Cardiac sodium channel, its mutations and their spectrum of arrhythmia phenotypes

Pérez‐Riera, Andrés Ricardo; Raimundo, Rodrigo Daminello; Watanabe, Rodrigo Akira; Figueiredo, José Luiz; Abreu, Luíz Carlos de

doi:10.7322/jhgd.122759

Cited by 7 publications

(8 citation statements)

References 77 publications

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“…Among some complications, continuous positive airway pressure is related to decrease cerebral perfusion due to increased average pressure and intracranial pressure. Others that can be cited are: trauma airway, nosocomial infections and bronchopulmonary dysplasia [23][24][25][26][27] .…”

Section: Discussionmentioning

confidence: 99%

Report a case of Ebstein's anomaly wich early diagnosis avoid iatrogenic acts

Pinasco

Rocha²,

Rocha³

et al. 2016

Int Arch Med

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Introduction: Ebstein's anomaly is a rare malformation that corresponds to less than 1% of all congenital heart anomalies. It consists in the caudal displacement of the tricuspid valve with retrograde flow to the right atrium due to valvular insufficiency and it is characterized by a variable spectrum of severity, being higher in the neonatal period. Objective: to report an Ebstein's anomaly case which early diagnosis avoided iatrogenic ducts. Case report: a newborn at term, appropriate weight for gestational age, female, was born of natural childbirth, with Apgar score 8/9 from pregnancy without complications. At birth, not in need of resuscitation in the delivery room, but presented heart murmur and fall of saturation, being supported and then forwarded to the NICU. Not present hemodynamic instability. The chest x-ray showed increased cardiac area with increased right atrium. The Transthoracic Echocardiogram showed mild right ventricular dilatation and important of the right atrium, tricuspid valve dysplasia with low implantation of posterior leaflet of tricuspid insufficiency presence important to Doppler, being diagnosed with Ebstein's anomaly. Evolved with progressive improvement of the frame and saturation above 95% on room air to pulse oximetry. Patient follows in outpatient follow-up in use of inotropic and diuretic, remaining asymptomatic. Conclusion: the recognition of the gravity of the picture is relevant to the proper management in order to prevent iatrogenic ducts, which can lead to complications or permanent sequelae.

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Section: Discussionmentioning

confidence: 99%

Report a case of Ebstein's anomaly wich early diagnosis avoid iatrogenic acts

Pinasco

Rocha²,

Rocha³

et al. 2016

Int Arch Med

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“…Phenotypes: Mutations in SCN5A lead to a broad spectrum of phenotypes, however the SCN5A gene is not commonly involved in the pathogenesis of BrS and associated disorders. Studies have revealed significant overlap between aberrant rhythm phenotypes, and single mutations have been identified that evoke multiple rhythm disorders with common gating lesions 19 . Figure 1 shows the numerous phenotypes with SCN5A mutations.…”

Section: Paralogs or Paralogous Genesmentioning

confidence: 99%

Brugada syndrome: current concepts and genetic background

Pérez‐Riera

Mendes

Silva

et al. 2021

jhgd

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Brugada syndrome (BrS) is a hereditary clinical-electrocardiographic arrhythmic entity with low worldwide prevalence. The syndrome is caused by changes in the structure and function of certain cardiac ion channels and reduced expression of Connexin 43 (Cx43) in the Right Ventricle (RV), predominantly in the Right Ventricular Outflow Tract (VSVD), causing electromechanical abnormalities. The diagnosis is based on the presence of spontaneous or medicated ST elevation, characterized by boost of the J point and the ST segment ≥2 mm, of superior convexity "hollow type" (subtype 1A) or descending rectilinear model (subtype 1B). BrS is associated with an increased risk of syncope, palpitations, chest pain, convulsions, difficulty in breathing (nocturnal agonal breathing) and/or Sudden Cardiac Death (SCD) secondary to PVT/VF, unexplained cardiac arrest or documented PVT/VF or Paroxysmal atrial fibrillation (AF) in the absence of apparent macroscopic or structural heart disease, electrolyte disturbance, use of certain medications or coronary heart disease and fever. In less than three decades since the discovery of Brugada syndrome, the concept of Mendelian heredity has come undone. The enormous variants and mutations found mean that we are still far from being able to concretely clarify a genotype-phenotype relationship. There is no doubt that the entity is oligogenetic, associated with environmental factors, and that there are variants of uncertain significance, especially the rare variants of the SCN5A mutation, with European or Japanese ancestors, as well as a spontaneous type 1 or induced pattern, thanks to gnomAD (coalition) researchers who seek to aggregate and harmonize exome and genome sequencing data from a variety of large scale sequencing projects and make summary data available to the scientific community at large). Thus, we believe that this in depth analytical study of the countless mutations attributed to BrS may constitute a real cornerstone that will help to better understand this intriguing syndrome.

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“…Mutations in several genes, including the SCN5A, SCN1B and TRPM4 genes, can cause PCCD. Mutations in the SCN5A gene are potential etiologic factors for a number of overlapping syndromes [21]. Several other genes may be the cause when PCCD occurs with congenital heart disease.…”

Section: Epidemiologymentioning

confidence: 99%

Left posterior fascicular block, state-of-the-art review: A 2018 update

Pérez‐Riera

Barbosa‐Barros

Daminello‐Raimundo

et al. 2018

Indian Pacing and Electrophysiology Journal

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We conducted a review of the literature regarding epidemiology, clinical, electrocardiographic and vectorcardiographic aspects, classification, and differential diagnosis of left posterior fascicular block.Isolated left posterior fascicular block (LPFB) is an extremely rare finding both in the general population and in specific patient groups. In isolated LPFB 20% of the vectorcardiographic (VCG) QRS loop is located in the right inferior quadrant and when associated with right bundle branch block (RBBB) ≥40%.The diagnosis of LPFB should always consider the clinical aspects, because a definite diagnosis cannot be made in the presence of right ventricular hypertrophy (RVH) (chronic obstructive pulmonary disease (COPD)/emphysema), extensive lateral myocardial infarction (MI) or extremely vertical heart.Intermittent LPFBs are never complete blocks (transient or second degree LPFB) and even in the permanent ones, one cannot be sure that they are complete. When LPFB is associated with RBBB and acute inferior MI, PR interval prolongation is very frequent.

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Cardiac sodium channel, its mutations and their spectrum of arrhythmia phenotypes

Cited by 7 publications

References 77 publications

Report a case of Ebstein's anomaly wich early diagnosis avoid iatrogenic acts

Report a case of Ebstein's anomaly wich early diagnosis avoid iatrogenic acts

Brugada syndrome: current concepts and genetic background

Left posterior fascicular block, state-of-the-art review: A 2018 update

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