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GE Healthcare
Jun 30, 2020 5 min read
Thankfully, clinicians can keep tabs on QT intervals with continuous monitoring, which has made
tremendous advances in recent years. Ian Rowlandson, GE Healthcare Chief Engineer and Scientist
for Diagnostic Electrocardiography, has helped to develop algorithms that go into GE Healthcare’s
ECG diagnostic carts and bedside monitors – including those that examine the complex and often
overlooked problem of long QT. Clinical View sat down with Ian to discuss long QT epidemiology and
signs, long QT measurement and reversal strategies, and the advantages GE Healthcare delivers to
the QT monitoring landscape.
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Ian Rowlandson: An electrocardiogram (ECG) measures the QT interval from the earliest onset of
depolarization (the start of the Q wave) to the latest offset of repolarization (the end of the T wave)—
or in simpler terms, the time it takes the heart to recharge between beats. A QT interval corrected
for heart rate results in the QTc value (corrected QT).
Prolongation of the QT/QTc interval, also referred to as long QT, occurs when the heart takes longer
than usual to recharge between beats. Long QT sets the stage for TdP, an abnormal and potentially
fatal heart rhythm.
Ian Rowlandson: There are two types of long QT: congenital and acquired. Congenital long QT cases
don’t generally come to light unless a patient exhibits symptoms such as fainting or blacking out,
which would lead to diagnosis and treatment, often of the patient’s entire family.
Acquired long QT may be either drug-induced or triggered by clinical conditions such as electrolyte
imbalances, arrhythmias, poor liver or heart function.
Drug-induced long QT is a dire concern, particularly in hospital settings, where use of QT-prolonging
drugs is prevalent. QT-prolonging drugs literally poison the ion channels in the heart membrane. The
list of drugs likely to prolong QT continues to grow and includes anti-arrhythmics such as Sotalol as
well as anti-psychotics, anti-depressants, antibiotics and some anesthetics. (Note: Sites such
as crediblemeds.org categorize drugs by their potential to cause long QT and/or TdP.)
Ian Rowlandson: That depends on the type. Up to one in 2,000 individuals may have congenital long
QT1, although we are learning that these genetic abnormalities might be more common than
originally thought.
Acquired long QT is thought to be even more common than congenital long QT.
A nationwide study from Denmark found that of 1,363 SCDs, nearly 20 percent of the deceased had
received a QT-prolonging drug less than 90 days before death.2
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Unfortunately, when clinicians are confronted with long QT, they don't know whether it is acquired,
congenital or drug-induced. They must simply deal with it.
Ian Rowlandson: There are no hard and fast rules, but an American Heart Association (AHA) and
American College of Cardiology Foundation (ACCF) joint statement on TdP prevention in hospital
settings3 views QTc prolongation to greater than 500 milliseconds as a prime ECG risk factor for TdP.
However, additional factors such as advanced age, female gender, administration of a QT-prolonging
drug, poor electrolytes, poor cardiac health, etc. increase the TdP risk.
This 500-millisecond long QT threshold is important, particularly as a benchmark for hospitals in the
defense of SCD cases. However, the ACC-ACCF also concede that, particularly for drug-induced long
QT, the change in QT over time may be more important than the absolute QT.3 That is why precise
and consistent QT monitoring matters, and why a single ECG may not be sufficient for patients
prescribed a QT-prolonging drug.
Ian Rowlandson: Long QT is extremely serious. Long QT causes death and, in cases of drug-induced
long QT, is often initiated by a clinician prescribing a QT-prolonging drug. When long QT goes
unnoticed, it creates a perfect storm for a life-threatening TdP event.
The irony is that long QT is preventable and reversible. Clinicians must be educated on QT
measurement as well as signs and treatment of long QT.
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Mistakes in QT measurement occur for a number of reasons, including technically suboptimal ECGs.
Another factor is that besides the ability to recognize long QT on the ECG, clinicians must also be
skilled at reading T- and U-wave shapes. A distorted T-wave—one that is flat, asymmetric and
notched—is another TdP red flag. In drug-induced long QT, the distorted T-wave may merge with a
bigger U-wave. Some clinicians have never seen a true prolonged QT or distorted T-wave on the ECG
of a TdP patient, but they can be taught to recognize and distinguish abnormal T- and U-wave shapes.
Ian Rowlandson: Step one is taking a thorough medical history, including any prescribed QT-
prolonging drugs and previously mentioned TdP risk factors.
Ideally, before administering any QT-prolonging drug, particularly a high-risk drug such as Sotalol, the
clinician should test the patient’s tolerance to the drug. To do so, the clinician should first conduct a
diagnostic resting 12-lead ECG to baseline the QT. Then, once the drug is administered, the patient
should be placed on a monitor to track the QT.
The clinician should watch for signs of arrhythmia. These include an increase in the QT interval by
more than 60 milliseconds from pre-drug baseline, QT prolongation to greater than 500 milliseconds,
a distorted T-U wave, and other markers. Should any warning signs occur, another 12-lead ECG
should be taken to clarify the reading.
These readings can be taken over a six- or 12-hour period and may include additional 12-lead ECGs.
With high-risk drugs like Sotalol, the patient might require admission and monitoring for up to three
days to ensure safe tolerance.
Finally, for QT monitoring consistency, the AHA-ACCF recommend the use of the same recording
device, ECG lead, heart rate correction formula, etc. both before and after drug administration.3
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Ian Rowlandson: The clinician has multiple options, including discontinuing the QT-prolonging drug,
adjusting electrolytes, administering magnesium sulfate, or considering a temporary pacemaker.
These patients should remain in the hospital unit with the highest level of ECG monitoring
surveillance and available defibrillation.
In developing its GE Marquette™ 12SL™ ECG analysis program, GE Healthcare fine-tuned the
algorithm’s QT measurements by participating in studies to determine drugs’ QT prolongation and
TdP risk. The 12SL algorithm received such high marks for accuracy and precision that no manual
intervention was required in selected drug tests.5
To support consistency of QT measurement, GE Healthcare has implemented its 12SL ECG algorithm
across all diagnostic ECGs and monitoring systems. As an added feature, the monitor can interface
with patients’ historical ECGs that were done on a resting electrocardiograph. That's important,
because the installed base of historical access of prior ECGs is much larger in GE Healthcare versus in
other.
consistent measurements compared to methods that use averaging or eliminate selected leads from
the calculation.
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Ian Rowlandson: First, we are taking a closer look at T-wave morphology as a marker for long QT
and TdP risk. Clinicians have requested more advanced tools for this purpose. A second related
priority is looking at T-wave shapes in the presence of atrial fibrillation, which is treated with Sotalol,
with its attendant risks for QT prolongation and TdP risk.
References
1. Professor Dr. med. Patrick Friederich, Monitoring of the QT interval in perioperative and critical
care. GE Healthcare white paper. Accessed May 21, 2019.
2. Risgaard, B., et al., Sudden Cardiac Death: Pharmacotherapy and Proarrhythmic Drugs: A
Nationwide Cohort Study in Denmark. JACC: Clinical Electrophysiology, 2017. 3(5): p. 473-481.
Accessed May 21, 2019.
3. Drew, B.J., et al., Prevention of torsade de pointes in hospital settings: a scientific statement from
the American Heart Association and the American College of Cardiology Foundation. Circulation,
2010. 121(8): p. 1047-60. Accessed May 20, 2019.
4. Viskin, S., et al., Inaccurate electrocardiographic interpretation of long QT: the majority of
physicians cannot recognize a long QT when they see one. Heart Rhythm Society, 2005. 2(6): p.
569-74. Accessed May 20, 2019.
5. Hnatkova, K., et al., Precision of QT Interval Measurement by Advanced Electrocardiographic
Equipment. Pacing Clin Electrophysiol, 2006. 29(11): p. 1277-84. Accessed May 21, 2019.
6. Kligfield, P., et al., Comparison of automated interval measurements by widely used algorithms in
digital electrocardiographs. American Heart Journal, 2018. Accessed May 19, 2019.
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