Search

Your search keyword '"Zareba, W."' showing total 12 results
Start Over Author "Zareba, W." Publication Type Electronic Resources
12 results on '"Zareba, W."'

1. Independent validation and clinical implications of the risk prediction model for long QT syndrome (1-2-3-LQTS-Risk): comment - Authors' reply

Author

Mazzanti, A, Trancuccio, A, Kukavica, D, Pagan, E, Wang, M, Mohsin, M, Peterson, D, Bagnardi, V, Zareba, W, Priori, S, Mazzanti A., Trancuccio A., Kukavica D., Pagan E., Wang M., Mohsin M., Peterson D., Bagnardi V., Zareba W., Priori S. G., Mazzanti, A, Trancuccio, A, Kukavica, D, Pagan, E, Wang, M, Mohsin, M, Peterson, D, Bagnardi, V, Zareba, W, Priori, S, Mazzanti A., Trancuccio A., Kukavica D., Pagan E., Wang M., Mohsin M., Peterson D., Bagnardi V., Zareba W., and Priori S. G.

Published
2022

2. An International Multicenter Evaluation of Type 5 Long QT Syndrome: A Low Penetrant Primary Arrhythmic Condition

Author

Roberts, J, Asaki, S, Mazzanti, A, Bos, J, Tuleta, I, Muir, A, Crotti, L, Krahn, A, Kutyifa, V, Shoemaker, M, Johnsrude, C, Aiba, T, Marcondes, L, Baban, A, Udupa, S, Dechert, B, Fischbach, P, Knight, L, Vittinghoff, E, Kukavica, D, Stallmeyer, B, Giudicessi, J, Spazzolini, C, Shimamoto, K, Tadros, R, Cadrin-Tourigny, J, Duff, H, Simpson, C, Roston, T, Wijeyeratne, Y, El Hajjaji, I, Yousif, M, Gula, L, Leong-Sit, P, Chavali, N, Landstrom, A, Marcus, G, Dittmann, S, Wilde, A, Behr, E, Tfelt-Hansen, J, Scheinman, M, Perez, M, Kaski, J, Gow, R, Drago, F, Aziz, P, Abrams, D, Gollob, M, Skinner, J, Shimizu, W, Kaufman, E, Roden, D, Zareba, W, Schwartz, P, Schulze-Bahr, E, Etheridge, S, Priori, S, Ackerman, M, Roberts JD, Asaki SY, Mazzanti A, Bos JM, Tuleta I, Muir AR, Crotti L, Krahn AD, Kutyifa V, Shoemaker MB, Johnsrude CL, Aiba T, Marcondes L, Baban A, Udupa S, Dechert B, Fischbach P, Knight LM, Vittinghoff E, Kukavica D, Stallmeyer B, Giudicessi JR, Spazzolini C, Shimamoto K, Tadros R, Cadrin-Tourigny J, Duff HJ, Simpson CS, Roston TM, Wijeyeratne YD, El Hajjaji I, Yousif MD, Gula LJ, Leong-Sit P, Chavali N, Landstrom AP, Marcus GM, Dittmann S, Wilde AAM, Behr ER, Tfelt-Hansen J, Scheinman MM, Perez MV, Kaski JP, Gow RM, Drago F, Aziz PF, Abrams DJ, Gollob MH, Skinner JR, Shimizu W, Kaufman ES, Roden DM, Zareba W, Schwartz PJ, Schulze-Bahr E, Etheridge SP, Priori SG, Ackerman MJ., Roberts, J, Asaki, S, Mazzanti, A, Bos, J, Tuleta, I, Muir, A, Crotti, L, Krahn, A, Kutyifa, V, Shoemaker, M, Johnsrude, C, Aiba, T, Marcondes, L, Baban, A, Udupa, S, Dechert, B, Fischbach, P, Knight, L, Vittinghoff, E, Kukavica, D, Stallmeyer, B, Giudicessi, J, Spazzolini, C, Shimamoto, K, Tadros, R, Cadrin-Tourigny, J, Duff, H, Simpson, C, Roston, T, Wijeyeratne, Y, El Hajjaji, I, Yousif, M, Gula, L, Leong-Sit, P, Chavali, N, Landstrom, A, Marcus, G, Dittmann, S, Wilde, A, Behr, E, Tfelt-Hansen, J, Scheinman, M, Perez, M, Kaski, J, Gow, R, Drago, F, Aziz, P, Abrams, D, Gollob, M, Skinner, J, Shimizu, W, Kaufman, E, Roden, D, Zareba, W, Schwartz, P, Schulze-Bahr, E, Etheridge, S, Priori, S, Ackerman, M, Roberts JD, Asaki SY, Mazzanti A, Bos JM, Tuleta I, Muir AR, Crotti L, Krahn AD, Kutyifa V, Shoemaker MB, Johnsrude CL, Aiba T, Marcondes L, Baban A, Udupa S, Dechert B, Fischbach P, Knight LM, Vittinghoff E, Kukavica D, Stallmeyer B, Giudicessi JR, Spazzolini C, Shimamoto K, Tadros R, Cadrin-Tourigny J, Duff HJ, Simpson CS, Roston TM, Wijeyeratne YD, El Hajjaji I, Yousif MD, Gula LJ, Leong-Sit P, Chavali N, Landstrom AP, Marcus GM, Dittmann S, Wilde AAM, Behr ER, Tfelt-Hansen J, Scheinman MM, Perez MV, Kaski JP, Gow RM, Drago F, Aziz PF, Abrams DJ, Gollob MH, Skinner JR, Shimizu W, Kaufman ES, Roden DM, Zareba W, Schwartz PJ, Schulze-Bahr E, Etheridge SP, Priori SG, and Ackerman MJ.

Abstract

Background: Insight into type 5 long QT syndrome (LQT5) has been limited to case reports and small family series. Improved understanding of the clinical phenotype and genetic features associated with rare KCNE1 variants implicated in LQT5 was sought through an international multicenter collaboration. Methods: Patients with either presumed autosomal dominant LQT5 (N = 229) or the recessive Type 2 Jervell and Lange-Nielsen syndrome (N = 19) were enrolled from 22 genetic arrhythmia clinics and 4 registries from 9 countries. KCNE1 variants were evaluated for ECG penetrance (defined as QTc >460 ms on presenting ECG) and genotype-phenotype segregation. Multivariable Cox regression was used to compare the associations between clinical and genetic variables with a composite primary outcome of definite arrhythmic events, including appropriate implantable cardioverter-defibrillator shocks, aborted cardiac arrest, and sudden cardiac death. Results: A total of 32 distinct KCNE1 rare variants were identified in 89 probands and 140 genotype positive family members with presumed LQT5 and an additional 19 Type 2 Jervell and Lange-Nielsen syndrome patients. Among presumed LQT5 patients, the mean QTc on presenting ECG was significantly longer in probands (476.9±38.6 ms) compared with genotype positive family members (441.8±30.9 ms, P<0.001). ECG penetrance for heterozygous genotype positive family members was 20.7% (29/140). A definite arrhythmic event was experienced in 16.9% (15/89) of heterozygous probands in comparison with 1.4% (2/140) of family members (adjusted hazard ratio [HR] 11.6 [95% CI, 2.6-52.2]; P=0.001). Event incidence did not differ significantly for Type 2 Jervell and Lange-Nielsen syndrome patients relative to the overall heterozygous cohort (10.5% [2/19]; HR 1.7 [95% CI, 0.3-10.8], P=0.590). The cumulative prevalence of the 32 KCNE1 variants in the Genome Aggregation Database, which is a human database of exome and genome sequencing data from now over 140 0

Published
2020

3. Assessment of absolute risk of life-threatening cardiac events in long QT syndrome patients

Author

Wang, M, Peterson, D, Pagan, E, Bagnardi, V, Mazzanti, A, Mcnitt, S, Rich, D, Seplaki, C, Kutyifa, V, Polonsky, B, Barsheshet, A, Kukavica, D, Rosero, S, Goldenberg, I, Priori, S, Zareba, W, Wang, M, Peterson, D, Pagan, E, Bagnardi, V, Mazzanti, A, Mcnitt, S, Rich, D, Seplaki, C, Kutyifa, V, Polonsky, B, Barsheshet, A, Kukavica, D, Rosero, S, Goldenberg, I, Priori, S, and Zareba, W

Abstract

Background: Risk stratification in long QT syndrome (LQTS) patients is important for optimizing patient care and informing clinical decision making. We developed a risk prediction algorithm with prediction of 5-year absolute risk of the first life-threatening arrhythmic event [defined as aborted cardiac arrest, sudden cardiac death, or appropriate implantable cardioverter defibrillator (ICD) shock] in LQTS patients, accounting for individual risk factors and their changes over time. Methods: Rochester-based LQTS Registry included the phenotypic cohort consisting of 1,509 LQTS patients with a QTc ≥ 470 ms, and the genotypic cohort including 1,288 patients with single LQT1, LQT2, or LQT3 mutation. We developed two separate risk prediction models which included pre-specified time-dependent covariates of beta-blocker use, syncope (never, syncope while off beta blockers, and syncope while on beta blockers), and sex by age < and ≥13 years, baseline QTc, and genotype (for the genotypic cohort only). Follow-up started from enrollment in the registry and was censored at patients’ 50s birthday, date of death due to reasons other than sudden cardiac death, or last contact, whichever occurred first. The predictive models were externally validated in an independent cohort of 1,481 LQTS patients from Pavia, Italy. Results: In Rochester dataset, there were 77 endpoints in the phenotypic cohort during a median follow-up of 9.0 years, and 47 endpoints in the genotypic cohort during a median follow-up of 9.8 years. The time-dependent extension of Harrell’s generalized C-statistics for the phenotypic model and genotypic model were 0.784 (95% CI: 0.740–0.827) and 0.785 (95% CI: 0.721–0.849), respectively, in the Rochester cohort. The C-statistics obtained from external validation in the Pavia cohort were 0.700 (95% CI: 0.610–0.790) and 0.711 (95% CI: 0.631–0.792) for the two models, respectively. Based on the above models, an online risk calculator estimating a 5-year risk of life-t

Published
2022

4. Independent validation and clinical implications of the risk prediction model for long QT syndrome (1-2-3-LQTS-Risk)

Author

Mazzanti, A, Trancuccio, A, Kukavica, D, Pagan, E, Wang, M, Mohsin, M, Peterson, D, Bagnardi, V, Zareba, W, Priori, S, Mazzanti, Andrea, Trancuccio, Alessandro, Kukavica, Deni, Pagan, Eleonora, Wang, Meng, Mohsin, Muhammed, Peterson, Derick, Bagnardi, Vincenzo, Zareba, Wojciech, Priori, Silvia G, Mazzanti, A, Trancuccio, A, Kukavica, D, Pagan, E, Wang, M, Mohsin, M, Peterson, D, Bagnardi, V, Zareba, W, Priori, S, Mazzanti, Andrea, Trancuccio, Alessandro, Kukavica, Deni, Pagan, Eleonora, Wang, Meng, Mohsin, Muhammed, Peterson, Derick, Bagnardi, Vincenzo, Zareba, Wojciech, and Priori, Silvia G

Abstract

Aims: Risk stratification of patients with long QT syndrome (LQTS) represents a difficult task. In 2018, we proposed a granular estimate of the baseline 5-year risk of life-threatening arrhythmias (LAE) for patients with LQTS, based on the genotype (long QT syndrome Type 1, long QT syndrome Type 2, and long QT syndrome Type 3) and the duration of the QTc interval. We sought to externally validate a novel risk score model (1-2-3-LQTS-Risk model) in a geographically diverse cohort from the USA and to evaluate its performance and assess potential clinical implication of this novel model. Methods and results: The prognostic model (1-2-3-LQTS-Risk model) was derived using data from a prospective, single-centre longitudinal cohort study published in 2018 (discovery cohort) and was validated using an independent cohort of 1689 patients enrolled in the International LQTS Registry (Rochester NY, USA). The validation study revealed a C-index of 0.69 [95% confidence interval (CI): 0.61-0.77] in the validation cohort, when compared with C-index of 0.79 (95% CI: 0.70-0.88) in the discovery cohort. Adopting a 5-year risk ≥5%, as suggested by the ROC curve analysis as the most balanced threshold for implantable cardioverter-defibrillator (ICD) implantation, would result in a number needed to treat (NNT) of nine (NNT = 9; 95% CI: 6.3-13.6). Conclusion: The 1-2-3-LQTS-Risk model, the first validated 5-year risk score model for patients with LQTS, can be used to aid clinicians to identify patients at the highest risk of LAE who could benefit most from an ICD implant and avoid unnecessary implants.

Published
2022

5. Multicenter Ozone Study in oldEr Subjects (MOSES): Part 2. Effects of Personal and Ambient Concentrations of Ozone and Other Pollutants on Cardiovascular and Pulmonary Function.

Author

Rich, D, Rich, D, Frampton, M, Bromberg, P, Hazucha, M, Thurston, S, Alexis, N, Zareba, W, Koutrakis, P, Thevenet-Morrison, K, Arjomandi, Mehrdad, Ganz, Peter, Balmes, John, Rich, D, Rich, D, Frampton, M, Bromberg, P, Hazucha, M, Thurston, S, Alexis, N, Zareba, W, Koutrakis, P, Thevenet-Morrison, K, Arjomandi, Mehrdad, Ganz, Peter, and Balmes, John

Abstract

INTRODUCTION: The Multicenter Ozone Study of oldEr Subjects (MOSES) was a multi-center study evaluating whether short-term controlled exposure of older, healthy individuals to low levels of ozone (O3) induced acute changes in cardiovascular biomarkers. In MOSES Part 1 (MOSES 1), controlled O3 exposure caused concentration-related reductions in lung function with evidence of airway inflammation and injury, but without convincing evidence of effects on cardiovascular function. However, subjects prior exposures to indoor and outdoor air pollution in the few hours and days before each MOSES controlled O3 exposure may have independently affected the study biomarkers and/or modified biomarker responses to the MOSES controlled O3 exposures. METHODS: MOSES 1 was conducted at three clinical centers (University of California San Francisco, University of North Carolina, and University of Rochester Medical Center) and included healthy volunteers 55 to 70 years of age. Consented participants who successfully completed the screening and training sessions were enrolled in the study. All three clinical centers adhered to common standard operating procedures and used common tracking and data forms. Each subject was scheduled to participate in a total of 11 visits: screening visit, training visit, and three sets of exposure visits consisting of the pre-exposure day, the exposure day, and the post-exposure day. After completing the pre-exposure day, subjects spent the night in a nearby hotel. On exposure days, the subjects were exposed for 3 hours in random order to 0 ppb O3 (clean air), 70 ppb O3, and 120 ppm O3. During the exposure period the subjects alternated between 15 minutes of moderate exercise and 15 minutes of rest. A suite of cardiovascular and pulmonary endpoints was measured on the day before, the day of, and up to 22 hours after each exposure. UNLABELLED: In MOSES Part 2 (MOSES 2), we used a longitudinal panel study design, cardiopulmonary biomarker data from MOSES 1, p

Published
2020

6. Chronic kidney disease and arrhythmias: Conclusions from a Kidney Disease: Improving Global Outcomes (KDIGO) Controversies Conference

Author

Turakhia, M, Blankestijn, P, Carrero, J, Clase, C, Deo, R, Herzog, C, Kasner, S, Passman, R, Pecoits-Filho, R, Reinecke, H, Shroff, G, Zareba, W, Cheung, M, Wheeler, D, Winkelmayer, W, Wanner, C, Genovesi, S, Turakhia, Mintu P, Blankestijn, Peter J, Carrero, Juan-Jesus, Clase, Catherine M, Deo, Rajat, Herzog, Charles A, Kasner, Scott E, Passman, Rod S, Pecoits-Filho, Roberto, Reinecke, Holger, Shroff, Gautam R, Zareba, Wojciech, Cheung, Michael, Wheeler, David C, Winkelmayer, Wolfgang C, Wanner, Christoph, Turakhia, M, Blankestijn, P, Carrero, J, Clase, C, Deo, R, Herzog, C, Kasner, S, Passman, R, Pecoits-Filho, R, Reinecke, H, Shroff, G, Zareba, W, Cheung, M, Wheeler, D, Winkelmayer, W, Wanner, C, Genovesi, S, Turakhia, Mintu P, Blankestijn, Peter J, Carrero, Juan-Jesus, Clase, Catherine M, Deo, Rajat, Herzog, Charles A, Kasner, Scott E, Passman, Rod S, Pecoits-Filho, Roberto, Reinecke, Holger, Shroff, Gautam R, Zareba, Wojciech, Cheung, Michael, Wheeler, David C, Winkelmayer, Wolfgang C, and Wanner, Christoph

Published
2018

7. Multicenter Ozone Study in oldEr Subjects (MOSES): Part 1. Effects of Exposure to Low Concentrations of Ozone on Respiratory and Cardiovascular Outcomes.

Author

Frampton, M, Frampton, M, Hazucha, M, Rich, D, Hollenbeck-Pringle, D, Dagincourt, N, Alexis, N, Zareba, W, Costantini, M, Bromberg, P, Stark, P, Arjomandi, Mehrdad, Ganz, Peter, Balmes, John, Frampton, M, Frampton, M, Hazucha, M, Rich, D, Hollenbeck-Pringle, D, Dagincourt, N, Alexis, N, Zareba, W, Costantini, M, Bromberg, P, Stark, P, Arjomandi, Mehrdad, Ganz, Peter, and Balmes, John

Abstract

INTRODUCTION: Exposure to air pollution is a well-established risk factor for cardiovascular morbidity and mortality. Most of the evidence supporting an association between air pollution and adverse cardiovascular effects involves exposure to particulate matter (PM). To date, little attention has been paid to acute cardiovascular responses to ozone, in part due to the notion that ozone causes primarily local effects on lung function, which are the basis for the current ozone National Ambient Air Quality Standards (NAAQS). There is evidence from a few epidemiological studies of adverse health effects of chronic exposure to ambient ozone, including increased risk of mortality from cardiovascular disease. However, in contrast to the well-established association between ambient ozone and various nonfatal adverse respiratory effects, the observational evidence for impacts of acute (previous few days) increases in ambient ozone levels on total cardiovascular mortality and morbidity is mixed. UNLABELLED: Ozone is a prototypic oxidant gas that reacts with constituents of the respiratory tract lining fluid to generate reactive oxygen species (ROS) that can overwhelm antioxidant defenses and cause local oxidative stress. Pathways by which ozone could cause cardiovascular dysfunction include alterations in autonomic balance, systemic inflammation, and oxidative stress. These initial responses could lead ultimately to arrhythmias, endothelial dysfunction, acute arterial vasoconstriction, and procoagulant activity. Individuals with impaired antioxidant defenses, such as those with the null variant of glutathione S-transferase mu 1 (GSTM1), may be at increased risk for acute health effects. UNLABELLED: The Multicenter Ozone Study in oldEr Subjects (MOSES) was a controlled human exposure study designed to evaluate whether short-term exposure of older, healthy individuals to ambient levels of ozone induces acute cardiovascular responses. The study was designed to test the a pr

Published
2017

8. Mutation-Specific Risk in Two Genetic Forms of Type 3 Long QT Syndrome

Author

Liu, J, Moss, A, Jons, C, Benhorin, J, Schwartz, P, Spazzolini, C, Crotti, L, Ackerman, M, Mcnitt, S, Robinson, J, Qi, M, Goldenberg, I, Zareba, W, Liu JF, Moss AJ, Jons C, Benhorin J, Schwartz PJ, Spazzolini C, Crotti L, Ackerman MJ, McNitt S, Robinson JL, Qi M, Goldenberg I, Zareba W, Liu, J, Moss, A, Jons, C, Benhorin, J, Schwartz, P, Spazzolini, C, Crotti, L, Ackerman, M, Mcnitt, S, Robinson, J, Qi, M, Goldenberg, I, Zareba, W, Liu JF, Moss AJ, Jons C, Benhorin J, Schwartz PJ, Spazzolini C, Crotti L, Ackerman MJ, McNitt S, Robinson JL, Qi M, Goldenberg I, and Zareba W

Abstract

The clinical course of patients with 2 relatively common long QT syndrome type 3 mutations has not been well described. In the present study, we investigated the mutational-specific risk in patients with deletional (DeltaKPQ) and missense (D1790G) mutations involving the SCN5A gene. The study population involved 50 patients with the DeltaKPQ mutation and 35 patients with the D1790G mutation. The cumulative probability of a first cardiac event (syncope, aborted cardiac arrest, or long QT syndrome-related sudden death) was evaluated using the Kaplan-Meier method. The Cox proportional hazards survivorship model was used to determine the independent contribution of clinical and genetic factors to the first occurrence of cardiac events from birth through 40 years of age. The Andersen-Gill proportional intensity regression model was used to analyze the factors associated with recurrent syncope. Patients with a DeltaKPQ mutation had a significantly greater probability of a first cardiac event from birth through 40 years of age (34%) than those with the D1790G mutation (20%; p <0.001). Multivariate analysis demonstrated an increased risk of cardiac events among DeltaKPQ carriers compared to D1790G carriers (hazard ratio 2.42, p <0.0001) after adjustment for gender and QTc duration. Patients with DeltaKPQ mutations also had an increased risk of recurrent syncope (hazard ratio 5.20, p <0.001). In conclusion, the clinical course of patients with long QT syndrome type with DeltaKPQ mutations was shown to be more virulent than those with D1790G mutations, and this effect was independent of QTc duration. The findings highlight the importance of knowing the specific mutation in risk stratification of patients with long QT syndrome type 3

Published
2010

9. Clinical Implications for Patients With Long QT Syndrome Who Experience a Cardiac Event During Infancy

Author

Spazzolini, C, Mullally, J, Schwartz, P, Moss, A, Mcnitt, S, Ouellet, G, Fugate, T, Goldenberg, I, Jons, C, Zareba, W, Robinson, J, Ackerman, M, Benhorin, J, Crotti, L, Kaufman, E, Locati, E, Ming, Q, Napolitano, C, Priori, S, Towbin, J, Vincent, G, Spazzolini C, Mullally J, Schwartz PJ, Moss AJ, McNitt S, Ouellet G, Fugate T, Goldenberg I, Jons C, Zareba W, Robinson JL, Ackerman MJ, Benhorin J, Crotti L, Kaufman ES, Locati EH, Ming Q, Napolitano C, Priori SG, Towbin JA, Vincent GM., Spazzolini, C, Mullally, J, Schwartz, P, Moss, A, Mcnitt, S, Ouellet, G, Fugate, T, Goldenberg, I, Jons, C, Zareba, W, Robinson, J, Ackerman, M, Benhorin, J, Crotti, L, Kaufman, E, Locati, E, Ming, Q, Napolitano, C, Priori, S, Towbin, J, Vincent, G, Spazzolini C, Mullally J, Schwartz PJ, Moss AJ, McNitt S, Ouellet G, Fugate T, Goldenberg I, Jons C, Zareba W, Robinson JL, Ackerman MJ, Benhorin J, Crotti L, Kaufman ES, Locati EH, Ming Q, Napolitano C, Priori SG, Towbin JA, and Vincent GM.

Abstract

Objectives: This study was designed to evaluate the clinical and prognostic aspects of long QT syndrome (LQTS)-related cardiac events that occur in the first year of life (infancy). Background: The clinical implications for patients with long QT syndrome who experience cardiac events in infancy have not been studied previously. Methods: The study population of 3,323 patients with QT interval corrected for heart rate (QTc) ≥450 ms enrolled in the International LQTS Registry involved 20 patients with sudden cardiac death (SCD), 16 patients with aborted cardiac arrest (ACA), 34 patients with syncope, and 3,253 patients who were asymptomatic during the first year of life. Results: The risk factors for a cardiac event among 212 patients who had an electrocardiogram recorded in the first year of life included QTc ≥500 ms, heart rate ≤100 beats/min, and female sex. An ACA before age 1 year was associated with a hazard ratio of 23.4 (p < 0.01) for ACA or SCD during ages 1 to 10 years. During the 10-year follow-up after infancy, beta-blocker therapy was associated with a significant reduction in ACA/SCD only in those with a syncopal episode within 2 years before ACA/SCD but not for those who survived ACA in infancy. Conclusions: Patients with LQTS who experience ACA during the first year of life are at very high risk for subsequent ACA or death during their next 10 years of life, and beta-blockers might not be effective in preventing fatal or near-fatal cardiac events in this small but high-risk subset

Published
2009

10. Clinical Implications for Patients With Long QT Syndrome Who Experience a Cardiac Event During Infancy

Author

Spazzolini, C, Mullally, J, Schwartz, P, Moss, A, Mcnitt, S, Ouellet, G, Fugate, T, Goldenberg, I, Jons, C, Zareba, W, Robinson, J, Ackerman, M, Benhorin, J, Crotti, L, Kaufman, E, Locati, E, Ming, Q, Napolitano, C, Priori, S, Towbin, J, Vincent, G, Spazzolini C, Mullally J, Schwartz PJ, Moss AJ, McNitt S, Ouellet G, Fugate T, Goldenberg I, Jons C, Zareba W, Robinson JL, Ackerman MJ, Benhorin J, Crotti L, Kaufman ES, Locati EH, Ming Q, Napolitano C, Priori SG, Towbin JA, Vincent GM., Spazzolini, C, Mullally, J, Schwartz, P, Moss, A, Mcnitt, S, Ouellet, G, Fugate, T, Goldenberg, I, Jons, C, Zareba, W, Robinson, J, Ackerman, M, Benhorin, J, Crotti, L, Kaufman, E, Locati, E, Ming, Q, Napolitano, C, Priori, S, Towbin, J, Vincent, G, Spazzolini C, Mullally J, Schwartz PJ, Moss AJ, McNitt S, Ouellet G, Fugate T, Goldenberg I, Jons C, Zareba W, Robinson JL, Ackerman MJ, Benhorin J, Crotti L, Kaufman ES, Locati EH, Ming Q, Napolitano C, Priori SG, Towbin JA, and Vincent GM.

Abstract

Objectives: This study was designed to evaluate the clinical and prognostic aspects of long QT syndrome (LQTS)-related cardiac events that occur in the first year of life (infancy). Background: The clinical implications for patients with long QT syndrome who experience cardiac events in infancy have not been studied previously. Methods: The study population of 3,323 patients with QT interval corrected for heart rate (QTc) ≥450 ms enrolled in the International LQTS Registry involved 20 patients with sudden cardiac death (SCD), 16 patients with aborted cardiac arrest (ACA), 34 patients with syncope, and 3,253 patients who were asymptomatic during the first year of life. Results: The risk factors for a cardiac event among 212 patients who had an electrocardiogram recorded in the first year of life included QTc ≥500 ms, heart rate ≤100 beats/min, and female sex. An ACA before age 1 year was associated with a hazard ratio of 23.4 (p < 0.01) for ACA or SCD during ages 1 to 10 years. During the 10-year follow-up after infancy, beta-blocker therapy was associated with a significant reduction in ACA/SCD only in those with a syncopal episode within 2 years before ACA/SCD but not for those who survived ACA in infancy. Conclusions: Patients with LQTS who experience ACA during the first year of life are at very high risk for subsequent ACA or death during their next 10 years of life, and beta-blockers might not be effective in preventing fatal or near-fatal cardiac events in this small but high-risk subset

Published
2009

Catalog

Books, media, physical & digital resources
See catalog results