EMS was dispatched for a 30-something male who feels his heart is racing. Sudden onset.
The patient had no previous medical history.
Vitals were normal except for a heart rate of 226.
A prehospital 12-lead was recorded:
The patient was given 6mg, then 12 mg, of adenosine, without a change in the rhythm.
He arrived in the ED and had an immediate bedside cardiac ultrasound while this ECG was being recorded.
The bedside ultrasound (video not available) reportedly showed only a slightly reduced LV function.
Here is the ECG:
There is a wide complex regular tachycardia at a rate of 226. The first part of the QRS is slow onset (see magnification below). The differential is VT vs. AVRT.
Could it be RVOT (Right ventricular outflow tract VT). No, this requires inferior axis and LBBB morphology. There is no inferior axis.
RVOT VT:
Could it be fascicular VT or Bundle Branch VT (i.e., idiopathic VT)? No, because the first part of the QRS is slow onset (see magnified V1-V6 below).
Could it be standard VT? Yes, but this would be unusual in someone with no cardiac history and a reasonably good contractility on echo.
Could it be AVRT? Yes.
If AVRT, adenosine is likely to work, but it did not work in the prehospital setting.
Perhaps:
1) it is VT
2) the dose of adenosine was too low or
3) the adenosine was not given fast enough.
V1-V6 magnified, with lines marking onset of QRS and end of first part of QRS:
Case continued.
The patient was immediately electrically cardioverted.
Here is the post cardioversion ECG:
He underwent an MRI to look for scar as a nidus for VT:
IMPRESSION
1) Borderline LV function with no focal wall motion abnormalities
2) Normal dimensions of all cardiac chambers
3) No evidence of myocardial scar on delayed enhancement sequences after contrast administration
4) No MRI evidence of arrhythmogenic right ventricular dysplasia.
EP note:
"He had wide-complex monomorphic tachycardia with extreme axis concerning for VT. He is young and the tachycardia was not polymorphic in nature, so this is very unlikely to be an ischemic rhythm and much more likely scar mediated. He got an MR, however that showed no scar or evidence of AVRD and he had a stress test with no evidence of inducible ischemia with almost 20 METs."
He underwent an EP study 5/10/2022 for evaluation of pre-excitation/accessory tract which found a left sided accessory pathway - he is currently in the EP study now. Cardiology consults will continue to follow in the morning and address necessary cardiology follow-up.
- In my opinion — it is a mistake to interpret arrhythmias in strict "binary" fashion — since rather than "either/or" — optimal interpretation is more of a probability statement.
- Rather than calling this rhythm "definitely" VT — optimal interpretation would entail description of this rhythm as a regular WCT ( = Wide-Complex Tachycardia) at ~225-230/minute, without clear sign of atrial activity.
- The above statistics are derived from an unselected adult population. Additional factors may help greatly to narrow down and increase relative probability of one or another diagnosis.
- For example — in an adult of a "certain age" (ie, a patient beyond the "young adult" age range — usually beginning near "middle-age") — IF the patient has underlying heart disease — then even before looking at the actual ECG, statistical odds that a regular WCT rhythm without sign of atrial activity will turn out to be VT approach 90%.
- Use of QRS morphology may help to further increase the accuracy of this prediction. For example, IF this patient were an adult of a "certain age" who had known underlying heart disease — the fact that the QRS complex during the WCT rhythm in Figure-1 is extremely wide — with an amorphous QRS complex in all anterior leads, in which there is very slow initial depolarization — with predominant negativity of the QRS in lead V6 — and — with a QRS morphology that fails to resemble any form of known conduction defect — would suggest >95-98% likelihood that this WCT rhythm was VT.
- Not commonly appreciated is how surprisingly common VT may be in younger adult patients who present with a regular WCT rhythm without clear sign of P waves. That said — such patients almost always have idiopathic VT, in which there is no underlying heart disease!
- I've reproduced in Figure-2 — the KEY features of QRS morphology characteristic of some form of idiopathic VT. These generally entail fascicular VT (most commonly manifesting RBBB-LAHB or RBBB-LPHB-like morphology) or RVOT VT (recognized by LBBB-like morphology in the chest leads with an inferior frontal plane axis). The marked QRS widening, with amorphous shape in anterior leads seen in today's tracing is clearly not suggestive of idiopathic VT.
- BOTTOM Line: As per Dr. Smith — the fact that today's patient was a previously healthy young adult who presents with the markedly abnormal QRS morphology seen in the WCT shown in Figure-1 — dramatically reduces the likelihood of VT (especially given no sign of anatomic cardiomyopathy on bedside ultrasound!).
Figure-1: The initial ECG that was recorded in the ED. |
- As per Dr. Smith — this establishes AVRT as the principal diagnostic consideration. The overwhelming majority of AVRT reentry SVTs are conducted "orthodromic" (ie, passing first down the normal AV nodal pathway — thereby resulting in a narrow QRS complex).
- That said — from 1-to-5% of reentry AVRT rhythms are "antidromic", in which the reentry circuit passes first down the AP (Accessory Pathway) — which results in a wide QRS. Antidromic AVRT is precisely the mechanism for the overly wide and unusual QRS morphology seen in today's case!
- There is a tendency to assume that regular WCT rhythms without atrial activity are VT. While true in >95% of cases — it is well to keep in mind that on occasion (especially in a previously healthy younger adult) — we may see a regular WCT due to antidromic AVRT. Distinctinction between antidromic AVRT and VT may not be possible from the single ECG obtained during the WCT rhythm (as was the case today!).
Figure-2: Review of the KEY features regarding Idiopathic VT (which I previously published in My Comment at the bottom of the page in the May 14, 2022 post in Dr. Smith's ECG Blog). |
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