Criteria for arrhythmogenicity in genetically-modified Langendorff-perfused murine hearts modelling the congenital long QT syndrome type 3 and the Brugada syndrome

Abstract The characteristic shape of the T-wave in congenital long -QT syndrome type 3 (LQTS3) is considered a late-onset T-wave. We analyzed the difference in the shapes of T-waves between LQTS3 cases and normal subjects using generalized Procrustes analysis (GPA). The J and Q points of V5 in the ECGs of LQTS3 cases are shifted to the upper left compared to those of normal subjects. SdFmax is the point on the ECG where the second derivative is first maximized. The curvature of the T-wave takes the first maximum value at SdFmax where the T-wave has the smallest radius of curvature.The SdFmax in LQTS3 cases is shifted to the lower right compared to normal subjects. The interval from J to SdFmax of LQTS3 cases is expanded compared with that of normal subjects. As a result of principal component analysis (PCA) of the Procrustes mean shape of the T-wave landmarks, the second principal component (PC2) shows the shift in SdFmax to the lower right. These results can quantitatively explain why the T-wave of LQTS3 cases looks like a late-onset T-wave. Fitted to a multivariate logistic regression model, LQTS3 cases and normal subjects can be distinguished by the second independent component (IC2).

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E1784K, the most common Brugada syndrome and long-QT syndrome type 3 mutant, disrupts sodium channel inactivation through two separate mechanisms

The Journal of General Physiology ◽

10.1085/jgp.202012595 ◽

2020 ◽

Vol 152 (9) ◽

Author(s):

Colin H. Peters ◽

Abeline R. Watkins ◽

Olivia L. Poirier ◽

Peter C. Ruben

Keyword(s):

Long Qt Syndrome ◽

Brugada Syndrome ◽

Double Mutant ◽

Voltage Dependence ◽

Syndrome Type ◽

Fast Inactivation ◽

Long Qt ◽

Qt Syndrome ◽

Type 3 ◽

Dependent Interaction

Inheritable and de novo variants in the cardiac voltage-gated sodium channel, Nav1.5, are responsible for both long-QT syndrome type 3 (LQT3) and Brugada syndrome type 1 (BrS1). Interestingly, a subset of Nav1.5 variants can cause both LQT3 and BrS1. Many of these variants are found in channel structures that form the channel fast inactivation machinery, altering the rate, voltage dependence, and completeness of the fast inactivation process. We used a series of mutants at position 1784 to show that the most common inheritable Nav1.5 variant, E1784K, alters fast inactivation through two separable mechanisms: (1) a charge-dependent interaction that increases the noninactivating current characteristic of E1784K; and (2) a hyperpolarized voltage dependence and accelerated rate of fast inactivation that decreases the peak sodium current. Using a homology model built on the NavPaS structure, we find that the charge-dependent interaction is between E1784 and K1493 in the DIII–DIV linker of the channel, five residues downstream of the putative inactivation gate. This interaction can be disrupted by a positive charge at position 1784 and rescued with the K1493E/E1784K double mutant that abolishes the noninactivating current. However, the double mutant does not restore either the voltage dependence or rates of fast inactivation. Conversely, a mutant at the bottom of DIVS4, K1641D, causes a hyperpolarizing shift in the voltage dependence of fast inactivation and accelerates the rate of fast inactivation without causing an increase in noninactivating current. These findings provide novel mechanistic insights into how the most common inheritable arrhythmogenic mixed syndrome variant, E1784K, simultaneously decreases transient sodium currents and increases noninactivating currents, leading to both BrS1 and LQT3.

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