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In Reply: We thank Dr. Ratanapo and colleagues for their interest in our article. As we mentioned in our paper, and as they emphasized, the QT interval response to heart rate variation seems to be minimal. They wonder if using a beta-blockers in addition to Holter monitoring can provide a better estimate of the “true corrected QT interval” since it will allow the measurement of corrected QT with slower heart rates. While we agree that Holter monitoring may provide an opportunity to observe the lack of prolongation of the QT interval when the heart rate slows down naturally (eg, during sleep), we have reservations about the other points.
First, we prefer not to use the term “true corrected QT interval” because, as we mentioned in our article, the correction formulas do not perform well in short QT syndrome. A better thing would be to use the QT interval itself, no matter what the heart rate is.
Second, whether beta-blockers would alter the heart rate without altering the QT interval is something that deserves to be evaluated in patients with an established diagnosis of short QT syndrome. Since catecholamines can cause shortening of the QT interval,1 could beta-blockers have a different effect on the QT interval in patients with and without short QT syndrome? To our knowledge, there are no data that specifically address this question.
The last point we would like to emphasize is the complexity of making the diagnosis of short QT syndrome. Electrocardiographic criteria, especially when equivocal, should probably not be the sole diagnostic basis for short QT syndrome. A personal or family history of arrhythmias, with or without genetic testing, has additive value as demonstrated by the excellent paper by Gollob et al.2
- Bjerregaard P, Gusak I. Short QT syndrome: mechanism, diagnosis, and treatment. Nat Clin Pract Cardiovasc Med 2005; 2:84–87.
- Gollob MH, Redpath CJ, Roberts JD. The short QT syndrome: proposed diagnostic criteria. J Am Coll Cardiol 2011; 57:802–812.
In Reply: We thank Dr. Ratanapo and colleagues for their interest in our article. As we mentioned in our paper, and as they emphasized, the QT interval response to heart rate variation seems to be minimal. They wonder if using a beta-blockers in addition to Holter monitoring can provide a better estimate of the “true corrected QT interval” since it will allow the measurement of corrected QT with slower heart rates. While we agree that Holter monitoring may provide an opportunity to observe the lack of prolongation of the QT interval when the heart rate slows down naturally (eg, during sleep), we have reservations about the other points.
First, we prefer not to use the term “true corrected QT interval” because, as we mentioned in our article, the correction formulas do not perform well in short QT syndrome. A better thing would be to use the QT interval itself, no matter what the heart rate is.
Second, whether beta-blockers would alter the heart rate without altering the QT interval is something that deserves to be evaluated in patients with an established diagnosis of short QT syndrome. Since catecholamines can cause shortening of the QT interval,1 could beta-blockers have a different effect on the QT interval in patients with and without short QT syndrome? To our knowledge, there are no data that specifically address this question.
The last point we would like to emphasize is the complexity of making the diagnosis of short QT syndrome. Electrocardiographic criteria, especially when equivocal, should probably not be the sole diagnostic basis for short QT syndrome. A personal or family history of arrhythmias, with or without genetic testing, has additive value as demonstrated by the excellent paper by Gollob et al.2
In Reply: We thank Dr. Ratanapo and colleagues for their interest in our article. As we mentioned in our paper, and as they emphasized, the QT interval response to heart rate variation seems to be minimal. They wonder if using a beta-blockers in addition to Holter monitoring can provide a better estimate of the “true corrected QT interval” since it will allow the measurement of corrected QT with slower heart rates. While we agree that Holter monitoring may provide an opportunity to observe the lack of prolongation of the QT interval when the heart rate slows down naturally (eg, during sleep), we have reservations about the other points.
First, we prefer not to use the term “true corrected QT interval” because, as we mentioned in our article, the correction formulas do not perform well in short QT syndrome. A better thing would be to use the QT interval itself, no matter what the heart rate is.
Second, whether beta-blockers would alter the heart rate without altering the QT interval is something that deserves to be evaluated in patients with an established diagnosis of short QT syndrome. Since catecholamines can cause shortening of the QT interval,1 could beta-blockers have a different effect on the QT interval in patients with and without short QT syndrome? To our knowledge, there are no data that specifically address this question.
The last point we would like to emphasize is the complexity of making the diagnosis of short QT syndrome. Electrocardiographic criteria, especially when equivocal, should probably not be the sole diagnostic basis for short QT syndrome. A personal or family history of arrhythmias, with or without genetic testing, has additive value as demonstrated by the excellent paper by Gollob et al.2
- Bjerregaard P, Gusak I. Short QT syndrome: mechanism, diagnosis, and treatment. Nat Clin Pract Cardiovasc Med 2005; 2:84–87.
- Gollob MH, Redpath CJ, Roberts JD. The short QT syndrome: proposed diagnostic criteria. J Am Coll Cardiol 2011; 57:802–812.
- Bjerregaard P, Gusak I. Short QT syndrome: mechanism, diagnosis, and treatment. Nat Clin Pract Cardiovasc Med 2005; 2:84–87.
- Gollob MH, Redpath CJ, Roberts JD. The short QT syndrome: proposed diagnostic criteria. J Am Coll Cardiol 2011; 57:802–812.