Your search keyword '"Selima Siala"' showing total 4 results

1. Arteriovenous Cerebral High Flow Shunts in Children: From Genotype to Phenotype

Author

Berivan Tas, Daniele Starnoni, Stanislas Smajda, Alexandre J. Vivanti, Catherine Adamsbaum, Mélanie Eyries, Judith Melki, Marcel Tawk, Augustin Ozanne, Nicole Revencu, Florent Soubrier, Selima Siala, Miikka Vikkula, Kumaran Deiva, and Guillaume Saliou

Subjects

vein of Galen aneurysmal malformation, cerebral arteriovenous fistula, arteriovenous shunt (AVS), Rendu-Osler-Weber disease, RASA1 mutation, EPHB4 mutation, Pediatrics, RJ1-570

Abstract

ObjectiveTo study the genotypes and phenotypes of cerebral arteriovenous fistulas that drain or do not drain through the vein of Galen, and true vein of Galen aneurysmal malformations, in order to determine whether genotyping could help improve classification of these malformations and their management.MethodsWe carried out a retrospective review of genetic and phenotypic data in databases of four centers. All children with cerebral arteriovenous fistula or vein of Galen aneurysmal malformations aged below 18 years at onset were included. We recorded the nature of the genetic variant or absence of variant, age at onset, type of malformation, symptoms at onset (hemorrhage, neurological deficit, hydrocephalus, incidental, and heart failure), type of venous drainage and the long-term outcome.ResultsOne hundred and fifteen children were included. Autosomal dominant variants were identified in 39% of patients. The most frequent variant affected was the RASA1 gene (25%) followed by EPHB4 (8%) and the HHT-associated genes (5%). HHT gene variants were only observed in pial arteriovenous fistula not draining into the vein of Galen; on the contrary, EPHB4 variants were only seen in genuine vein of Galen aneurysmal malformation. RASA1 variants were identified in all types of shunts.ConclusionsEPHB4 variants seem specific to the vein of Galen aneurysmal malformation, RASA1 variants are associated with either pial arteriovenous fistulas or with genuine VGAM and HHT gene variants seem specific to pial arteriovenous fistulas. The genetic data helps to classify these malformations and to guide treatment toward lowest risk of post-operative cerebral ischemic-hemorrhagic complications.

Published

2022

2. Case report: Severe brain hypoxic damages after acute methanol poisoning

Author

Ameni Abidi, Asma Souid, Khalaf B Abdallah, Nadia Hammami, Selima Siala, Nozha Brahmi, and Mohamed B Hamouda

Subjects

case report, hemorrhagic necrosis, hypoxia, magnetic resonance imaging, methanol poisoning, white matter demyelination, Medicine, Medicine (General), R5-920

Abstract

Abstract Methanol poisoning is a challenging clinical situation with irreversible neurologic complication mainly encountered in developed countries. We report a case of a 50‐year‐old patient who presented with methanol poisoning, symptomatic of respiratory and neurologic failure. In this context, cerebral magnetic resonance imaging concluded entangled injury mechanisms leading to neurologic failure.

Published

2022

3. Imaging of the septum pellucidum: normal, variants and pathology

Author

Selima Siala, Dean Homen, Benjamin Smith, and Carolina Guimaraes

Subjects

Radiology, Nuclear Medicine and imaging, General Medicine

Abstract

The septum pellucidum is a largely neglected anatomical midline structure during post-natal neuroimaging interpretation. Conversely, it is one of the anatomical landmarks used on pre-natal ultrasound to access normal midline formation. Because of its importance during the pre-natal period, the awareness of its primary malformative abnormalities is much higher than its disruptive acquired pathologies, often leading the misinterpretation. In this article, we will review the normal septum pellucidum formation, anatomy, and anatomical variants and will describe the imaging findings in primary malformative and secondary disruptive abnormalities affecting the septum pellucidum.

Published

2023

4. Arteriovenous Cerebral High Flow Shunts in Children: From Genotype to Phenotype

Author

Berivan, Tas, Daniele, Starnoni, Stanislas, Smajda, Alexandre J, Vivanti, Catherine, Adamsbaum, Mélanie, Eyries, Judith, Melki, Marcel, Tawk, Augustin, Ozanne, Nicole, Revencu, Florent, Soubrier, Selima, Siala, Miikka, Vikkula, Kumaran, Deiva, Guillaume, Saliou, and UCL - SSS/DDUV/GEHU - Génétique

Subjects

arteriovenous shunt (AVS), vein of Galen aneurysmal malformation, cerebral arteriovenous fistula, cardiovascular system, EPHB4 mutation, Perinatology and Child Health, Rendu-Osler-Weber disease, Pediatrics, RASA1 mutation

Abstract

To study the genotypes and phenotypes of cerebral arteriovenous fistulas that drain or do not drain through the vein of Galen, and true vein of Galen aneurysmal malformations, in order to determine whether genotyping could help improve classification of these malformations and their management. We carried out a retrospective review of genetic and phenotypic data in databases of four centers. All children with cerebral arteriovenous fistula or vein of Galen aneurysmal malformations aged below 18 years at onset were included. We recorded the nature of the genetic variant or absence of variant, age at onset, type of malformation, symptoms at onset (hemorrhage, neurological deficit, hydrocephalus, incidental, and heart failure), type of venous drainage and the long-term outcome. One hundred and fifteen children were included. Autosomal dominant variants were identified in 39% of patients. The most frequent variant affected was the gene (25%) followed by (8%) and the HHT-associated genes (5%). HHT gene variants were only observed in pial arteriovenous fistula not draining into the vein of Galen; on the contrary, variants were only seen in genuine vein of Galen aneurysmal malformation. variants were identified in all types of shunts. variants seem specific to the vein of Galen aneurysmal malformation, variants are associated with either pial arteriovenous fistulas or with genuine VGAM and HHT gene variants seem specific to pial arteriovenous fistulas. The genetic data helps to classify these malformations and to guide treatment toward lowest risk of post-operative cerebral ischemic-hemorrhagic complications.

Published

2022