk for
bleeding (Class 1)

71
Direct Thrombin Inhibitors

NSTE ACS
bivalirudin option in patients undergoing
planned early angiography revascularization
(Class 1)
Inhibit clot-bound circulating thrombin
Does not bind plasma proteins
More predictable response than UFH
Antiplatelet activity

72
Direct Thrombin Inhibitors

ACUITY trial (Acute Catheterization and Urgent
Intervention Triage StrategY)
Moderate to high risk patients with ACS
undergoing invasive intervention (n13,819)
evaluated after 1 year
3 groups
bivalirudin
bivalirudin GP IIb/IIIa inhibitor
heparin/enoxaparin GP IIb/IIIa inhibitor
Outcomes death, MI, unplanned revascularization

White HD, Ohman EM, Lincoff AM, et al. Safety and
efficacy of bivalirudin with and without
glycoprotein IIb/IIIa inhibitors in patients with
acute coronary syndromes undergoing percutaneous
coronary intervention 1-year results from the
ACUITY (Acute Catheterization and Urgent
Intervention Triage strategy) trial. J Am Coll
Cardio. 200852(10)807-14.
73
Direct Thrombin Inhibitors

ACUITY results
no difference in incidence of ischemic events or
mortality at 1 year between the 3 regimens
43 relative risk reduction for major bleeding in
bivalirudin monotherapy group at 30 days compared
to UFH or enoxaparin GP IIb/IIIa inhibitor
bilvalirudin alone can replace UFH or enoxaparin
GP IIb/IIIa inhibitor in moderate to high risk
ACS patients undergoing PCI

Given to both STE NSTE ACS patients ischemic
chest pain relief (Class 1)
No mortality benefit in acute MI
Symptom relief only
Dose 0.4 mg SL tab every 5 min up to 3 times
if chest pain persists, IV nitroglycerin may be
indicated for 24 hr after relief of ischemia

75
Nitrates

Promote release of nitric oxide producing
vasodilation myocardial ischemia relief
venodilation lowers myocardial O2 demand
preload
arterial vasodilation may lower BP
Contraindicated in patients with recent
phoshodiesterase-5 inhibitor use
Adverse effects

headache
flushing

hypotension
tachycardia

76
ß-Blockers

Cardioselective
atenolol, betaxolol, bisoprolol, metoprolol,
nebivolol
Nonselective
nadolol, propranolol, timolol
Mixed a- ß-blockers
carvedilol, labetolol
IV only
esmolol

77
ß-Blockers

Should be given early to STE ACS NSTE ACS
patients in the absence of contraindications
(Class 1)
continue indefinitely
quality care indicator for MI patients
IV ß-blockers only given to hemodynamically
stable patients without signs/symptoms of
decompensated HF
risk of cardiogenic shock

78
ß-Blockers

Competitive blockade of myocardium ß1 receptors
reduce
HR
myocardial contractility
BP
myocardial O2 demand
Improve ventricular filling time artery
perfusion

79
ß-Blockers

Adverse effects
hypotension
acute HF
bradycardia
heart block
may mask hypoglycemia symptoms
use short acting agents in patients with
bronchospastic pulmonary disease

80
Calcium Channel Blockers

Dihydropyridines
amlodipine
felodipine
nifedipine
nicardipine
clevidipine
Non-dihydropyridines (negative inotropic effects)
verapamil
diltiazem

81
Calcium Channel Blockers

Use in STE NSTE ACS reserved for patients with
contraindications to ß-blockers (Class 1)
Inhibit Ca2 influx to myocardial vascular
smooth muscle cells
cause vasodilation
Non-dihydropyridines have additional antiischemic
effects
slow HR via AV node conduction
Little benefit shown beyond symptom relief
Negative inotropic effects may worsen outcomes

82
2MI Prevention Goals

Control modifiable CHD risk factors
Prevent development of systolic HF
Prevent recurrent MI, stroke
Prevent death, including sudden cardiac death

83
2MI Prevention

Following STEMI/NSTEMI, treat patients
indefinitely with ASA, ß-blocker, ACEI
NTG for ischemic chest discomfort
many patients should also receive clopidogrel
Annual influenza vaccination
Warfarin in select patients
controversial
Statins used in most patients
Glycemic control is important

84
Modifiable Risk Factors

Smoking cessation
HTN control
Weight loss
Glycemic control
Dyslipidemia treatment

85
Aspirin

Decreases risk of death, recurrent MI, stroke
following MI
Quality care indicator for MI patients
Continue indefinitely unless contraindicated
Dose 75 to 81 mg
patients with stents 325 mg for 1 to 12 months
Monitor for bleeding
especially when used in combination with warfarin
or clopidogrel

86
Clopidogrel

Decreases risk of death, MI, stroke in NSTE ACS
patients
clopidogrel aspirin for up to 1 yr
STEMI patients who did not have revascularization
may receive 14 to 28 days of clopidogrel
Continue for at least 1 yr if possible in
patients with stent placement
Monitoring
bleeding, rash, GI upset

87
Clinical Controversy

Interactions between clopidogrel PPIs
Retrospective cohort study (n8205)
5244 patients taking clopidogrel PPI after
hospitalization for ACS 2961 did not receive a
PPI
Clopidogrel PPI associated with higher risk of
death or rehospitalization for ACS compared with
clopidogrel without PPI
adjusted hazard ratio, 1.27 95 CI, 1.10-1.46
FDA issued a safety bulletin, additional studies
in progress

Ho PM, Maddox TM, Wang L, et al. Risk of adverse
outcomes associated with concomitant use of
clopidogrel and proton pump inhibitors following
acute coronary syndrome. JAMA. 2009301(9)937-44.
88
Warfarin

Consider anticoagulation in select patients
following ACS
LV thrombus
history of thromboembolic events
chronic atrial fibrillation
Routine warfarin treatment should not be used in
HF patients in normal sinus rhythm without
another indication
Reduces risk of death, MI, stroke
Doubles major bleeding risk

89
Warfarin

INR monitoring required
Many drug food interactions
Addition of warfarin to aspirin clopidogrel
further increases risk for bleeding
Not currently recommended by any professional
organization except select situations

90
Clinical Controversies

Combination ASA, clopidogrel, warfarin not well
studied
Used in patients with stents patients with
indications for anticoagulation along with
history of low EF MI
Requires close monitoring
Lower INR target (2 to 2.5) may be appropriate

91
ACE Inhibitors

Start in all MI patients to reduce mortality,
decrease reinfarction prevent HF (Class 1)
prevent cardiac remodeling
start PO ACE inhibitor within 24 hrs of MI
Rx for ACE inhibitor or ARB at hospital discharge
is a quality care indicator
Continue indefinitely in patients with LVEF lt
40, HTN, DM, CKD

92
Angiotensin Receptor Blockers

Candesartan valsartan shown to improve clinical
outcomes in HF patients (Class 1 for patients
with ACE inhibitor intolerance)
alternatives for patients with low EF following
MI unable to take ACE inhibitors
class effect?
Little to no evidence ARBs are useful in
diastolic HF
Lower incidence of cough angioedema compared to
ACE inhibitors

93
Aldosterone Antagonists

Eplerenone PostAcute Myocardial Infarction Heart
Failure Efficacy and SUrvival Study (EPHESUS)
Showed reduced mortality from sudden death, HF,
MI in patients treated with eplerenone compared
to placebo
Consider eplerenone or spironolactone within 2
weeks following MI in certain patients (Class 1)
those already receiving an ACE inhibitor with EF
lt 40 HF symptoms or DM

Pitt B, Remme W, Zannad F, et al. Eplerenone, a
selective aldosterone blocker in patients with
left ventricular dysfunction after myocardial
infarction. N Engl J Med 200334813091321.
94
Aldosterone Antagonists

Aldosterone causes vascular myocardial
fibrosis, endothelial dysfunction, HTN, LV
hypertrophy, electrolyte abnormalities,
arrhythmias
Monitor K
especially patients with renal dysfunction
Spironolactone can cause gynecomastia, sexual
dysfunction, menstrual irregularities
eplerenone less likely to cause adverse reactions

95
Lipid Lowering Agents

HMG-CoA reductase inhibitors (statins)
simvastatin, atorvastatin, lovastatin,
fluvastatin, pravastatin, rosuvastatin
ezetimbe
fenofibrate, gemfibrozil (drug interaction with
statins)
niacin
fish oil

96
Lipid Lowering Agents

Patients with CAD have LDL cholesterol goal lt 100
mg/dL
LDL cholesterol lt 70 mg/dL optional goal
All ACS patients should receive a statin
Statins have anti-inflammatory anti-thrombotic
properties
lipid lowering therapy at discharge is a quality
care indicator
Consider a fibrate or niacin in patients with a
low HDL (lt 40 mg/dL) or high triglycerides (gt
200 mg/dL)

97
Glycemic Control

Hyperglycemia associated with increased morbidity
mortality in hospitalized patients
NICE-SUGAR (Normoglycemia in Intensive Care
Evaluation-Survival Using Glucose Algorithm
Regulation)
n6104
blood glucose target lt 180 mg/dL for critically
ill patients resulted in lower mortality than
intensive glucose control (target 81 to 108 mg/dL)

The NICE-SUGAR Study Investigators. The
Normoglycemia in Intensive Care
Evaluation-Survival Using Glucose Alogorithm
Regulation (NICE-SUGAR). NEJM. 20093601283-1297
98
Monitoring

Parameters for monitoring efficacy of
nonpharmacologic pharmacotherapy for STE NSTE
ACS are similar
relief of ischemic discomfort
return of ECG changes to baseline
absence or resolution of HF signs

99
Monitoring
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
100
Monitoring
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
101
Monitoring
DiPiro JT, Talbert RL, Yee GC, Matzke GR, Wells
BG, Posey LM Pharmacotherapy A Pathophysiologic
Approach, 7th Edition http//www.accesspharmacy.c
om
102
Acknowledgements