Written by Pendell Meyers
A male in his 60s with no known past medical history presented at midnight with chest pain over the past 3 hours. The pain started just after eating, and at first he thought it was "reflux," however he decided to call 911 after a few hours when it did not improve.
Here is his presenting ECG:
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| What do you think? |
Here are the relevant findings:
Slight STE in V1
2.5 mm STE in V2
Slight STD in V4-V6
Definite STD in II, III, and aVF
Hyperacute T-waves in V2, and likely also in aVL
These findings are highly specific for LAD occlusion. We have many cases of this pattern on this blog, involving STE and hyperacute T-waves in V1-V2, with STD in the lateral leads (see below for links). In this case there is also reciprocal STD in inferior leads and hyperacute T-waves in aVL.
Side note: Sometimes this pattern includes morphology which some have described as "new tall T-wave in V1," or sometimes "T-wave in V1 greater than in V6" which is essentially just a description of a hyperacute T-wave in V1, with the exception that it would be better described as both tall and fat/large/wide/bulky T-waves, not just "tall". Dr. Smith noted "new tall T-wave in V1" in 14% of cases of early repolarization vs. 34% of subtle LAD occlusions in the derivation study of the anterior OMI formula. This initial ECG does not have this pattern, however lookout for this pattern in the serial ECGs.
Our team recognized that this ECG represents LAD occlusion. But it does not technically meet STEMI criteria. We immediately called the interventionalist to explain our concerns. They evaluated the patient and were also concerned, however they felt that immediate cath was not warranted because the STEMI criteria were not met.
We began maximal medical therapy, including nitroglycerin infusion.
To make matters more difficult, the first troponin of course returned undetectable (our contemporary assay rarely budges until 4-6 hours after onset of OMI).
During this time, we incessantly performed serial ECGs, trying to find one that convinced cardiology.
Here is the clearest one we could get:
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| By my measurement, there is at least 1 mm in V1, and at least 2 mm in V2. This meets formal STEMI criteria for a male over age 40. The T-wave in V1 is now relatively hyperacute compared to the first ECG. Lead aVL is definitely hyperacute now that we have a clear tracing of it. ST depression in V4-V6 is more evident. |
Despite the fact that we believed this ECG meets STEMI criteria, cardiology colleagues disagreed. This is not uncommon, and not unexpected, as prior evidence (see the end of the post for literature review) shows that we have very poor inter- and even intra-reader reliability for measuring the ST segment.
The cardiologist stayed in the room personally to see if the patients symptoms and ECG findings would be persistent despite medical therapy.
Sure enough, the ECG findings and ischemic pain indeed persisted over the course of 20-25 minutes, and the cardiologists correctly decided to proceed with emergent cath rather than further medical management, as is recommended by multi-national guidelines regardless of the ECG findings or interpretation.
We got one last ECG before the patient went to cath:
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| Now there is ST depression in V3, almost as if a de Winter's T-wave is developing. |
100% mid LAD thrombotic occlusion was found and stented with excellent angiographic result.
Here is an ECG the next day confirming downstream reperfusion:
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| Of note, there is lack of pathologic Q-waves and expected reperfusion findings, suggesting relatively favorable infarct size compared to the at-risk territory. |
Echo showed wall motion abnormalities of the anterior, septal, lateral, and apical areas.
Peak troponin T was 1.87 ng/mL.
Learning Points:
We must be expert at subtle ECG findings of Occlusion MI, because our current paradigm is insufficient.
Serial ECGs can often help to make a difficult decision easier.
Persistent ischemia despite maximal medical management is highly likely to be due to Occlusion MI and is an indication for emergent catheterization regardless of ECG findings.
Contemporary troponin assays are frequently undetectable within the first 4-6 hours of Occlusion MI, when the benefit of emergent reperfusion is maximal.
See these other cases of LAD occlusion with similar subtle patterns of STE and hyperacute T-waves in V1-V2, with STD in V5-V6:
How long would you like to wait for your Occlusion MI to show a STEMI? Sometimes serial ECGs minimizes the delay.
McCabe et al, Journal of the American Heart Association. Physician accuracy in interpreting potential ST-segment elevation myocardial infarction electrocardiograms. Journal of the American Heart Association 2013;2:e000268.
A cross-sectional survey was performed by having emergency medicine physicians, cardiologists, and interventional cardiologists review 36 ECGs from the Activate-SF database of prospective STEMI activations. 12 (33%) of the 36 cases had no culprit lesion (defined as no STEMI), whereas the other 24 (66%) were true positives with total acute occlusion (defined as STEMI). This corresponded well with the actual overall rate of false positive STEMI activations in the entire registry of 36% which was recorded from prospective practice. For each ECG clinicians were asked, “based on the ECG above, is there a blocked coronary artery present causing a STEMI?” 124 physicians interpreted a total of 4392 ECGs. Overall kappa value of interreader agreement was only 0.33, reflecting poor agreement. Overall sensitivity and specificity for true positive STEMI (occlusion) was only 65% (95%CI 63-67%) and 79% (95%CI 77-81%). There was a 6% increase in the odds of successful interpretation with every 5 years of experience since medical school graduation. After adjusting for experience there was no difference in the odds of overall accurate interpretation between specialties. However, interventional cardiologists had the highest group specificity at 89%, while emergency medicine attendings had the highest group sensitivity at 74%. This excellent study is supported by many others showing poor inter-rater reliability (35-37).
Carley et al. What’s the point of ST elevation? Emergency Medicine Journal 2002;19:126-128.
Cross sectional study in which 63 clinicians who commonly prescribe thrombolytics for acute MI were asked to identify and quantify the degree of STE present in 3 sample ECG complexes. They were also asked to mark the ECG where they identified the J-point. Overall, STE was not identified in 23 (12%) cases. For figures 1-3 below, the percentage of doctors who correctly identified the J-point correctly was 29%, 61%, and 13%.
Tandberg et al. Observer variation in measured ST-segment elevation. Annals of Emergency Medicine 1999 Oct;34;448-52.
A blinded, paired-sample survey was administered to 52 subjects including emergency physicians, emergency medicine residents, and senior medical students. They were given a packet of 40 ECGs, blinded to the fact that it actually consisted of a random order of identical pairs of only 20 ECGs from patients with “enzymatically proven myocardial infarction.” They were asked to measure all ECGs, then the difference between the each reader’s two measurement of the same ECG was studied. The average difference in segment height among all groups was 0.28 mm. Overall statistical agreement between paired ST-segment measurements was very good (K=0.85). However, “one fifth of the time, intraobserver measurements of paired ST-segment elevations differed by more than half a millimeter.” When specifically asked whether the ST-segment elevation was greater than or equal to 2.0 mm, readers disagreed with themselves in 14% of cases.
