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Genetic Analysis Algorithm for the Study of Patients with Multiple Congenital Anomalies and Isolated Congenital Heart Disease.

Delea, Marisol; Massara, Lucia S; Espeche, Lucia D; Bidondo, María Paz; Barbero, Pablo; Oliveri, Jaen; Brun, Paloma; Fabro, Mónica; Galain, Micaela; Fernández, Cecilia S; Taboas, Melisa; Bruque, Carlos D; Kolomenski, Jorge E; Izquierdo, Agustín; Berenstein, Ariel; Cosentino, Viviana; Martinoli, Celeste; Vilas, Mariana; Rittler, Mónica; Mendez, Rodrigo; Furforo, Lilian; Liascovich, Rosa; Groisman, Boris; Rozental, Sandra; Dain, Liliana.

Genes (Basel) ; 13(7)2022 06 29.

Artigo em Inglês | MEDLINE | ID: mdl-35885957

RESUMO

Congenital anomalies (CA) affect 3-5% of newborns, representing the second-leading cause of infant mortality in Argentina. Multiple congenital anomalies (MCA) have a prevalence of 2.26/1000 births in newborns, while congenital heart diseases (CHD) are the most frequent CA with a prevalence of 4.06/1000 births. The aim of this study was to identify the genetic causes in Argentinian patients with MCA and isolated CHD. We recruited 366 patients (172 with MCA and 194 with isolated CHD) born between June 2015 and August 2019 at public hospitals. DNA from peripheral blood was obtained from all patients, while karyotyping was performed in patients with MCA. Samples from patients presenting conotruncal CHD or DiGeorge phenotype (n = 137) were studied using MLPA. Ninety-three samples were studied by array-CGH and 18 by targeted or exome next-generation sequencing (NGS). A total of 240 patients were successfully studied using at least one technique. Cytogenetic abnormalities were observed in 13 patients, while 18 had clinically relevant imbalances detected by array-CGH. After MLPA, 26 patients presented 22q11 deletions or duplications and one presented a TBX1 gene deletion. Following NGS analysis, 12 patients presented pathogenic or likely pathogenic genetic variants, five of them, found in KAT6B, SHH, MYH11, MYH7 and EP300 genes, are novel. Using an algorithm that combines molecular techniques with clinical and genetic assessment, we determined the genetic contribution in 27.5% of the analyzed patients.

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Anormalidades Múltiplas , Cardiopatias Congênitas , Anormalidades Múltiplas/genética , Algoritmos , Testes Genéticos , Cardiopatias Congênitas/genética , Histona Acetiltransferases , Humanos , Cariotipagem

Análisis de anomalías cromosómicas, desbalances genómicos y variantes de secuencia como causa de cardiopatías congénitas / Analysis of chromosomal abnormalities, genomic imbalances, and sequence variants as cause of congenital heart defects

Delea, Marisol; Massara, Soledad; Bruque, Carlos David; Espeche, Lucía Daniela; Taboas, Melisa Ivana; Barbero, Pablo; Bidondo, María Paz; Liascovich, Rosa; Groisman, Boris; Cosentino, Viviana; Martinoli, Celeste; Furforo, Lilian; Ritler, Mónica; Kolomenski, Emilio; Oliveri, Jaen; Brun, Paloma; Rozental, Sandra; Dain, Liliana Beatriz.

Rev. argent. salud publica ; 13: 1-8, 5/02/2021.

Artigo em Espanhol | LILACS, ARGMSAL, BINACIS | ID: biblio-1147271

RESUMO

INTRODUCCIÓN: Las cardiopatías congénitas (CC) son causadas por el desarrollo anómalo del corazón durante el período embriofetal. Abarcan un amplio espectro de anomalías estructurales de las cavidades cardíacas o de los grandes vasos, con una prevalencia mundial de 6 a 9 por 1000 nacimientos. En Argentina constituyen un tercio de las anomalías congénitas (AC) al nacimiento. Si bien su etiología es heterogénea, se ha observado recurrencia familiar acorde con la influencia de factores genéticos. El objetivo del estudio fue evaluar la presencia de anomalías cromosómicas, desbalances genómicos o variantes de secuencias en una muestra de niños afectados con CC en Argentina. MÉTODOS: Se incluyó a 289 pacientes con CC de hasta 16 años. Se realizó un cariotipo para pacientes con otras AC y análisis por amplificación múltiple de sondas dependiente de ligación (MLPA) de regiones genómicas asociadas a CC para aquellos con CC conotroncales. En muestras seleccionadas, se analizaron desbalances genómicos por microarreglos de ADN (array-CGH) o variantes de secuencia en el gen NKX2-5. RESULTADOS: Hubo 9 pacientes que presentaron anomalías cromosómicas, 21 desbalances por MLPA y 8 por array-CGH. No se hallaron variantes patogénicas en NKX2-5 en los casos estudiados. DISCUSIÓN: Se halló la causa de la afección en el 13% de los casos analizados. El estudio de pacientes con CC aisladas o asociadas a otras AC no había sido abordado previamente en Argentina mediante este algoritmo

Assuntos

Aberrações Cromossômicas , Genética Médica , Cardiopatias

Genetic Imbalances in Argentinean Patients with Congenital Conotruncal Heart Defects.

Delea, Marisol; Espeche, Lucía D; Bruque, Carlos D; Bidondo, María Paz; Massara, Lucía S; Oliveri, Jaen; Brun, Paloma; Cosentino, Viviana R; Martinoli, Celeste; Tolaba, Norma; Picon, Claudina; Ponce Zaldua, María Eugenia; Ávila, Silvia; Gutnisky, Viviana; Perez, Myriam; Furforo, Lilian; Buzzalino, Noemí D; Liascovich, Rosa; Groisman, Boris; Rittler, Mónica; Rozental, Sandra; Barbero, Pablo; Dain, Liliana.

Genes (Basel) ; 9(9)2018 Sep 11.

Artigo em Inglês | MEDLINE | ID: mdl-30208644

RESUMO

Congenital conotruncal heart defects (CCHD) are a subset of serious congenital heart defects (CHD) of the cardiac outflow tracts or great arteries. Its frequency is estimated in 1/1000 live births, accounting for approximately 10â»30% of all CHD cases. Chromosomal abnormalities and copy number variants (CNVs) contribute to the disease risk in patients with syndromic and/or non-syndromic forms. Although largely studied in several populations, their frequencies are barely reported for Latin American countries. The aim of this study was to analyze chromosomal abnormalities, 22q11 deletions, and other genomic imbalances in a group of Argentinean patients with CCHD of unknown etiology. A cohort of 219 patients with isolated CCHD or associated with other major anomalies were referred from different provinces of Argentina. Cytogenetic studies, Multiplex-Ligation-Probe-Amplification (MLPA) and fluorescent in situ hybridization (FISH) analysis were performed. No cytogenetic abnormalities were found. 22q11 deletion was found in 23.5% of the patients from our cohort, 66% only had CHD with no other major anomalies. None of the patients with transposition of the great vessels (TGV) carried the 22q11 deletion. Other 4 clinically relevant CNVs were also observed: a distal low copy repeat (LCR)D-E 22q11 duplication, and 17p13.3, 4q35 and TBX1 deletions. In summary, 25.8% of CCHD patients presented imbalances associated with the disease.

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