Genetic analysis of syndromic and nonsyndromic patients with craniosynostosis identifies novel mutations in the TWISTI and EfnbI Genes

Επιστημονική δημοσίευση - Άρθρο Περιοδικού uoadl:2990273 7 Αναγνώσεις

Μονάδα:
Ερευνητικό υλικό ΕΚΠΑ
Τίτλος:
Genetic analysis of syndromic and nonsyndromic patients with craniosynostosis identifies novel mutations in the TWISTI and EfnbI Genes
Γλώσσες Τεκμηρίου:
Αγγλικά
Περίληψη:
Introduction: Craniosynostosis, the premature fusion of cranial sutures, is usually divided into 2 major categories: syndromic and nonsyndromic. Mutations in the FGFR1, FGFR2, FGFR3, TWIST1, and EFNB1 genes cause the common craniosynostosis syndromes Muenke, Crouzon and Crouzon with acanthosis nigricans, Apert, Pfeiffer, Saethre-Chotzen, and Craniofrontonasal. Overlapping features among craniosynostosis syndromes, phenotypic heterogeneity even within the same syndrome, especially in the case of Muenke syndrome, and inadequate clinical evaluation can lead to misdiagnosis, which molecular testing can help clarify. Objective: The aim of this study is to investigate the underlying genetic cause in 46 patients with syndromic or nonsyndromic craniosynostosis by direct sequencing and/or microdeletion/microduplication analysis of the FGFR1-3, TWIST1, and EFNB1 genes. Results: Genetic analysis identified 3 novel mutations, c.413T>C - p.(Leu138Pro) [p.(L138P)] in TWIST1, the previously reported c.373G>A - p.(Glu125Lys) [p.(E125K)], and c.717dupA - p.(Leu240IlefsTer79) [p.(L240fs)] mutation in EFNB1 gene as well as 6 previously known mutations and a heterozygous TWIST1 gene deletion. The 2 novel mutations within EFNB1 gene arose de novo, but the novel mutation p.(L138P) within TWIST1 gene was inherited from the patient’s father, who was found to be mosaic for the mutation. To our knowledge, this is the first case of mosaicism described for TWIST1 gene. Conclusions: The contribution of molecular genetic analysis to the diagnosis of patients with syndromic craniosynostosis was useful because some were originally misdiagnosed. Conversely, thorough clinical evaluation can guide molecular testing and result in a correct diagnosis. © 2018, American Cleft Palate-Craniofacial Association.
Έτος δημοσίευσης:
2018
Συγγραφείς:
Apostolopoulou, D.
Kaxira, O.S.
Hatzaki, A.
Panagopoulos, K.P.
Alexandrou, K.
Stratoudakis, A.
Kollia, P.
Aleporou, V.
Περιοδικό:
THE CLEFT PALATE-CRANIOFACIAL JOURNAL
Εκδότης:
SAGE Publications Ltd
Τόμος:
55
Αριθμός / τεύχος:
8
Σελίδες:
1092-1102
Λέξεις-κλειδιά:
ephrin B1; fibroblast growth factor receptor 1; fibroblast growth factor receptor 2; fibroblast growth factor receptor 3; Twist related protein 1, acrocephalosyndactyly; agar gel electrophoresis; amino acid substitution; amplified fragment length polymorphism; Article; child; clinical article; clinical evaluation; craniofacial synostosis; craniofrontonasal syndrome; Crouzon syndrome; Cyprus; DNA sequence; frameshift mutation; gene deletion; gene mutation; genetic analysis; genetic screening; Greece; heterozygote; human; missense mutation; molecular diagnosis; mosaicism; Muenke syndrome; mutational analysis; paternal inheritance; phenotype; polymerase chain reaction; priority journal; short tandem repeat
Επίσημο URL (Εκδότης):
DOI:
10.1177/1055665618760412
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