Screening of NKX2.5 gene in Moroccan Tetralogy of Fallot (TOF) patients: worldwide mutation rate comparisons show a significant association between R25C variant and TOF phenotype

Bouchikhi, Ihssane El; Belhassan, Khadija; Moufid, Fatima Zohra; Bouguenouch, Laila; Samri, Imane; Houssaini, Mohammed Iraqui; Ouldim, Karim; Atmani, S.

doi:10.1186/s43042-021-00136-1

Cited by 3 publications

(3 citation statements)

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“…Bioinformatic predictions indicate that the E21E variant might impair NKX2.5 transcript splicing by removing a whole exon from the transcript, resulting in translation of a shortened protein that is most likely inactive. Further in vitro functional tests are needed to validate this finding ( EL Bouchikhi et al, 2021 ).…”

Section: Introductionmentioning

confidence: 98%

“…Several studies have also reported that variants in NKX2.5 cause a wide range of CHDs, including ASD, VSD, TOF, HLH, CoA, TGA, Double Outlet Right Ventricle (DORV), IAA, and cardiac outflow tract (OFT) anomalies; reviewed in ( Chung and Rajakumar, 2016 ). Recently, new NKX2.5 variants were discovered in a Moroccan cohort with non-syndromic TOF; a missense variant R25C and a synonymous variant E21E ( EL Bouchikhi et al, 2021 ). The R25C variant is expected to impair NKX2.5 dimerisation and impede activation of downstream target genes ( Kasahara et al, 2000 ; Dentice et al, 2006 ).…”

Section: Introductionmentioning

confidence: 99%

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Genetic insights into non-syndromic Tetralogy of Fallot

Althali

Hentges

2022

Front. Physiol.

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Congenital heart defects (CHD) include structural abnormalities of the heart or/and great vessels that are present at birth. CHD affects around 1% of all newborns worldwide. Tetralogy of Fallot (TOF) is the most prevalent cyanotic congenital cardiac abnormality, affecting three out of every 10,000 live infants with a prevalence rate of 5–10% of all congenital cardiac defects. The four hallmark characteristics of TOF are: right ventricular hypertrophy, pulmonary stenosis, ventricular septal defect, and overriding aorta. Approximately 20% of cases of TOF are associated with a known disease or chromosomal abnormality, with the remaining 80% of TOF cases being non-syndromic, with no known aetiology. Relatively few TOF patients have been studied, and little is known about critical causative genes for non-syndromic TOF. However, rare genetic variants have been identified as significant risk factors for CHD, and are likely to cause some cases of TOF. Therefore, this review aims to provide an update on well-characterized genes and the most recent variants identified for non-syndromic TOF.

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Section: Introductionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

Genetic insights into non-syndromic Tetralogy of Fallot

Althali

Hentges

2022

Front. Physiol.

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“…The human NKX2-5 gene maps to chromosome 5q34 and consists of two exons that encode a 324-amino acid protein [ 16 ]. Previous studies evaluated the exonic regions of the NKX2-5 gene; however, recent findings instead investigate the mutations and associated CHDs in the intronic and promoter regions of the NKX2-5 gene [ 17 ]. Functional analysis has elucidated the mechanism of action in various mutations of the NKX2-5 gene and future studies are required in order to understand the involvement of NKX2-5 in complex cardiac abnormalities [ 18 ].…”

Section: Introductionmentioning

confidence: 99%

Mutational Assessment in NKX2-5 and ACTC1 Genes in Patients with Congenital Cardiac Septal Defect (CCSD) from Ethnic Kashmiri Population

Nazeer

Bhat

Rah

et al. 2022

IJERPH

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(1) Background globe. The etiology of CHDs is complex and involves both genetic and non-genetic factors. Although, significant progress has been made in deciphering the genetic components involved in CHDs, recent reports have revealed that mutations in Nk2 homeobox5 (NKX2-5) and actin alpha cardiac muscle1 (ACTC1) genes play a key role in CHDs such as atrial and ventricular septum defects. Therefore, the present study evaluates the role of key hotspot mutations in NKX2-5 and ACTC1 genes of congenital cardiac septal defect (CCSD) in ethnic Kashmiri population. (2) Methods: A total of 112 confirmed CHD patients were included in the current study, of which 30 patients were evaluated for mutational analysis for hotspot mutations of NKX2-5 and ACTC1 genes. The total genomic DNA was extracted from the samples (cardiac tissue/blood) and were subjected to amplification for NKX2-5 (exon 1 and 2), and ACTC1 (exon 2) genes by using PCR specific primers to analyze the hotspot mutations in respective exons. The amplified products obtained were sent to Macrogen Korea for sequencing by Sanger’s method. (3) Results: Our results confirmed that not a single mutation was found in either hotspot exon 1 and 2 of NKX2-5 and exon 2 of ACTC1 in the patients included in the current study. Interestingly, a novel synonymous nucleotide variation leading to G > C transversion (GCG > GCC) was found in exon 2 of NKX2-5 gene of CCSD patient. (4) Conclusions: The current findings demonstrated the role of NKX2-5 and ACTC1 in cardiac development. The study will provide an insight in understanding the genetic etiology and highlights the role of newly identified mutations in patients with CDS’s in ethnic Kashmiri population. In silico findings revealed amino acid changes, splice site variation and the creation of new site. Furthermore, the study warrants complete screening of genes involved in CCSDs.

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Síndrome genital, ocular, cardiaco y de agenesia del cuerpo calloso. Reporte de caso

Montero-Vázquez,

Méndez-Contreras

2024

Case reports

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Resumen Introducción. El estudio etiopatogénico de las malformaciones tanto mayores como menores, así como su identificación, son requisito indispensable para el pediatra ya que es el médico de primer contacto en la atención natal y postnatal de gran parte de los recién nacidos. El síndrome genital, ocular, cardiaco y de agenesia del cuerpo calloso (ACOGS por sus siglas en inglés) es una entidad compleja y de muy baja incidencia, causada por mutaciones del gen CDH2 en el cromosoma 18q12. Las anomalías de esta patología se pueden expresar en varios sistemas: a nivel ocular con complicaciones como la anoftalmia y la microftalmia, a nivel cardiaco puede presentar problemas en la comunicación interventricular y a nivel cerebral se pueden presentar patologías como la ventriculomegalia, la agenesia del cuerpo calloso, entre otras. Presentación del caso. Recién nacido con antecedente prenatal de macrocefalia diagnosticada por ultrasonido pélvico, quien es remitido al Servicio de Pediatría de una institución de segundo nivel de complejidad en la ciudad de Acapulco (México) por dificultad respiratoria. A su ingreso se identificó macrocefalia, soplo cardiaco y criptorquidia, además de dificultad respiratoria manejada con fase ll de ventilación. Se realizó ultrasonido transfontanelar y tomografía axial de cráneo, cuyos hallazgos fueron coincidentes con agenesia del cuerpo calloso, hidrocefalia e hipoplasia cerebelar. En el ecocardiograma realizado se identificó una Tetralogía de Fallot. Dichos resultados, sumados al conjunto de anomalías encontradas, fueron consistentes con ACOGS. Conclusión. El ACOGS es un conjunto heterogéneo y poco común de malformaciones mayores recientemente descrito en la literatura, que se debe sospechar en aquellos pacientes con alteraciones cardiacas, genitales y del tubo neural.

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Screening of NKX2.5 gene in Moroccan Tetralogy of Fallot (TOF) patients: worldwide mutation rate comparisons show a significant association between R25C variant and TOF phenotype

Cited by 3 publications

References 37 publications

Genetic insights into non-syndromic Tetralogy of Fallot

Genetic insights into non-syndromic Tetralogy of Fallot

Mutational Assessment in NKX2-5 and ACTC1 Genes in Patients with Congenital Cardiac Septal Defect (CCSD) from Ethnic Kashmiri Population

Síndrome genital, ocular, cardiaco y de agenesia del cuerpo calloso. Reporte de caso

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