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Dive into the research topics where Charlotte Brouwer is active.

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Featured researches published by Charlotte Brouwer.


European Heart Journal | 2018

Whole human heart histology to validate electroanatomical voltage mapping in patients with non-ischaemic cardiomyopathy and ventricular tachycardia

Claire A Glashan; A.F.A. Androulakis; Qian Tao; Ross N Glashan; Lambertus J. Wisse; Micaela Ebert; Marco C de Ruiter; Berend J van Meer; Charlotte Brouwer; Olaf M. Dekkers; Daniël A. Pijnappels; Jacques M.T. de Bakker; Marta de Riva; Sebastiaan R.D. Piers; Katja Zeppenfeld

Aims Electroanatomical voltage mapping (EAVM) is an important diagnostic tool for fibrosis identification and risk stratification in non-ischaemic cardiomyopathy (NICM); currently, distinct cut-offs are applied. We aimed to evaluate the performance of EAVM to detect fibrosis by integration with whole heart histology and to identify the fibrosis pattern in NICM patients with ventricular tachycardias (VTs). Methods and results Eight patients with NICM and VT underwent EAVM prior to death or heart transplantation. EAVM data was projected onto slices of the entire heart. Pattern, architecture, and amount of fibrosis were assessed in transmural biopsies corresponding to EAVM sites. Fibrosis pattern in NICM biopsies (n = 507) was highly variable and not limited to mid-wall/sub-epicardium. Fibrosis architecture was rarely compact, but typically patchy and/or diffuse. In NICM, biopsies without abnormal fibrosis unipolar voltage (UV) and bipolar voltage (BV) showed a linear association with wall thickness (WT). The amount of viable myocardium showed a linear association with both UV and BV. Accordingly, any cut-off to delineate fibrosis performed poorly. An equation was generated calculating the amount of fibrosis at any location, given WT and UV or BV. Conclusion Considering the linear relationships between WT, amount of fibrosis and both UV and BV, the search for any distinct voltage cut-off to identify fibrosis in NICM is futile. The amount of fibrosis can be calculated, if WT and voltages are known. Fibrosis pattern and architecture are different from ischaemic cardiomyopathy and findings on ischaemic substrates may not be applicable to NICM.


Arrhythmia and Electrophysiology Review | 2016

Anatomical Substrates and Ablation of Reentrant Atrial and Ventricular Tachycardias in Repaired Congenital Heart Disease.

Charlotte Brouwer; Mark G. Hazekamp; Katja Zeppenfeld

Advances in surgical repair techniques for various types of congenital heart disease have improved survival into adulthood over the past decades, thus exposing these patients to a high risk of atrial and ventricular arrhythmias later in life. These arrhythmias arise from complex arrhythmogenic substrates. Substrate formation may depend on both pathological myocardial remodelling and variable anatomical boundaries, determined by the type and timing of prior corrective surgery. Accordingly, arrhythmogenic substrates after repair have changed as a result of evolving surgical techniques. Radiofrequency catheter ablation offers an important therapeutic option but remains challenging due to the variable anatomy, surgically created obstacles and the complex arrhythmogenic substrates. Recent technical developments including electroanatomical mapping and image integration for delineating the anatomy facilitate complex catheter ablation procedures. The purpose of this review is to provide an update on the changing anatomical arrhythmogenic substrates and their potential impact on catheter ablation in patients with repaired congenital heart disease and tachyarrhythmias.


JACC: Clinical Electrophysiology | 2018

Slow Conducting Electroanatomic Isthmuses: An Important Link Between QRS Duration and VT in Tetralogy of Fallot

Gijsbert F.L. Kapel; Charlotte Brouwer; Zakaria Jalal; Frederic Sacher; Jeroen Venlet; Martin J. Schalij; Jean-Benoit Thambo; Monique R.M. Jongbloed; Nico A. Blom; Marta de Riva; Katja Zeppenfeld


JACC: Clinical Electrophysiology | 2018

Noninvasive Identification of Ventricular Tachycardia–Related Anatomical Isthmuses in Repaired Tetralogy of Fallot: What Is the Role of the 12-Lead Ventricular Tachycardia Electrocardiogram

Charlotte Brouwer; Gijsbert F.L. Kapel; Monique R.M. Jongbloed; Martin J. Schalij; Marta De Riva Silva; Katja Zeppenfeld


JACC: Clinical Electrophysiology | 2018

Slow Conducting Electroanatomic Isthmuses: An Important Link Between QRS Duration and Ventricular Tachycardia in Tetralogy of Fallot

Gijsbert F.L. Kapel; Charlotte Brouwer; Zakaria Jalal; Frederic Sacher; Jeroen Venlet; Martin J. Schalij; Jean-Benoit Thambo; Monique R.M. Jongbloed; Nico A. Blom; Marta de Riva; Katja Zeppenfeld


European Heart Journal | 2017

P809Targeting the hidden substrate unmasked by right ventricular extrastimulation improves ventricular tachycardia ablation outcome after myocardial infarction

M. De Riva Silva; Y. Naruse; Masaya Watanabe; A P Wijnmaalen; Jeroen Venlet; A.F.A. Androulakis; Charlotte Brouwer; M. J. Schalij; Katja Zeppenfeld


European Heart Journal | 2017

P211612-lead ECG algorithm to differentiate between ARVC and cardiac sarcoidosis

Jeroen Venlet; Saurabh Kumar; Charlotte Brouwer; A.F.A. Androulakis; Srd Piers; Y. Naruse; M. De Riva; W.G. Stevenson; Katja Zeppenfeld


Europace | 2017

1218Targeting the hidden substrate unmasked by right ventricular extrastimulation improves ventricular tachycardia ablation outcome after myocardial infarction

M. De Riva; Y. Naruse; M. Watanabe; A P Wijnmaalen; Jeroen Venlet; Af. Androulakis; Charlotte Brouwer; M. J. Schalij; Katja Zeppenfeld


Europace | 2017

753The role of the 12-lead VT ECG in patients with repaired tetralogy of Fallot: non-invasive identification of VT related anatomic isthmuses

Charlotte Brouwer; Gfl Kapel; M. J. Schalij; M. De Riva Silva; Katja Zeppenfeld


Europace | 2017

P267The transmural activation interval: a new mapping tool to identify protected VT substrates in ARVC

Jeroen Venlet; Afa Androulakis; Charlotte Brouwer; Srd Piers; M. De Riva; Y. Naruse; Katja Zeppenfeld

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Katja Zeppenfeld

Leiden University Medical Center

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Jeroen Venlet

Leiden University Medical Center

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Martin J. Schalij

Leiden University Medical Center

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Y. Naruse

Leiden University Medical Center

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A.F.A. Androulakis

Leiden University Medical Center

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M. De Riva

Leiden University Medical Center

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M. J. Schalij

Leiden University Medical Center

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