Your search keyword '"Veltra, Danai"' showing total 3 results

1. Retrospective analysis of persistent HyperCKemia with or without muscle weakness in a case series from Greece highlights vast DMD variant heterogeneity.

Author

Kekou, Kyriaki, Svingou, Maria, Vogiatzakis, Nikos, Nitsa, Evangelia, Veltra, Danai, Marinakis, Nikolaos M., Tilemis, Faidon-Nikolaos, Tzetis, Maria, Mitrakos, Anastasios, Tsaroucha, Charalambia, Selenti, Nicoletta, Papadimas, Giorgos-Konstantinos, Papadopoulos, Constantinos, Traeger-Synodinos, Joanne, Lochmuller, Hanns, and Sofocleous, Christalena

Abstract

Persistent hyperCKemia results from muscle dysfunction often attributed to genetic alterations of muscle-related genes, such as the dystrophin gene (DMD). Retrospective assessment of findings from DMD analysis, in association with persistent HyperCKemia, was conducted. Evaluation of medical records from 1354 unrelated cases referred during the period 1996–2021. Assessment of data concerning the detection of DMD gene rearrangements and nucleotide variants. A total of 730 individuals (657 cases, 569 of Greek and 88 of Albanian origins) were identified, allowing an overall estimation of dystrophinopathy incidence at ~1:3800 live male births. The heterogeneous spectrum of 275 distinct DMD alterations comprised exon(s) deletions/duplications, nucleotide variants, and rare events, such as chromosome translocation {t(X;20)}, contiguous gene deletions, and a fused gene involving the DMD and the DOCK8 genes. Ethnic-specific findings include a common founder variant in exon 36 ('Hellenic' variant). Some 50% of hyperCKemia cases were characterized as dystrophinopathies, highlighting that DMD variants may be considered the most common cause of hyperCKemia in Greece. Delineation of the broad genetic and clinical heterogeneity is fundamental for actionable public health decisions and theragnosis, as well as the establishment of guidelines addressing ethical considerations, especially related to the mild asymptomatic patient subgroup. [ABSTRACT FROM AUTHOR]

Published

2023

2. Combined exome analysis and exome depth assessment achieve a high diagnostic yield in an epilepsy case series, revealing significant genomic heterogeneity and novel mechanisms.

Author

Veltra, Danai, Tilemis, Faidon-Nikolaos, Marinakis, Nikolaos M., Svingou, Maria, Mitrakos, Anastasios, Kosma, Konstantina, Tsoutsou, Irene, Makrythanasis, Periklis, Theodorou, Virginia, Katsalouli, Marina, Vorgia, Pelagia, Niotakis, Georgios, Vartzelis, Georgios, Dinopoulos, Argirios, Evangeliou, Athanasios, Mouskou, Stella, Korona, Anastasia, Mastroyianni, Sotiria, Papavasiliou, Antigone, and Tzetis, Maria

Abstract

Genetics of epilepsy are highly heterogeneous and complex. Lesions detected involve genes encoding various types of channels, transcription factors, and other proteins implicated in numerous cellular processes, such as synaptogenesis. Consequently, a wide spectrum of clinical presentations and overlapping phenotypes hinders differential diagnosis and highlights the need for molecular investigations toward delineation of underlying mechanisms and final diagnosis. Characterization of defects may also contribute valuable data on genetic landscapes and networks implicated in epileptogenesis. This study reports on genetic findings from exome sequencing (ES) data of 107 patients with variable types of seizures, with or without additional symptoms, in the context of neurodevelopmental disorders. Multidisciplinary evaluation of ES, including ancillary detection of copy number variants (CNVs) with the ExomeDepth tool, supported a definite diagnosis in 59.8% of the patients, reflecting one of the highest diagnostic yields in epilepsy. Emerging advances of next-generation technologies and 'in silico' analysis tools offer the possibility to simultaneously detect several types of variations. Wide assessment of variable findings, specifically those found to be novel and least expected, reflects the ever-evolving genetic landscape of seizure development, potentially beneficial for increased opportunities for trial recruitment and enrollment, and optimized, even personalized, medical management. [ABSTRACT FROM AUTHOR]

Published

2023

3. Detection of a novel unbalanced X;21 translocation in a girl with Turner syndrome phenotype.

Author

Kouvidi, Elisavet, Zachaki, Sophia, Selenti, Nikoletta, Veltra, Danai, Evmorfopoulou, Theodora, Tsoutsou, Eirini, Tzifa, Garifallia, Sofocleous, Christalena, Gagos, Sarantis, and Mavrou, Ariadni

Subjects

TURNER'S syndrome, PEPTIDE nucleic acids, PHENOTYPES, X chromosome, FLUORESCENCE in situ hybridization

Abstract

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Published

2021