A previously healthy woman about 50 years old with no previous medical history or coronary risk factors presented 30 minutes after the sudden onset of severe substernal chest pain. An ECG was recorded and interpreted within 13 minutes:
We gave clopidogrel 600 mg, aspirin, and a heparin bolus. There was time to get another ECG, 13 minutes later, before going to the cath lab:
Cath lab results
The patient went to the cath lab and had a door to balloon time of 50 minutes, for a total symptom onset to balloon time of 80 minutes (very fast). There was complete occlusion of the proximal LAD which was opened and revealed a very large first diagonal (this explains the predominance of V4-V6 on the ECG). After reperfusion, there was somewhat less "blush" (micovascular reperfusion as demonstrated by slight opacification, by contrast, of the affected myocardium).
There was now TIMI-3 flow, and the patient was pain free, but there was persistent ST elevation in lead V5 on the 6-lead monitor in the cath lab. Therefore, in addition to thrombectomy, the interventionalist gave intra-coronary adenosine (a vasodilator) to try to improve distal microvascular flow. As is routine, he also gave intracoronary nitro. And, of course, he used an eptifibatide bolus and infusion to maximally inhibit platelets. He did not see any distal "cut off" of vessels in the distribution of the large diagonal or the LAD, but he suspected, based on the persistent ST elevation, that the patient had a significant shower of debris down the diagonal distribution. He states that "this probably occurred at the time of the acute vessel closure because we did not have any "no flow" or "slow flow" issues that developed acutely during the case."
Here was the post-cath ECG:
After cath, the troponin I was already 107 ng/mL at 5 hours after presentation, and peaked at 178 ng/mL (very large MI).
The patient had a post cath ejection fraction of 36% and persistent chest pain for much of the day. Due to high risk of cardiogenic shock and dysrhythmia, ICU admission was warranted (usually not necessary for completely successful reperfusion).
Usually, a low ejection fraction in a patient with rapid restoration of TIMI-3 flow means that the patient has stunned myocardium that will recover. However, the absence of resolution of ST elevation here is consistent with poor microvascular reperfusion, as is the very high troponin I, and thus recovery of function is not likely to be excellent.
The pain did eventually resolve, but significant damage was done. For instance, the risk of sudden death from dysrhythmia is much higher than it would have been with good microvascular reperfusion, and she may need to go home on a temporary external automatic defibrillator.
2 days after presentation, here is the ECG:
No Reflow
This patient had remarkably fast symptom onset to balloon time, and optimal reperfusion therapy, and yet did not get good reperfusion because of poor microvascular reperfusion (thought to be due mostly to downstream microvascular obstruction and/or vasoconstriction). About 2-5% of patients with successful PCI have no reflow. Absence of resolution of ST elevation on the ECG is the best indicator of no reflow. Suffice it to say that these patients have a much worse outcome than patients with good microvascular reperfusion. It's etiology is not uniform for every patient. It is associated with, among other factors, clopidogrel resistance. (We usually think of using Prasugrel or Ticagrelor to prevent re-occlusion; maybe we should be using these alternatives to clopidogrel to prevent "no reflow." The therapy of "No reflow" is based on vasodilators such as adenosine, verapamil, and nitroprusside, as well as on triple antiplatelet therapy; no single mechanical or pharmacologic therapy has proven consistently effective.
Here is one review from 2010.
Here is another review from 2012.
Reperfusion on the ECG: Summary
I will leave the details for the below chapter from my book.
1. The ECG is the best predictor of reperfusion of the microvasculature, even better than angiographic assessment by TIMI flow. Notice that the interventionalist relied on the ECG to diagnose "no reflow" in this patient.
2. TIMI myocardial perfusion grading (TMP) flows 1-3 grade the amount of microvascular reperfusion seen on angiogram, called "blush". Absence of microvascular perfusion in the presence of good epicardial blood flow is called "no reflow."
3. "No reflow" is probably mostly caused by downstream showering emboli of platelet aggregates, and also by vasoconstriction.
4. After reperfusion, the first ECG marker of microvascular reperfusion is T-wave inversion
5. After reperfusion, the best ECG marker of microvascular reperfusion is resolution of ST segment elevation by at least 50% from maximum, and preferably, > 70% (or complete) resolution.
6. The ECG is far more reliable at gauging microvascular reperfusion than is resolution of chest pain.
Chapter 27:
TIMI Frame Count
Reperfusion:
General background
Angiographic
reperfusion grades, persistent ST elevation, and prognosis
ST recovery and
prognosis
 |
| Sinus rhythm. Intraventricular conduction delay with a QRS of 117 ms (really, incomplete LBBB) There are hyperacute T-waves in V4-V6, I and aVL, with reciprocal ST depression and T-wave in version in III and aVF. V4 shows a de Winter's T-wave, with some ST depression. This is diagnostic of proximal LAD occlusion, and I activated the cath lab the moment I saw this ECG. |
We gave clopidogrel 600 mg, aspirin, and a heparin bolus. There was time to get another ECG, 13 minutes later, before going to the cath lab:
 |
| Now there is evolution to ST elevation in V2-V6. |
The patient went to the cath lab and had a door to balloon time of 50 minutes, for a total symptom onset to balloon time of 80 minutes (very fast). There was complete occlusion of the proximal LAD which was opened and revealed a very large first diagonal (this explains the predominance of V4-V6 on the ECG). After reperfusion, there was somewhat less "blush" (micovascular reperfusion as demonstrated by slight opacification, by contrast, of the affected myocardium).
There was now TIMI-3 flow, and the patient was pain free, but there was persistent ST elevation in lead V5 on the 6-lead monitor in the cath lab. Therefore, in addition to thrombectomy, the interventionalist gave intra-coronary adenosine (a vasodilator) to try to improve distal microvascular flow. As is routine, he also gave intracoronary nitro. And, of course, he used an eptifibatide bolus and infusion to maximally inhibit platelets. He did not see any distal "cut off" of vessels in the distribution of the large diagonal or the LAD, but he suspected, based on the persistent ST elevation, that the patient had a significant shower of debris down the diagonal distribution. He states that "this probably occurred at the time of the acute vessel closure because we did not have any "no flow" or "slow flow" issues that developed acutely during the case."
Here was the post-cath ECG:
 |
| Sinus rhythm and a narrower QRS. There is persistent ST elevation, and persistently upright T-waves (absence of reperfusion T-waves) in V4-V6. Though T-waves are inverted in aVL, they are not inverted in lead I, and there is persistent ST elevation in aVL. |
After cath, the troponin I was already 107 ng/mL at 5 hours after presentation, and peaked at 178 ng/mL (very large MI).
The patient had a post cath ejection fraction of 36% and persistent chest pain for much of the day. Due to high risk of cardiogenic shock and dysrhythmia, ICU admission was warranted (usually not necessary for completely successful reperfusion).
Usually, a low ejection fraction in a patient with rapid restoration of TIMI-3 flow means that the patient has stunned myocardium that will recover. However, the absence of resolution of ST elevation here is consistent with poor microvascular reperfusion, as is the very high troponin I, and thus recovery of function is not likely to be excellent.
The pain did eventually resolve, but significant damage was done. For instance, the risk of sudden death from dysrhythmia is much higher than it would have been with good microvascular reperfusion, and she may need to go home on a temporary external automatic defibrillator.
2 days after presentation, here is the ECG:
 |
| There is still persistent ST elevation in lateral leads, though now there is T-wave inversion. There is a new Q-wave in lead I. |
No Reflow
This patient had remarkably fast symptom onset to balloon time, and optimal reperfusion therapy, and yet did not get good reperfusion because of poor microvascular reperfusion (thought to be due mostly to downstream microvascular obstruction and/or vasoconstriction). About 2-5% of patients with successful PCI have no reflow. Absence of resolution of ST elevation on the ECG is the best indicator of no reflow. Suffice it to say that these patients have a much worse outcome than patients with good microvascular reperfusion. It's etiology is not uniform for every patient. It is associated with, among other factors, clopidogrel resistance. (We usually think of using Prasugrel or Ticagrelor to prevent re-occlusion; maybe we should be using these alternatives to clopidogrel to prevent "no reflow." The therapy of "No reflow" is based on vasodilators such as adenosine, verapamil, and nitroprusside, as well as on triple antiplatelet therapy; no single mechanical or pharmacologic therapy has proven consistently effective.
Here is one review from 2010.
Here is another review from 2012.
Reperfusion on the ECG: Summary
I will leave the details for the below chapter from my book.
1. The ECG is the best predictor of reperfusion of the microvasculature, even better than angiographic assessment by TIMI flow. Notice that the interventionalist relied on the ECG to diagnose "no reflow" in this patient.
2. TIMI myocardial perfusion grading (TMP) flows 1-3 grade the amount of microvascular reperfusion seen on angiogram, called "blush". Absence of microvascular perfusion in the presence of good epicardial blood flow is called "no reflow."
3. "No reflow" is probably mostly caused by downstream showering emboli of platelet aggregates, and also by vasoconstriction.
4. After reperfusion, the first ECG marker of microvascular reperfusion is T-wave inversion
5. After reperfusion, the best ECG marker of microvascular reperfusion is resolution of ST segment elevation by at least 50% from maximum, and preferably, > 70% (or complete) resolution.
6. The ECG is far more reliable at gauging microvascular reperfusion than is resolution of chest pain.
The ECG in REPERFUSION AND REOCCLUSION
This is Chapter 27 (Reperfusion and Reocclusion) from my book, The ECG in Acute MI. It is long, and has a detailed annotated bibliography. It comes from literature before 2002, but it is still accurate and almost everything you need to know (unless you are an interventionalist) about the ECG in Reperfusion and Reocclusion.Chapter 27:
GENERAL BACKGROUND
Arterial patency and
microvascular circulation
Reperfusion therapy is guided by the ongoing
assessment of myocardial reperfusion.
This depends on two factors: 1) reperfusion
of the epicardial infarct-related
artery (IRA); and 2) reperfusion of the microvascular circulation, which may be damaged by ischemia and
reperfusion (the “no-reflow” phenomenon) and result in impeded capillary
flow.
Hemodynamic status and age are the best clinical
prognostic indicators for AMI outcome.
The best ECG indicator for AMI outcome is ST resolution or the
lack thereof (318-322). The best
overall predictor of failed myocardial reperfusion is a finding of < 50% recovery of ST segments from
maximal elevation. However, the ECG
cannot determine whether the cause of failed reperfusion is persistent arterial
occlusion or microvascular damage. Angiography is necessary to assess and
grade IRA patency and microvascular circulation and to guide subsequent
therapy. Rescue PCI, which we define as PCI undertaken within 6 hours of the
start of thrombolytic therapy, (323) should be strongly considered when
clinicians have determined that thrombolytic reperfusion has failed and should be done immediately after transfer to a PCI facility if there is no ECG evidence of good reperfusion (324). This
is especially true for a large AMI, as indicated by anterior location,
high ST elevation, or ST deviation in numerous leads. A patent IRA with inadequate flow may be due
to residual stenosis or abnormal microvascular circulation and may be treated
with vasodilators, antiplatelet,
and antithrombotic agents +/- PCI.
TIMI grading of IRA
patency
IRA patency can only be definitively assessed by
angiography. Angiographic assessments
are then systematized by TIMI grading, as follows (325):
· TIMI-0 = no flow
· TIMI-1 = penetration of
contrast without perfusion. These
patients have persistent ST elevation and a poor prognosis and must be
identified for rescue PCI
· TIMI-2 = partial
reperfusion. These patients may have resolution of ST elevation and a prognosis
intermediate between TIMI 0/1 and TIMI 3 flow.
· TIMI-3 = complete
reperfusion. These patients usually (but
not always) show ST resolution. TIMI-3
flow after reperfusion is associated with lower mortality and lower incidence
of CHF (326, 327), but its prognostic value may not be
independent of resolution of ST elevation (318).
By outcome measures, a flow grade < TIMI-3 indicates failed reperfusion (26, 328). After reperfusion therapy for AMI, TIMI-3
flow is associated with a 30-42 day mortality of 3.6%, in contrast to TIMI-2
flow (6.6% mortality) and TIMI-0/1 flow (9.5% mortality) (327).
TIMI Frame Count
The TIMI frame count (TFC) further systematizes TIMI flow
categorization. The TFC is the measure
of the exact number of cineangiographic frames required for contrast to
reach a defined distal segment of the IRA (see Background discussion under
Angiographic Reperfusion Grades in the
annotated bibliography of this chapter).
TIMI myocardial
perfusion grading of microvasculature
TIMI flow and TFC are impacted by both the severity
of the underlying stenosis and thrombus and by the microvasculature. Intact microvasculature is most accurately
assessed by the appearance on an angiogram of diffuse and faint highlighting of
the myocardium by contrast, known as “myocardial blush.” These assessments are systematized with TIMI myocardial perfusion grading (TMP),
which is based on a scale from 0-3 as follows (319, 326, 329):
· TMP grade 0 = no
microvascular perfusion
· TMP grade 1 = no clearance
of contrast
· TMP grade 2 = slow clearance
of contrast
· TMP grade 3 = normal
clearance.
An open coronary artery may have brisk TIMI-3 flow
but have a TMP grade of 0 or 1 (326); patients with these findings show
persistent ST elevation (318, 319, 329).
TMP grade 3 is associated with a
good prognosis, independent of TIMI flow.
ECG DIAGNOSIS OF REPERFUSION
ST segments in reperfusion
With a reperfused IRA AND intact microcirculation, ST segments usually
fall rapidly and are near baseline within
3 hours of reperfusion (see Case 27-1).
Approximately 80% of cases with IRA reperfusion manifest 50% ST recovery
within 90 minutes. Most of the remaining
20% likely have microvascular injury with resultant poor capillary flow; their
prognosis is as poor as patients with poor flow in the IRA (318, 319, 329).
This contrasts with a non-reperfused IRA, in which ST segments fall gradually and plateau,
with or without persistent elevation.
Plateauing occurs as early as 6 to 12 hours, due to myocardial cell
death (330).
ST resolution is an accurate
predictor of reperfusion, especially in patients whose ECG’s show ST elevation > 4 mm
(331). During or shortly before reperfusion, ST segments often continue to rise
before resolving, frequently with an increase in CP (156, 157, 332, 333, 334). Some patients experience “cyclic reperfusion,” in which there is
reperfusion and subsequent reocclusion.
This may occur with or without therapy.
Cyclic reperfusion occurs in 25-30% of AMI before reperfusion therapy
and can be detected with ST segment monitoring (335).
T-waves in reperfusion
In reperfused AMI, terminal
T-wave inversion often occurs rapidly
(within 90 minutes) in the leads that manifested the greatest ST elevation on
presentation, and before full ST resolution (156, 157). This contrasts with non-reperfused AMI, 90% of which show gradual T-wave inversion (over 48 to 72
hours), with a depth < 3 mm (94)
(Fig. 8-3). If there is some myocardial injury,
as measured by elevated troponin, expect terminal T-wave inversion to develop
into deep and symmetric T-wave inversion over the first 48 hours after the
onset of AMI (94) (see Case 27-2). Accordingly, early T-wave inversion (< 24 hours) is
associated with greater IRA patency, better perfusion grade, and a more benign
in-hospital course than later inversion (336). In some patients with
very early reperfusion and very little or no myocardial cell death, as measured
by troponin, there may be no T-wave inversion, very late inversion, or
reversible inversion (94).
Q-wave and
R-wave changes are not accurate markers of AMI reperfusion (337).
Reperfusion monitoring
Monitoring for reperfusion may
include observation of 5 elements, as follows: 1) ST resolution, or
“recovery;” 2) terminal T-wave inversion; 3) resolution of CP; 4) reperfusion
arrhythmias; and 5) biochemical markers.
1. ST
resolution
ST segment resolution, or “recovery,” is the best
marker for reperfusion (see Cases 27-1 and 27-2). ST
segments may be monitored continuously or with static ECG’s every 5 minutes
from the time of thrombolytic administration.
If ST elevation is > 4 mm and
there is NEITHER >/= 50% recovery at
60 minutes NOR terminal T-wave inversion, TIMI-3 flow is unlikely. Strongly consider rescue PCI.
Continuous ST segment monitoring is the best method
for monitoring ST segment changes (156, 159, 338, 339) (see Case
27-3). Commercial products are
available. Select one lead with the
greatest ST elevation, plot the ST segment elevation continuously, and observe
for peaks and troughs. By convention, ST elevation is measured on continuous monitors at 80 ms after the
J-point. See Table 27-1.
· ST recovery >/= 50% from MAXIMAL ST elevation
(peak level attained) within 60 minutes and without re-elevation is a very good
predictor of reperfusion. These patients do not need early angiography or
rescue PCI. ST recovery >/= 50% has a positive predictive value (PPV) for patency (TIMI-2 or -3
flow) of 87%.
· ST recovery < 50%, consider rescue PCI. The negative predictive value (NPV) for
occlusion (lack of recovery) is 71%; i.e., 71 % of patients who do not show ST
recovery >/= 50% have closed arteries and 29% have TIMI 2-3 flow. These patients are candidates for
rescue PCI. Most importantly, ST
recovery < 50% with no terminal T-wave inversion indicates a TIMI flow of
0-2 with a PPV of 86%. TIMI-3 flow
is true successful reperfusion. Of
patients with persistent ST elevation (< 50% recovery), 14% have TIMI-3 flow
but presumably continue to have ST elevation due to microvascular injury.
· The higher the maximal or
initial ST elevation, the more accurate the patency prediction (331).
Although static ECG’s are inferior to
continuous ST segment monitoring (339), if continuous monitoring is
unavailable, recording static ECG’s every 5 minutes from the time of
thrombolytic administration is a reasonable substitute (158). Use the single lead with the highest ST
elevation and measure resolution from the maximal height. ST resolution > 50% at 60 minutes after
treatment is a good indicator of reperfusion (158). Complete ST resolution assures reperfusion
but occurs infrequently by 60 minutes after treatment (339).
2. Terminal T-wave inversion
(See
also Chapter 8)
Terminal T-wave inversion within the first 90
minutes is
a specific marker of reperfusion and is approximately 60% sensitive (156,
157, 158). If leads with ST
elevation develop terminal T-wave inversion within 60 minutes of thrombolysis,
reperfusion is highly likely. Because T-wave inversion usually indicates some
myocardial injury, rapid ST resolution without any T-wave inversion may be
evidence that reperfusion occurred before myocardial cell death; in such cases,
biomarkers may not be elevated. Terminal
T-wave inversion usually occurs before full resolution of the ST segment.
Deep,
symmetric T-wave inversion (> 3 mm) indicates reperfusion that is less
recent than reperfusion indicated by terminal T-wave inversion (see Case 27-2). Terminal T-wave inversion undergoes further
development into symmetric T-wave inversion (94). Deep, symmetric T-wave inversion need not be
preceded by ST elevation, although there is usually no development of Q-waves
without ST elevation. Symmetric T-wave
inversion is generally present after full resolution of the ST segment.
T-waves also
eventually invert in persistently occluded vessels. T-wave inversion in the presence of deep
Q-waves, especially QS-waves, may be
a manifestation either of reperfusion late in the course of AMI or of a well-developed,
non-reperfused AMI (94, 340).
These inverted T-waves are usually < 3 mm, in contrast with inverted
T-waves of reperfused AMI, which are > 3 mm (94). Such T-wave inversion may be evident at
presentation if the patient presents late after onset (see Case 33-3).
With posterior
AMI, if the T-wave is upright before reperfusion and there is ST recovery,
reperfusion usually results in precordial T-waves (especially V2) becoming
fully upright and taller and wider than before AMI onset. This is a reciprocal view of posterior
inverted T-waves. Reocclusion in this
case is unlikely to result in T-wave inversion.
If the T-wave is asymmetrically inverted before reperfusion, reperfusion
usually results in T-waves pseudonormalizing
(turning upright) and becoming taller and wider than before the onset of AMI;
reocclusion generally results in re-inversion of T-waves. See Case 27-1. (See also: Cases 16-10 and 13-4).
3. Relief of Chest Pain
Two studies showed that complete relief of CP, often with an initial transient increase in
pain, had a good PPV, with an 84% (339) to 96% (156) chance of
reperfusion. However, relief of CP with
neither any recovery of ST segments nor terminal T-wave inversion is unlikely
to represent reperfusion. If CP resolves,
record serial ECG’s; pursue rescue angioplasty if there is no ECG evidence of
reperfusion.
With spontaneous relief of CP, do not abort reperfusion
unless accompanied by some amount of ST recovery:
·
With increased, unchanged, or < 25% ST elevation resolution, continue
reperfusion therapy.
·
With 25%-50% resolution, or terminal T-wave inversion, record serial
ECG’s or continuous monitoring and look for >/= 50% ST resolution.
· With 50%-100% resolution,
reperfusion therapy may be suspended, pending further assessment, especially
continuous ST monitoring.
Relief of CP has a poor NPV, in that persistent pain
did not necessarily imply persistent occlusion (159, 339).
4. Reperfusion arrhythmias
Occurrence of early accelerated idioventricular rhythm (AIVR) indicates
reperfusion with 97% specificity but only 45% sensitivity (335). A sudden burst of ventricular tachycardia may
also indicate reperfusion.
5. Biochemical markers of reperfusion
Biochemical markers may also be useful in assessing reperfusion; see
Chapter 29 for details.
See Cases 27-1 to 27-3 for examples of
reperfusion. (See also: Cases 6-4, 12-3,
16-10, 20-11, and 32-1).
.
Management
A
meta-analysis of randomized trials showed that rescue angioplasty performed in
patients with failed reperfusion results in a decreased incidence of CHF,
death, and recurrent MI, without significant adverse effects (324). These trials were performed without
the latest technology and with prolonged time intervals from thrombolysis to
rescue. In this age of abciximab and
stenting, we highly recommend rapid
rescue PCI for failed reperfusion as evidenced by the above-mentioned ECG
indicators or by persistent clinical instability. If
TIMI-3 flow is present but TMP grade is low, treatment with vasodilators,
antiplatelet, and antithrombotic agents is particularly important.
REOCCLUSION
Once reperfusion is achieved, monitor ST segments
for reocclusion. Symptoms are not
reliable indicators of reocclusion and many recurrent AMI’s are asymptomatic
(69, 89). If continuous
monitoring is unavailable, record
frequent static ECG’s every 30 to 60 minutes until stability is assured. At a minimum, record hourly ECG’s for several
hours after reperfusion.
ECG manifestations of reocclusion
Each AMI has an “ischemic fingerprint,” such that
reocclusion of the same vessel at the same location reproduces the same ECG
findings (83, 190). Thus,
reocclusion manifests the reverse of reperfusion on the ECG, as follows:
· Initial rapid “pseudonormalization” of T-waves, in which inverted T-waves turn upright.
· Subsequent re-elevation of ST segments.
Caution: post-infarction regional pericarditis
(PIRP) may mimic reocclusion (see Chapter 28) (94). This is characterized by gradual pseudonormalization
of T-waves or persistent upright T-waves in the leads that had the greatest ST
elevation at presentation. There is also
gradual ST re-elevation, over 24-72 hours. PIRP lacks the typical diffuse ST elevation
of nonspecific pericarditis.
See Case 27-3 of reocclusion. (See also: Case 8-12, of pseudonormalization
of symmetrically inverted T-waves; Case
13-4 of an inferoposterior AMI with reperfusion and reocclusion; and Case 3-3
of reocclusion a week after reperfusion).
Management
Reocclusion after thrombolysis mandates either
repeat thrombolysis or, preferably, rescue angiography +/- PCI.
ANNOTATED BIBLIOGRAPHY
Reperfusion:
General background
Krucoff MW et al., Continuously
updated 12-lead ST-segment recovery analysis for myocardial infarct artery
patency assessment and its correlation with multiple simultaneous early
angiographic observations, 1993.
Methods: Krucoff et al.
(341) performed angiography and continuous ST segment monitoring in 22 AMI
patients.
Findings: Forty-four
episodes of arterial patency and multiple ST trend transitions in 11 of 22 patients
after thrombolysis suggested cyclic changes in coronary flow before
catheterization.
Comment: These authors and others (158, 159) have shown repeatedly that ST recovery must be measured
from maximal ST elevation for accurate assessment of reperfusion. Peak ST elevation may occur in the absence of
or any time after thrombolytic therapy.
Static ECG’s are less effective than continuous monitoring because ST
segments may rise from baseline before actual reperfusion and fall again (or
vice versa) to nearly the same level without detection.
Angiographic
reperfusion grades, persistent ST elevation, and prognosis
Background: TIMI flow grade is a measurement of
reperfusion of a coronary vessel and TMP flow grade is a measurement of
myocardial microvascular perfusion. TFC
is the measure of the exact number of cineangiographic frames required
for contrast to reach a defined distal segment of the IRA. TFC is especially
helpful to further categorize TIMI-2 and TIMI-3 flow. Normal mean TFC’s are: 36.2 +/- 2.6 for the
LAD, 20.4 +/- 3.0 for the RCA, and 22.2 +/- 4.1 for the circumflex artery
(342). To standardize TFC for all
arteries, the TFC of the LAD is divided by 1.7 to give a “corrected” TFC (CTFC)
(342). At 90 minutes after thrombolysis
for STEMI in all locations. a CTFC of 0-13 is above normal blood flow and is
associated with mortality of 0%. A CTFC
of 14-40 is associated with mortality of 2.7%, and a CTFC > 40 is associated
with mortality of 6.4% (343). Of
patients with TIMI-3 flow, CTFC </= 20 vs. > 20 is associated with
complication rates of 7.9% vs. 15.5%, respectively (343).
Van’t Hof et al., Clinical value of 12-lead electrocardiogram after
successful reperfusion therapy for acute myocardial infarction, 1998.
Methods: Van ‘t Hof et al. (320) studied ST resolution
in 403 AMI patients with TIMI-3 flow after primary angioplasty.
Findings: ST segments normalized in 51% of patients (ST
< 0.1 mV). Partial normalization
(30-70% of initial height) was associated with a relative risk (RR) of death of
3.6 (CI = 1.6-8.3) compared with full
normalization(< 30% of initial height).
Absence of resolution or increased ST elevation was associated with a RR
of death of 8.7 (range = 3.7-20.1).
Van’t Hof et al., Angiographic assessment of myocardial reperfusion in
patients treated with primary angioplasty for acute myocardial infarction:
myocardial blush grade, 1998.
Methods: Van ‘t Hof et al. (329) studied myocardial
blush during primary angioplasty in 777 AMI patients.
Findings: Angioplasty resulted in TIMI-3 flow in 89% of
patients and in TIMI-0, -1, or -2 flow in 11%.
Patients with TMP grades 3, 2, and 0/1 had: 1) CK infarct sizes of 757 IU/L, 1143 IU/L,
and 1623 IU/L; 2) EF’s of 50%, 46%, and 39%; and 3) mortality (after a mean
follow-up of 1.9 +/- 1.7 years) of 3%, 6%, and 23%, respectively. TMP grade predicted mortality independently
of Killip class, TIMI grade flow, EF, and other clinical variables. TMP grade was the best predictor of 3-year
mortality, with rates of 3%, 15%, and 37% for patients with grades 3 (19% of
patients), 2, and 0/1, respectively.
Among TMP grade 3 patients, ST elevation normalized in 65% and ST
elevation decreased in an additional 28%.
Gibson CM et al., Relationship of TIMI myocardial
perfusion grade to mortality after administration of thrombolytic drugs, 2000.
Methods: Gibson et al. (326) studied 762 patients in
the TIMI-10B trial, in which 854 patients with AMI were randomized to TNK-tPA
or standard alteplase and underwent angiography at 90 minutes post-thrombolytic
administration.
Findings: TMP grade 3 myocardial perfusion was
independently associated with low 30-day mortality of 2.0%, as compared to 3.5%
for patients with TIMI-3 flow. The
decreased risk was additive to the low risk of TIMI-3 flow, such that mortality
was a mere 0.73% (1 of 137) for patients with TIMI-3 flow and TMP grade
3 perfusion compared to a 10.9% mortality (14 of 129) for those with both TIMI
0-2 and TMP 0/1
grading. Mortality was approximately
the same for patients with: (1) both TIMI 0-2 flow and TMP grade 3 perfusion,
presumably through collaterals; and (2) both TIMI-3 flow and TMP 0/1 perfusion.
ST recovery and
prognosis
ST
recovery can be a good prognostic indicator, even in the presence of an
occluded vessel. Lack of ST recovery
portends a poor prognosis, even with an open artery.
Claeys MJ, Determinants and prognostic
implications of persistent ST-segment elevation after primary angioplasty for
acute myocardial infarction: importance of microvascular reperfusion injury on
clinical outcome, 1999.
Methods:
Claeys et al. (319) studied 91 AMI patients with reperfusion after
angioplasty.
Findings:
Of 91 patients, 75 had TIMI-3 and 16 had TIMI-2 flow. Persistent ST elevation, defined as ST >/=
50% of the initial height, was observed in 33 (36%) patients and was associated
with high one-year mortality (15% vs. 2%) and high total major adverse cardiac
event rate (45% vs. 15%). Persistent ST elevation was the most
important independent determinant of major adverse cardiac event rate, with
an adjusted RR of 3.4, and both were attributed to impaired microvascular
circulation.
Shah A et al.,
Prognostic implications of TIMI flow grade
in the infarct related artery compared with continuous 12-lead ST-segment
resolution analysis. Reexamining the
"gold standard” for myocardial reperfusion treatment, 2000.
Methods: Shah et al. (318) identified 258 AMI patients who
underwent thrombolysis and then angiography in the TIMI-7 and GUSTO-1 trials
(see Appendix). Patients were stratified
according to TIMI 0-3 reperfusion and by ST resolution >/= 50% vs. <
50%.
Findings: ST
resolution WAS an independent predictor of the combined clinical outcome of
death or CHF but TIMI flow grade was NOT.
ST resolution among patients
with TIMI grade 0-1 flow identified a group with a relatively benign clinical
course.
Dissman R et al., Early
assessment of outcome by ST segment analysis after thrombolytic therapy in
acute myocardial infarction, 1994.
Methods: Dissman et al. (321) studied CK levels and
EF’s in 77 AMI patients to correlate ST resolution and infarct size.
Findings: The enzyme-determined infarct size and the
resulting EF correlated closely with complete (>70%), partial (30-70%), or
no ST (<30 3="" 43="" 53="" 58="" and="" at="" complete="" ef="" for="" hours="" nbsp="" no="" o:p="" or="" partial="" patients="" post-thrombolysis.="" resolution="" respectively.="" s="" were="" with="">
Schroder R et al., Extent of
early ST segment elevation resolution: a strong predictor of outcome in
patients with acute myocardial infarction and a sensitive measure to compare
thrombolytic regimens, 1995.
Methods: Schroder et al. (322) analyzed ECG’s, CK
levels, and mortality data of 1909 AMI patients randomized to reteplase or
SK.
Findings: In 1398 patients who presented </= 6 hours
from AMI onset, 35-day mortality rates for complete (>/= 70%), partial
(30-70 %), or no (< 30%) ST resolution by 3 hours post-thrombolytic
administration were 2.5%, 4.3%, and 17.5%, respectively.
Saran
RK et al., Reduction in ST segment elevation after thrombolysis predicts either
coronary reperfusion or preservation of left ventricular function, 1990.
Methods:
Saran et al. (344) studied ST
segment changes and angiographic findings in 45 patients (see more detailed
annotation below).
Findings: LV
function was well-preserved if the ST segment had fallen by >/= 25% at 3
hours.
Continuous ECG
monitoring for prediction of reperfusion
Note: It is important to remember when evaluating
the following studies that 15% of IRA’s are open without treatment by
6-8 hours post-coronary occlusion (345).
Krucoff MW et al., Continuous 12-lead ST-segment recovery analysis in the
TAMI 7 study. Performance of a
non-invasive method for real-time detection of failed myocardial reperfusion,
1993.
Methods: Krucoff et al. (159) tested a method of
12-lead continuous ST segment recovery in a blinded, prospective, and
angiographically correlated study of 144 TAMI-7 patients who received
thrombolytics in early MI. Summated ST
elevation was plotted against time by PC-based software and read by experienced
cardiologists. The ST segment was
plotted and assessed for peaks, troughs, and general trend. The ST score at the moment of angiography was
compared to the peak elevation attained.
Patency was predicted based on ST recovery, defined as a 50% drop from
the maximum summated ST elevation, and continued downward trend. Occlusion was predicted by (1) persistent ST
elevation, (2) re-elevation after recovery or a downward trend, or (3)
increased ST elevation. The study was
considered indeterminate if no definite peaks or troughs and corresponding
trends could be discerned.
Findings: There were 144 ST segment analyses. Of 35 angiograms performed during definite
(re-) elevation periods (indicating occlusion), 25 IRA’s were
angiographically occluded. Of 91
angiograms during definite recovery periods (indicating reperfusion), 81
IRA’s were angiographically patent. Of
18 indeterminate analyses, 14 were angiographically patent. If the indeterminate group is considered to
be “probably not occluded,” then the IRA was patent in 95 of 109 cases (87%) so
predicted and occluded in 25 of 35 cases (71%) so predicted. Of 35 patients whose ST recovery analysis
determined IRA’s to be “occluded” (based on persistent or recurrent ST
elevation), only 5 had TIMI-3 flow. In
109 patients, analysis determined “probably not occluded,” (“indeterminate” or
“patent”) and 73 of these had TIMI-3 flow, 22 had TIMI-2 flow, and 14 had
TIMI-0 or 1 flow. Thus, “occluded” had a PPV for TIMI 0-2 flow of
86% and “probably not occluded” had a sensitivity of 94% and a PPV of 67% for
TIMI-3 flow and of 87% for TIMI-2 or -3 flow.
Comment: Post-thrombolytic TIMI-3 flow is associated
with a much better outcome than even TIMI-2 flow (26, 328). Therefore, the ability to distinguish TIMI-3
flow from TIMI-0 to -2 flow on the ECG is important.
Klootwijk P et al.,
Non-invasive prediction of reperfusion and coronary artery patency by
continuous ST segment monitoring in the GUSTO-I trial, 1996.
Methods: Klootwijk et al. (331) studied ECG’s of 373
GUSTO-1 patients (see Appendix) using continuous 12-lead ST segment recovery
analysis.
Findings: The predictive values for reperfusion or
persistent occlusion were not as good as in the study of Krucoff et al.
described above (159). Angiograms were
performed significantly later (between 90-180 minutes) in this study. Thus, the predictive accuracy would be
expected to be lower because ST segments in areas of persistent infarction
decline over time, due to myocardial cell death. A decrease of >/= 50% from peak and no
persistent re-elevation before angiography was used as a prediction of
“patent.” Accuracy was very high (79-100%) in patients with high ST elevation
(> 4 mm). In 116 patients with a peak
ST elevation >/= 4 mm, a prediction of “patent” had a PPV of 79% and NPV of
75%.
Doevendans PA et al.,
Electrocardiographic diagnosis of reperfusion during thrombolytic therapy in
acute myocardial infarction, 1995.
Methods: Doevendans et al. (156) performed continuous
ST segment monitoring of 61 AMI patients for 60 minutes after thrombolytic
therapy.
Findings: Reperfusion
was associated with rapid ST resolution, often after a transient elevation. Of 44 patients with reperfusion, 42 showed
>/= 25% decrease in ST elevation from maximal height (sensitivity 95%), but
only one of 17 patients without reperfusion showed this amount of normalization
(specificity 94%). Using a 50% decrease
in ST elevation as a cutoff, sensitivity was 85% (38 of 44 patients) and
specificity was, again, 94%. Relief of CP was also a very sensitive
sign of reperfusion; 25 of 26 patients with reperfusion had relief within 1
hour. Eighteen patients experienced
relief after a transient, often marked, increase in pain. Terminal
T-wave inversion was very specific for reperfusion; 28 of 44 patients with
reperfusion had terminal T-wave inversion, whereas only 1 of 17 without
reperfusion had terminal T-wave inversion.
AIVR was a specific but
insensitive marker of reperfusion; 16 of 42 in the reperfused group demonstrated
AIVR vs. one of 17 in the nonreperfused group.
Other “reperfusion arrhythmias” were uncommon and of little prognostic
utility. CK-MB peaked earlier in the
reperfused group.
Veldkamp RF et al., Comparison
of continuous ST-segment recovery analysis with methods using static
electrocardiograms for noninvasive patency assessment during acute myocardial
infarction, 1994.
Methods: Veldkamp et
al. (346) analyzed ECG’s and clinical data from 82 patients in the above study
by Krucoff et al. (159) to compare continuous ST recovery analysis with 5
static methods.
Findings: Static
methods such as those used by Saran et al. (344), Hackworthy et al. (347), and
Clemmensen et al. (348) had comparable accuracies to continuous ST recovery
analysis; see section below on static ECG’s.
Hohnloser SH et al., Assessment
of coronary artery patency after thrombolytic therapy: accurate prediction
using the combined analysis of three noninvasive markers, 1991.
Methods: Hohnloser et al. (338) used Holter monitoring and angiography in a prospective study
of 82 patients undergoing thrombolysis for first MI.
Findings: Of 82 patients, 63 had TIMI-2 or -3
reperfusion. A 50% reduction in ST
elevation measured 60 to 90 minutes after thrombolysis had a PPV of 97% and an
NPV of 43% for reperfusion. CK
peak < 12 hours was an accurate marker of reperfusion.
Frequent static ECG’s
Shah PK et al., Angiographic
validation of bedside markers of reperfusion, 1993.
Methods: Shah et al. (158) obtained static ECG’s every 5-10
minutes after thrombolytic therapy in 82 AMI patients, for up to 3 hours, until
angiography.
Findings: Their
findings were very similar to those of Doevendans et al. (156) described
above. Angiography demonstrated that 69
of 82 patients had a patent IRA with TIMI-3 flow and that these patients
consistently manifested a rapid, progressive decrease in both CP and ST
elevation. Pain resolved in 24 +/- 23 minutes (maximum 50 minutes) and decreased
ST elevation >/= 50% occurred within 16 +/- 14 minutes (maximum 41 minutes)
after restoration of TIMI-3 flow. Terminal
T-wave inversion and AIVR were also specific but insensitive markers of
reperfusion. This study demonstrates the importance of
frequent static ECG’s and the insensitivity of using only 2 static ECG’s to
detect reperfusion. In 58% of patients,
ST segments were unstable, rising and falling, before final resolution.
Infrequent static ECG’s
Califf RM et al., Failure of
simple clinical measurements to predict perfusion status after intravenous
thrombolysis, 1988.
Methods: Califf et al. (339)
performed angiography on 386 TAMI patients at 60 and 90 minutes
post-administration of tissue plasminogen activator (tPA). They recorded a baseline ECG and another at
90 minutes post-tPA, before the 90-minute coronary injection.
Findings: They
found no sensitive AND specific marker of reperfusion using infrequent static
ECG’s. Complete resolution of ST
segment and T-wave changes was associated with a 96% IRA patency rate at 90
minutes post-tPA, but this occurred in only 6% of patients. Only 38% of patients had “partial resolution”
of ST segments, 84% of whom showed reperfusion.
Complete resolution of CP occurred in 29%, of whom 84% had reperfusion
of the IRA. Unchanged or worsened CP
occurred in 20%, of whom 60% showed reperfusion. Patent IRA’s were demonstrated in 56% of
patients with neither symptom nor ST resolution and 63% of patients with no
change in ST segments showed reperfusion.
Although arrhythmias occurred frequently during the first 90 minutes of
therapy, none were associated with a higher patency rate.
Saran RK et al., Reduction in
ST segment elevation after thrombolysis predicts either coronary reperfusion or
preservation of left ventricular function, 1990.
Methods: Saran et al. (344) performed angiography on
45 AMI patients by 3 hours post-administration of anistreplase.
Findings: Using the lead with the greatest ST elevation
on static ECG’s, ST recovery
>/= 25% at 3 hours was nonspecific.
ST segments had fallen by >/= 25% in 30 of 31 patients with TIMI-2 or
-3 reperfusion, but also in 8 of 14 patients who had only TIMI-0 or -1
flow. Thus, if the ST segment fell by
>/= 25%, the specificity was only 43%; that is, many IRA’s remained
occluded. Three hours post-thrombolytic therapy is too late for ST recovery to be a meaningful indication of reperfusion because ST segments fall gradually,
even in persistently infarcted myocardium.
It is also too late to make a
decision for rescue PCI. If the ST
segment fell by < 25%, persistent occlusion was likely, with a PPV of
86%. Importantly, the global EF was well maintained in patients whose ST segments
fell > 25% and whose arteries were occluded. Saran et al. concluded that a reduction in ST
elevation of > 25% within 3 hours of thrombolysis indicates either a patent
IRA or preservation of LV function.
Clemmensen P et al., Changes in
standard electrocardiographic ST-segment elevation predictive of successful
reperfusion in acute myocardial infarction, 1990.
Methods: Clemmensen et al. (348) studied 53 patients
up to 8 hours post-SK administration.
They calculated the ST score as the sum of ST elevation in 11 leads,
based on static ECG’s obtained within 5 minutes of angiography.
Findings: Angiography demonstrated reperfusion (TIMI-2
or -3 flow) in 33 of 53 patients. A
decrease of >/= 20% in ST elevation was 88% sensitive and 80% specific for
reperfusion, with a PPV of 88% and an NPV of 80%. Clemmensen et al. concluded that a decrease of only 20% in the ST score
following thrombolytic therapy is a useful and noninvasive predictor of
reperfusion status in patients with evolving AMI.
Comment: The use of angiographic patency assessment up
to 8 hours post-treatment diminishes the value of this data.
T-wave
inversion and prognosis
See also Doevendans et
al. (156) above.
Oliva
PB et al., Electrocardiographic diagnosis of postinfarction regional
pericarditis: ancillary observations regarding the effect of reperfusion on the
rapidity and amplitude of T wave inversion after acute myocardial infarction,
1993.
Methods:
Oliva et al. (94) studied 200 AMI patients to assess serial T-wave
changes as prognostic indicators.
Findings:
Ninety percent of patients with reperfusion demonstrated a maximum
T-wave negativity of >/= 3 mm in the lead that initially showed the greatest
ST elevation within 48 hours of CP onset.
Seventy-six percent of patients with no reperfusion demonstrated a
maximum T-wave negativity of </= 2 mm within 72 hours. Oliva et al. conclude that rapid evolution and deepening of the T-wave
may be useful noninvasive markers of reperfusion.
Matetzky S et al., Early T wave
inversion after thrombolytic therapy predicts better coronary perfusion:
clinical and angiographic study, 1994.
Methods: Matetzky (336) et al. performed admission and
pre-discharge angiography and radionuclide ventriculography on 94 consecutive
AMI patients who received tPA.
Findings: Early
T-wave inversion (< 24 hours) was associated with greater IRA patency,
better perfusion grade, and a more benign in-hospital course. Additionally, although the number of patients
with normal EF’s (>55%) at presentation was similar, 71% of patients with
early T-wave inversion had a normal EF at discharge, vs. 44% of patients
without early T-wave inversion.
Increased pain
and ST elevation post-thrombolytic therapy
Dissman R et al., Sudden
increase of the ST segment elevation at a time of reperfusion predicts
extensive infarcts in patients with intravenous thrombolysis, 1993.
Methods: Dissman et al. (332) measured ST elevation
and CK every 15 minutes after thrombolytic administration in 61 AMI
patients.
Findings: Eight patients showed increased ST elevation
immediately after reperfusion. This was
associated with an enzymatically very large AMI, a very early enzyme peak, and
much worse LV EF (39% +/- 14 vs. 58% +/- 11, p < 0.0005). Six patients also experienced very clearly
intensified CP at the time of the ST elevation.
The study by Doevendans et al. (156) described above and a study by
Wehrens et al. (157) both found a similar increase in CP after treatment and
before ECG evidence of reperfusion.
Reciprocal
depression and reperfusion
Shah A et al., Comparative
prognostic significance of simultaneous versus independent resolution of ST
segment depression relative to ST segment elevation during acute myocardial
infarction, 1997.
Methods: Shah et al. (143) performed continuous ST
segment monitoring of 413 AMI patients who received thrombolytics; 261 patients
met technical criteria for blinded analysis of ST depression resolution
patterns.
Findings: In-hospital mortality was 13% among patients
whose reciprocal ST depression persisted after resolution of ST elevation vs.
1% mortality for patients whose ST elevation and ST depression resolved
simultaneously.
Reperfusion arrhythmias
Although
there is little literature to support malignant reperfusion ventricular
arrhythmias, many interventionalists and clinicians who treat AMI are certain
that runs of ventricular tachycardia are directly related to opening the IRA,
especially in large infarcts that are reperfused very early.
Gorgels AP et al., Usefulness
of the accelerated idioventricular rhythm as a marker for myocardial necrosis
and reperfusion during thrombolytic therapy in acute myocardial infarction,
1988 and Goldberg S et al., Limitation of infarct size with
thrombolytic agents: electrocardiographic indexes, 1983 and Miller FC
et al., Ventricular arrhythmias during reperfusion, 1986.
Methods: Gorgels et al. (349) and Goldberg et al.
(350) were among the first to describe “reperfusion arrhythmias.” Gorgels et
al. prospectively studied 87 patients admitted with ischemic CP and Goldberg et
al. studied 44 AMI patients who underwent angiography. Miller et al. (351) conducted Holter
monitoring of 52 patients.
Findings: Gorgels et al. found AIVR in 27 of 70 AMI
patients with reperfusion. Goldberg et
al. found some type of reperfusion arrhythmia, most commonly AIVR, in 20 of 27
AMI patients with reperfusion. Miller et
al. found no significant relationship of either AIVR or ventricular tachycardia
with reperfusion or persistent occlusion.
Hohnloser SH et al., Assessment
of coronary artery patency after thrombolytic therapy: accurate prediction
using the combined analysis of three noninvasive markers, 1991.
Methods: Hohnloser et al. (338)
prospectively studied 82 first AMI patients treated with thrombolytics.
Findings: AIVR was associated with reperfusion only in
inferior AMI.
Shah PK et al., Angiographic
validation of bedside markers of reperfusion, 1993.
Findings: Shah et al. (158) (described above) found
that 49% of patients with reperfusion developed AIVR.
Gore JM et al., Arrhythmias in
the assessment of coronary artery reperfusion following thrombolytic therapy,
1988.
Methods: Gore et al. (352) performed angiography
within 8 hours of symptom onset in 67 AMI patients treated with
thrombolytics.
Findings: Fifty-six patients had total IRA occlusion,
25 of whom reperfused within 90 minutes of treatment. Arrhythmias (including AIVR) were not
significantly associated with reperfusion.
Gressin V et al., Holter
recording of ventricular arrhythmias during intravenous thrombolysis for acute
myocardial infarction, 1992.
Methods: Gressin et al. (353) performed 24-hour Holter
monitoring of 40 AMI patients treated with thrombolytics.
Findings: Increased incidence of AIVR was associated
with IRA patency.
Clements IP, The
electrocardiogram in acute myocardial infarction, 1998.
Findings: Clements (335) cites a thesis by Veldkamp,
who combined analysis from 6 studies (317 patients) and found that early AIVR
predicted patency with a specificity of 97% but a sensitivity of only 45%.
Vectorcardiography
Dellborg M et al., Dynamic QRS
complex and ST segment vectorcardiographic monitoring can identify vessel patency
in patients with acute myocardial infarction treated with reperfusion therapy,
1991.
Findings: Dellborg et al. (354) identified 15 of 16
patients with reperfusion and 5 of 6 with persistent occlusion using
vectorcardiographic analysis of ST vectors.
Further detail is beyond the scope of this book. See Clements (335) for an excellent
discussion of alternative electrocardiographic methods such as
vectorcardiography and precordial mapping.
See also von Essen et al. (355) and Badir et al. (356) for vectorcardiographic
analyses of reperfusion.
Rescue PCI
Ross AM et al., Rescue
angioplasty after failed thrombolysis: technical and clinical outcomes in a
large thrombolysis trial, 1998.
Methods: Ross et al. (323) analyzed GUSTO-1 (see
Appendix) data on rescue angioplasty, defined as angioplasty undertaken within
6 hours of the start of thrombolytic therapy.
They compared 198 patients selected non-randomly for rescue angioplasty,
226 patients with failed thrombolysis who were managed conservatively, and 1058
patients with successful thrombolysis.
Findings: Patients with rescue angioplasty had more
impaired LV function prior to intervention.
Rescue was successful in 88.4% of occluded arteries, resulting in TIMI-3
flow in 68%. Successful rescue angioplasty
was associated with better LV function and lower mortality than
conservative management of occluded arteries.
Neither bleeding complications (8.6% vs. 6.8%) nor the need for CABG
(1.0% vs. 0.4%) differed significantly between the 2 groups.
Ellis SG et al., Randomized
comparison of rescue angioplasty with conservative management of patients with
early failure of thrombolysis for acute anterior myocardial infarction, 1994.
Methods: Ellis et al. (357) randomized 151 patients
with first anterior AMI and failed thrombolysis, as determined by angiography
done within 8 hours after treatment, to angioplasty or to conservative
management.
Findings: Angioplasty performed at a mean of 4.5 +/-
1.9 hours after thrombolytic therapy was successful in 72 of 78 (92%)
patients. Outcomes in the angioplasty
vs. conservatively managed groups, respectively, were death in 5% vs. 10% (P =
0.18), severe heart failure in 1% vs. 7% (P = 0.11), and either death or severe
heart failure in 6% vs. 17% (P = 0.05).
LV function at rest did not differ.
McKendall GR et al., Value of
rescue percutaneous transluminal coronary angioplasty following unsuccessful
thrombolytic therapy in patients with acute myocardial infarction, 1995.
Methods: McKendall et al. (358) studied 133 patients
enrolled in TIMI Phase I Open Label and Phase II trials; 100 had received no
rescue angioplasty and 33 patients had undergone rescue angioplasty by protocol
(not by physician choice) if the 90-minute angiogram revealed persistent IRA
occlusion.
Findings: Time to angioplasty from symptom onset or
from thrombolytic treatment is not stated, but appears to be 90 to 120
minutes. The two groups had similar
baseline features. Rescue was
technically successful in 26 of 33 patients (82%). Mortality at 21 days was 12% in the rescue
group and 7% in the no-rescue group (p=NS).
Failed rescue was associated with a mortality of 33%. Mean LV EF was the same in both groups.
CORAMI Study Group, Outcome of
attempted rescue coronary angioplasty after failed thrombolysis for acute
myocardial infarction, 1994.
Methods: The CORAMI Study Group (359) evaluated short
and mid-term outcomes of 299 consecutive AMI patients who received
thrombolytics < 6 hours after symptom onset and underwent angiography at 90
minutes post-thrombolytics.
Findings: Of 299 patients, 87 (29%) had failed
thrombolysis (TIMI-0 to -1 flow), of whom 72 underwent rescue angioplasty within
8 hours of symptom onset. Seven
patients (10%) were in cardiogenic shock at the time of angiography. Technical success (TIMI-3 flow) was achieved
in 65 patients (90%) at a mean of 300 +/- 101 minutes after thrombolytic
therapy. Nine patients (12%) had
access site hematoma. Three patients
(4%) died, 2 of 65 successful rescues and 1 of 7 failed rescues.
Gibson C et al., Rescue
angioplasty in the Thrombolysis in Myocardial Infarction (TIMI) 4 trial, 1997.
Methods: Gibson et al. (360) studied 95 AMI patients
with failed thrombolysis (TIMI 0-1 flow) in the TIMI-4 trial.
Findings: Fifty-eight patients underwent rescue
angioplasty 120 minutes post-thrombolytic therapy and 37 had no rescue
angioplasty. Rescue and non-rescue
groups had similar baseline characteristics.
Fifty-two of 58 procedures were successful. In-hospital adverse outcomes, including
death, recurrent AMI, severe CHF, cardiogenic shock, and EF < 40%, occurred
in 35% of rescue cases (29% of successful rescues and 83% of failed rescues, p = 0.01), and also in 35% of
non-rescue cases (p = NS).
Miller JM et al., Effectiveness
of early coronary angioplasty and abciximab for failed thrombolysis (reteplase
or alteplase) during acute myocardial infarction (results from the GUSTO-III
trial), 1999.
Methods: Miller et al (361) prospectively studied 392
patients entered into the GUSTO-III trial (reteplase vs. tPA for STEMI) (362)
who underwent rescue angioplasty in a nonrandomized fashion; 83 patients
received abciximab and 309 did not.
Findings: When adjusted for baseline differences,
patients who received abciximab had significantly lower mortality. Incidence of severe bleeding (without ICH),
with vs. without the use of abciximab during angioplasty was 3.5% vs. 1.0% (p =
0.08).
Ellis SG et al., Review of
immediate angioplasty after fibrinolytic therapy for acute myocardial
infarction, 2000.
Methods: Ellis et al. (324)
performed a meta-analysis of 9 heterogeneous randomized trials of rescue
angioplasty (1456 patients).
Findings: Rescue angioplasty decreased the incidence of
CHF, death, and recurrent MI.
In summary, although
the value of rescue PCI makes intuitive and scientific sense, the available
studies are too small and the methodology inadequate for definite
conclusions. All of the studies had a
minimum delay of 2 hours and a mean delay of 4-5 hours between thrombolytic
therapy and balloon inflation. None used
up-to-date technique including stents, abciximab, and/or clopidogrel. We
recommend rescue PCI for large infarctions with no ECG evidence of reperfusion
at one hour post-thrombolytic therapy unless and until there are studies that take these factors into
account and demonstrate lack of efficacy.
Reocclusion
Langer A et al., Prognostic
significance of ST segment shift early after resolution of ST elevation in
patients with myocardial infarction treated with thrombolytic therapy: the
GUSTO-I ST Segment Monitoring Substudy, 1998.
Methods: Langer et al. (363) performed ST segment
monitoring within 30 minutes of thrombolytic therapy in 734 AMI patients.
Findings: “ST segment shift,” defined as elevation of
>/= 1 mm in the 6-24 hours after reperfusion, was correlated with 7.8%
mortality at 30 days and 10.3% mortality at 1 year vs. 2.3% and 5.7% mortality
respectively for patients without ST shift.
Ohman EM et al., Consequences
of reocclusion after successful reperfusion therapy in acute myocardial
infarction, 1991.
Methods: Ohman et al. (89) studied 810 AMI patients
who had angiography performed 90 minutes post-thrombolytic therapy.
Findings: Reperfusion occurred acutely in 735 patients,
645 of whom (88%) underwent angiography 7 days later. IRA REocclusion occurred in 91
patients (14%) and was symptomatic in 53.
Reocclusion was associated with greater in-hospital mortality (11% vs.
4.5%), a more complicated hospital course, and initial angiographic findings including
RCA stenosis, a greater degree of stenosis, and lower TIMI flow grade.
Dissman R et al., Early
recurrence of ST-segment elevation in patients with initial reperfusion during
thrombolytic therapy: impact on in-hospital reinfarction and long-term vessel
patency, 1994.
Methods: Dissman et al. (364) performed
24-hour Holter monitoring on 81 AMI patients.
Findings: ST resolution within the first 4 hours
occurred in 67 patients (83%), 31 of whom (46%, Group 1a) did have subsequent
ST re-elevations and 36 of whom (54%, Group 1b) did not. Group 1a had a much greater incidence of
CK-MB-confirmed re-infarction (26% vs. 6%) and angiographic occlusion at
follow-up (40% vs. 17%) than Group 1b.
Veldkamp RF et al., Performance
of an automated real-time ST segment analysis program to detect coronary
occlusion and reperfusion, 1996.
Methods: Veldkamp et al. (212) used an automated
real-time ST segment analysis program to detect reocclusion during 78 balloon
occlusions in 31 patients.
Findings: The program detected balloon reocclusion and
reperfusion within seconds of all occlusions that caused a peak ST elevation
>/= 0.2 mV.
Krucoff MW et al., Stability of
multilead ST-segment "fingerprints" over time after percutaneous
transluminal coronary angioplasty and its usefulness in detecting reocclusion,
1988.
Methods: Krucoff et al. (190) analyzed multi-lead ST
segment recordings performed during angioplasty in 39 patients.
Findings: Similar to Bush et al. (83) described above,
within one hour, balloon occlusion during repeat angioplasty resulted in an
identical “ischemic fingerprint” 90% of the time. AMI of the same vessel within 24 hours of the
balloon inflation resulted in this ischemic fingerprint 87% of the time.
Thus, reocclusion reliably
produces the initial ECG pattern of infarction.
Monitoring for reocclusion
can be done using continuous ST segment monitoring.
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Thanks for the excerpt. I remember you mentioned that you are considering the possibility of publishing an electronic version of the book. Are there still any chances? Unfortunately, after a year of monitoring the availability of printed copies is still on the "inaccessible" level.
ReplyDeletesend me your email to: dr.smiths.ecg.blog@gmail.com and I will send you a pdf through dropbox!
DeleteSteve Smith