Your search keyword '"Gatinois, V."' showing total 4 results

1. Le syndrome Kabuki : mise au point et revue de la littérature.

Author

Arnaud, M., Barat-Houari, M., Gatinois, V., Sanchez, E., Lyonnet, S., Touitou, I., and Geneviève, D.

Abstract

Résumé Le syndrome Kabuki (OMIM : 147920 ) est un syndrome rare, associant principalement un déficit intellectuel, un syndrome poly-malformatif et des variations morphologiques du visage spécifiques permettant le diagnostic. Il présente néanmoins une forte hétérogénéité clinique et biologique comportant des symptômes plus rares mais très divers (problèmes endocrinologiques, maladies auto-immunes, obésité, etc.). Le diagnostic clinique reste difficile car il repose sur un faisceau d’arguments cliniques, radiologiques et biologiques. Les complications sont multiples, parfois inter-pénétrantes, et un diagnostic précoce de la maladie est indispensable pour une prise en charge optimale. La mise au point de tests génétiques a donc été essentielle. Récemment, le séquençage de tous les exons (exome) a permis d’identifier successivement deux gènes responsables de la maladie : KMT2D , plus connu sous le nom de MLL2 , et KDM6A . Les études fonctionnelles de ces gènes aideront à la compréhension de leur rôle dans la pathogenèse de la maladie, notamment en testant l’hypothèse de modifications épigénétiques lors de l’embryogenèse et du développement. La compréhension des interactions entre KMT2D et ses gènes cibles pourrait permettre d’identifier d’autres gènes candidats pour les cas encore inexpliqués de syndrome Kabuki. Summary Kabuki syndrome (OMIM: 147920 ) is a rare condition, mainly associating intellectual deficiency, a polymalformative syndrome, and specific morphological changes in the face. It nevertheless has a strong clinical and biological heterogeneity with rarer but very different symptoms (endocrinological anomalies, autoimmune disorders, obesity, etc.). Clinical diagnosis is difficult because it is based on a spectrum of clinical, radiological, and biological factors. Complications are numerous, sometimes interpenetrating, and early diagnosis of the disease is essential for optimal management. The development of genetic testing is therefore essential for the diagnosis of this disease. Recently, exome sequencing has helped identify two genes responsible for the disease: KMT2D (lysine (K)-specific methyltransferase 2D, better known as MLL2 - mixed lineage leukemia), and KDM6A (lysine-specific demethylase 6A). Functional studies of these genes should help clarify their role in the pathogenesis of the disease, in particular to test the hypothesis of epigenetic changes during embryogenesis and development. Finally, understanding the interactions between KMT2D and its target genes could unravel other candidate genes for hitherto unexplained Kabuki syndrome cases. [ABSTRACT FROM AUTHOR]

Published

2015

2. Chromoanagenesis, the mechanisms of a genomic chaos.

Author

Pellestor, F., Gaillard, JB, Schneider, A., Puechberty, J., and Gatinois, V.

Subjects

*CHROMOSOME segregation, *CHROMOSOMAL rearrangement, *NUCLEOLUS, *CHROMATIN

Abstract

Designated under the name of chromoanagenesis, the phenomena of chromothripsis, chromanasynthesis and chromoplexy constitute new types of complex rearrangements, including many genomic alterations localized on a few chromosomal regions, and whose discovery over the last decade has changed our perception about the formation of chromosomal abnormalities and their etiology. Although exhibiting specific features, these new catastrophic mechanisms generally occur within a single cell cycle and their emergence is closely linked to genomic instability. Various non-exclusive exogenous or cellular mechanisms capable of generating chromoanagenesis have been evoked. However, recent experimental data shed light on 2 major processes, which following a defect in the mitotic segregation of chromosomes, can generate a cascade of cellular events leading to chromoanagenesis. These mechanisms are the formation of micronuclei integrating isolated chromosomal material, and the occurrence of chromatin bridges around chromosomal material resulting from telomeric fusions. In both cases, the cellular and molecular mechanisms of fragmentation, repair and transmission of damaged chromosomal material are consistent with the features of chromoanagenesis-related complex chromosomal rearrangements. In this review, we introduce each type of chromoanagenesis, and describe the experimental models that have allowed to validate the existence of chromoanagenesis events and to better understand their cellular mechanisms of formation and transmission, as well as their impact on the stability and the plasticity of the genome. [ABSTRACT FROM AUTHOR]

Published

2022

3. Molecular, clinical and neuropsychological study in 31 patients with Kabuki syndrome and KMT2D mutations.

Author

Lehman, N., Mazery, A.C., Visier, A., Baumann, C., Lachesnais, D., Capri, Y., Toutain, A., Odent, S., Mikaty, M., Goizet, C., Taupiac, E., Jacquemont, M.L., Sanchez, E., Schaefer, E., Gatinois, V., Faivre, L., Minot, D., Kayirangwa, H., Sang, K.‐H.L.Q., and Boddaert, N.

Subjects

*NEUROPSYCHOLOGY, *KABUKI syndrome, *INTELLECTUAL disabilities, *SHORT-term memory, *GENETIC mutation

Abstract

Kabuki syndrome ( KS-OMIM 147920) is a rare developmental disease characterized by the association of multiple congenital anomalies and intellectual disability. This study aimed to investigate intellectual performance in children with KS and link the performance to several clinical features and molecular data. We recruited 31 children with KMT2D mutations who were 6 to 16 years old. They all completed the Weschler Intelligence Scale for Children, fourth edition. We calculated all indexes: the Full Scale Intellectual Quotient ( FSIQ), Verbal Comprehension Index ( VCI), Perceptive Reasoning Index ( PRI), Processing Speed Index ( PSI), and Working Memory Index ( WMI). In addition, molecular data and several clinical symptoms were studied. FSIQ and VCI scores were 10 points lower for patients with a truncating mutation than other types of mutations. In addition, scores for FSIQ, VCI and PRI were lower for children with visual impairment than normal vision. We also identified a discrepancy in indexes characterized by high WMI and VCI and low PRI and PSI. We emphasize the importance of early identification and intensive care of visual disorders in patients with KS and recommend individual assessment of intellectual profile. [ABSTRACT FROM AUTHOR]

Published

2017

4. Discordant sex in monozygotic XXY/XX twins: a case report.

Author

Tachon, G., Lefort, G., Puechberty, J., Schneider, A., Jeandel, C., Boulot, P., Prodhomme, O., Meyer, P., Taviaux, S., Touitou, I., Pellestor, F., Geneviève, D., and Gatinois, V.

Subjects

*HUMAN phenotype, *ZYGOTES, *KLINEFELTER'S syndrome, *DISEASES in twins, *LANGUAGE disorders

Abstract

We report a case of discordant phenotypic sex in monozygotic twins mosaic 47,XXY/46,XX: monozygotic heterokaryotypic twins. The twins presented with cognitive and comprehension delay, behavioural and language disorders, all symptoms frequently reported in Klinefelter syndrome. Molecular zygosity analysis with several markers confirmed that the twins are in effect monozygotic (MZ). Array comparative genomic hybridization found no evidence for the implication of copy number variation in the phenotypes. Ultrasound scans of the reproductive organs revealed no abnormalities. Endocrine tests showed a low testosterone level in Twin 1 (male phenotype) and a low gonadotrophin level in Twin 2 (female phenotype) which, combined with the results from ultrasound examination, provided useful information for potentially predicting the future fertility potential of the twins. Blood karyotypes revealed the presence of a normal 46,XX cell line and an aneuploïd 47,XXY cell line in both patients. Examination of the chromosome constitutions of various tissues such as blood, buccal smear and urinary sediment not surprisingly showed different proportions for the 46,XX and 47,XXY cell lines, which most likely explains the discordant phenotypic sex and mild Klinefelter features. The most plausible underlying biological mechanism is a post-zygotic loss of the Y chromosome in an initially 47,XXY zygote. This would result in an embryo with both 46,XX and 47,XXY cells lines which could subsequently divide into two monozygotic embryos through a twinning process. The two cell lines would then be distributed differently between tissues which could result in phenotypic discordances in the twins. These observations emphasize the importance of regular paediatric evaluations to determine the optimal timing for fertility preservation measures and to detect new Klinefelter features which could appear throughout childhood in the two subjects. [ABSTRACT FROM AUTHOR]

Published

2014