| Literature DB >> 33505230 |
Olga M Moreno1, Ana I Sánchez1,2,3, Angélica Herreño1, Gustavo Giraldo1, Fernando Suárez1,4, Juan Carlos Prieto1, Ana Shaia Clavijo1, Mercedes Olaya5, Yaris Vargas6, Javier Benítez7, Jordi Surallés8, Adriana Rojas1.
Abstract
VACTERL association (OMIM 192350) is a heterogeneous clinical condition characterized by congenital structural defects that include at least 3 of the following features: vertebral abnormalities, anal atresia, heart defects, tracheoesophageal fistula, renal malformations, and limb defects. The nonrandom occurrence of these malformations and some familial cases suggest a possible association with genetic factors such as chromosomal alterations, gene mutations, and inherited syndromes such as Fanconi anemia (FA). In this study, the clinical phenotype and its relationship with the presence of chromosomal abnormalities and FA were evaluated in 18 patients with VACTERL association. For this, a G-banded karyotype, array-comparative genomic hybridization, and chromosomal fragility test for FA were performed. All patients (10 female and 8 male) showed a broad clinical spectrum: 13 (72.2%) had vertebral abnormalities, 8 (44.4%) had anal atresia, 14 (77.8%) had heart defects, 8 (44.4%) had esophageal atresia, 10 (55.6%) had renal abnormalities, and 10 (55.6%) had limb defects. Chromosomal abnormalities and FA were ruled out. In 2 cases, the finding of microalterations, namely del(15)(q11.2) and dup(17)(q12), explained the phenotype; in 8 cases, copy number variations were classified as variants of unknown significance and as not yet described in VACTERL. These variants comprise genes related to important cellular functions and embryonic development.Entities:
Keywords: Array-CGH; Chromosomal microalterations; Congenital malformations; Copy-number variants; Fanconi anemia; VACTERL association
Year: 2020 PMID: 33505230 PMCID: PMC7802448 DOI: 10.1159/000510910
Source DB: PubMed Journal: Mol Syndromol ISSN: 1661-8769