Tbx5 variants disrupt Nav1.5 function differently in patients diagnosed with Brugada or Long QT Syndrome

Nieto-Marín, Paloma; Tinaquero, David; Utrilla, Raquel G.; Cebrián, Jorge; González-Guerra, Andrés; Crespo-García, Teresa; Cámara-Checa, Anabel; Rubio-Alarcón, Marcos; Dago, María; Alfayate, Silvia; Filgueiras, David; Peinado, Rafaél; López‐Sendón, José; Jalife, José; Tamargo, Juan; Bernal, Juan A.; Caballero, Ricardo; Delpón, Eva

doi:10.1093/cvr/cvab045

Cited by 17 publications

(36 citation statements)

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“…Time dependence of I Na activation was quantified by fitting a monoexponential function to the activation phase of the maximum I Na trace of each experiment [ 13 ]. The activation time constant (τ act ) averaged 0.19 ± 0.01 ( n = 43) and 0.22 ± 0.03 ms ( n = 19) in cells transfected/not transfected with Zfhx3, respectively, indicating that the TF did not modify the activation kinetics ( p > 0.05) ( Table 1 ).…”

Section: Resultsmentioning

confidence: 99%

“…Consistently with these findings, Zfhx3 silencing did not modify it either ( Figure 3 B and Table 1 ). The persistent component of I Na or late I Na (I Na,L ) was quantified as the percentage of the peak I Na [ 13 ] and plotted in Figure 3 C,D. These figures demonstrate that I Na,L magnitude was not different in HL-1 cells transfected/not transfected with Zfhx3 ( Figure 3 C) ( p > 0.05, n ≥ 14) or in cells in which Zfhx3 expression was silenced/not silenced ( Figure 3 D) ( p > 0.05, n ≥ 7).…”

Section: Resultsmentioning

confidence: 99%

“…Additionally, both Zfhx3 and Pitx2c regulate the expression of other cardio-specific TF such as Tbx5 and Nkx2.5 [ 4 ]. Thus, we decided to test the effect of Zfhx3 on the expression of these TFs, which also regulated the magnitude of cardiac I Na [ 13 ]. Figure 5 A,B shows that transfection with Zfhx3 significantly decreased the protein expression of Tbx5 as demonstrated by WB experiments.…”

Section: Resultsmentioning

confidence: 99%

“…Thus, it plays a critical role in excitability and intracardiac conduction velocity. Recently, it was functionally demonstrated that Tbx5, a TF belonging to the T-box family, promotes the expression of the SCN5A gene, and thus increased I Na in human cardiomyocytes derived from induced pluripotent stem cells (hiPSC-CM) [ 13 ]. Furthermore, the Brugada Syndrome (BrS)-associated variant p.F206L Tbx5, lacks this pro-transcriptional effect, thus markedly reducing I Na [ 13 ].…”

Section: Introductionmentioning

confidence: 99%

“…Recently, it was functionally demonstrated that Tbx5, a TF belonging to the T-box family, promotes the expression of the SCN5A gene, and thus increased I Na in human cardiomyocytes derived from induced pluripotent stem cells (hiPSC-CM) [ 13 ]. Furthermore, the Brugada Syndrome (BrS)-associated variant p.F206L Tbx5, lacks this pro-transcriptional effect, thus markedly reducing I Na [ 13 ]. On the other hand, Nav1.5 expression decreases in atrial chamber-specific Pitx2 conditional mutants, suggesting that Pitx2c positively modulates Scn5a expression [ 14 ].…”

Section: Introductionmentioning

confidence: 99%

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Zfhx3 Transcription Factor Represses the Expression of SCN5A Gene and Decreases Sodium Current Density (INa)

Rubio-Alarcón

Cámara-Checa

Dago

et al. 2021

IJMS

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The ZFHX3 and SCN5A genes encode the zinc finger homeobox 3 (Zfhx3) transcription factor (TF) and the human cardiac Na+ channel (Nav1.5), respectively. The effects of Zfhx3 on the expression of the Nav1.5 channel, and in cardiac excitability, are currently unknown. Additionally, we identified three Zfhx3 variants in probands diagnosed with familial atrial fibrillation (p.M1260T) and Brugada Syndrome (p.V949I and p.Q2564R). Here, we analyzed the effects of native (WT) and mutated Zfhx3 on Na+ current (INa) recorded in HL-1 cardiomyocytes. ZFHX3 mRNA can be detected in human atrial and ventricular samples. In HL-1 cardiomyocytes, transfection of Zfhx3 strongly reduced peak INa density, while the silencing of endogenous expression augmented it (from −65.9 ± 8.9 to −104.6 ± 10.8 pA/pF; n ≥ 8, p < 0.05). Zfhx3 significantly reduced the transcriptional activity of human SCN5A, PITX2, TBX5, and NKX25 minimal promoters. Consequently, the mRNA and/or protein expression levels of Nav1.5 and Tbx5 were diminished (n ≥ 6, p < 0.05). Zfhx3 also increased the expression of Nedd4-2 ubiquitin-protein ligase, enhancing Nav1.5 proteasomal degradation. p.V949I, p.M1260T, and p.Q2564R Zfhx3 produced similar effects on INa density and time- and voltage-dependent properties in WT. WT Zfhx3 inhibits INa as a result of a direct repressor effect on the SCN5A promoter, the modulation of Tbx5 increasing on the INa, and the increased expression of Nedd4-2. We propose that this TF participates in the control of cardiac excitability in human adult cardiac tissue.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Zfhx3 Transcription Factor Represses the Expression of SCN5A Gene and Decreases Sodium Current Density (INa)

Rubio-Alarcón

Cámara-Checa

Dago

et al. 2021

IJMS

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Translational potential of hiPSCs in predictive modeling of heart development and disease

Mansfield

Zhao

Basu

2022

Birth Defects Research

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Congenital heart disease (CHD) represents a major class of birth defects worldwide and is associated with cardiac malformations that often require surgical intervention immediately after birth. Despite the intense efforts from multicentric genome/exome sequencing studies that have identified several genetic variants, the etiology of CHD remains diverse and often unknown. Genetically modified animal models with candidate gene deficiencies continue to provide novel molecular insights that are responsible for fetal cardiac development. However, the past decade has seen remarkable advances in the field of human induced pluripotent stem cell (hiPSC)‐based disease modeling approaches to better understand the development of CHD and discover novel preventative therapies. The iPSCs are derived from reprogramming of differentiated somatic cells to an embryonic‐like pluripotent state via overexpression of key transcription factors. In this review, we describe how differentiation of hiPSCs to specialized cardiac cellular identities facilitates our understanding of the development and pathogenesis of CHD subtypes. We summarize the molecular and functional characterization of hiPSC‐derived differentiated cells in support of normal cardiogenesis, those that go awry in CHD and other heart diseases. We illustrate how stem cell‐based disease modeling enables scientists to dissect the molecular mechanisms of cell–cell interactions underlying CHD. We highlight the current state of hiPSC‐based studies that are in the verge of translating into clinical trials. We also address limitations including hiPSC‐model reproducibility and scalability and differentiation methods leading to cellular heterogeneity. Last, we provide future perspective on exploiting the potential of hiPSC technology as a predictive model for patient‐specific CHD, screening pharmaceuticals, and provide a source for cell‐based personalized medicine. In combination with existing clinical and animal model studies, data obtained from hiPSCs will yield further understanding of oligogenic, gene–environment interaction, pathophysiology, and management for CHD and other genetic cardiac disorders.

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Cancer Chemotherapy-Induced Sinus Bradycardia: A Narrative Review of a Forgotten Adverse Effect of Cardiotoxicity

2022

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Tbx5 variants disrupt Nav1.5 function differently in patients diagnosed with Brugada or Long QT Syndrome

Cited by 17 publications

References 50 publications

Zfhx3 Transcription Factor Represses the Expression of SCN5A Gene and Decreases Sodium Current Density (INa)

Zfhx3 Transcription Factor Represses the Expression of SCN5A Gene and Decreases Sodium Current Density (INa)

Translational potential of hiPSCs in predictive modeling of heart development and disease

Cancer Chemotherapy-Induced Sinus Bradycardia: A Narrative Review of a Forgotten Adverse Effect of Cardiotoxicity

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