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Your search keyword '"Kien, P. Khau Van"' showing total 8 results
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8 results on '"Kien, P. Khau Van"'

1. Clinical and molecular findings in 39 patients with KBG syndrome caused by deletion or mutation of ANKRD11

Author

Goldenberg, A., Riccardi, F., Tessier, A., Pfundt, R.P., Busa, T., Cacciagli, P., Capri, Y., Coutton, C., Delahaye-Duriez, A., Frebourg, T., Gatinois, V., Guerrot, A.M., Genevieve, D., Lecoquierre, F., Jacquette, A., Kien, P. Khau Van, Leheup, B., Marlin, S., Verloes, A., Michaud, V., Nadeau, G., Mignot, C., Parent, P., Rossi, M., Toutain, A., Schaefer, E., Thauvin-Robinet, C., Maldergem, L. Van, Thevenon, J., Satre, V., Perrin, L., Vincent-Delorme, C., Sorlin, A., Missirian, C., Villard, L., Mancini, J., Saugier-Veber, P., Philip, N., Goldenberg, A., Riccardi, F., Tessier, A., Pfundt, R.P., Busa, T., Cacciagli, P., Capri, Y., Coutton, C., Delahaye-Duriez, A., Frebourg, T., Gatinois, V., Guerrot, A.M., Genevieve, D., Lecoquierre, F., Jacquette, A., Kien, P. Khau Van, Leheup, B., Marlin, S., Verloes, A., Michaud, V., Nadeau, G., Mignot, C., Parent, P., Rossi, M., Toutain, A., Schaefer, E., Thauvin-Robinet, C., Maldergem, L. Van, Thevenon, J., Satre, V., Perrin, L., Vincent-Delorme, C., Sorlin, A., Missirian, C., Villard, L., Mancini, J., Saugier-Veber, P., and Philip, N.

Abstract

Item does not contain fulltext, KBG syndrome, due to ANKRD11 alteration is characterized by developmental delay, short stature, dysmorphic facial features, and skeletal anomalies. We report a clinical and molecular study of 39 patients affected by KBG syndrome. Among them, 19 were diagnosed after the detection of a 16q24.3 deletion encompassing the ANKRD11 gene by array CGH. In the 20 remaining patients, the clinical suspicion was confirmed by the identification of an ANKRD11 mutation by direct sequencing. We present arguments to modulate the previously reported diagnostic criteria. Macrodontia should no longer be considered a mandatory feature. KBG syndrome is compatible with autonomous life in adulthood. Autism is less frequent than previously reported. We also describe new clinical findings with a potential impact on the follow-up of patients, such as precocious puberty and a case of malignancy. Most deletions remove the 5'end or the entire coding region but never extend toward 16q telomere suggesting that distal 16q deletion could be lethal. Although ANKRD11 appears to be a major gene associated with intellectual disability, KBG syndrome remains under-diagnosed. NGS-based approaches for sequencing will improve the detection of point mutations in this gene. Broad knowledge of the clinical phenotype is essential for a correct interpretation of the molecular results. (c) 2016 Wiley Periodicals, Inc.

Published
2016

2. Cloacal exstrophy in an infant with 9q34.1-qter deletion resulting from a de novo unbalanced translocation between chromosome 9q and Yq

Author

Thauvin-Robinet, Christel, Faivre, Laurence, Cusin, Véronica, Kien, Philippe Khau Van, Callier, Patrick, Parker, Keith L., Fellous, Marc, Borgnon, Joséphine, Gounot, Emmanuel, Huet, Frédéric, Sapin, Emmanuel, and Mugneret, Francine

Abstract

Cloacal exstrophy is a rare malformation, belonging to a spectrum of birth defects, which, in order of severity, includes phallic separation with epispadias, pubic diastasis, bladder exstrophy, and cloacal exstrophy. This malformation overlaps the OEIS complex (O = omphalocele, E = bladder exstrophy, I = imperforate anus, S = spinal defects). The etiology of cloacal exstrophy is unknown to date. It may result from either a single defect of early blastogenesis or a defect of mesodermal migration during the primitive streak period. We report an infant with cloacal exstrophy, exomphalos, right kidney agenesis, ambiguous external genitalia, and axial hypotonia. The karyotype showed a de novo unbalanced translocation between the long arm of chromosome 9 and the long arm of chromosome Y resulting in a 9q34.1-qter deletion. Reviewing the literature, we did not find any observation of cloacal exstrophy associated with a structural chromosomal abnormality. The steroidogenic factor 1 (SF1) gene, included in the deleted region, was a good candidate gene but no pathogenic mutation was found by direct sequencing. We hypothesize that another gene, expressed early in embryogenesis and responsible for cloacal exstrophy, is present in the 9q34.1-qter region. © 2003 Wiley-Liss, Inc.

Published
2004
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3. Mazabraud syndrome in two patients: Clinical overlap with McCune-Albright syndrome

Author

Faivre, L., Nivelon-Chevallier, A., Kottler, M.L., Robinet, C., Kien, P. Khau Van, Lorcerie, B., Munnich, A., Maroteaux, P., Cormier-Daire, V., and LeMerrer, M.

Abstract

Mazabraud syndrome is a rare sporadic disorder, mainly characterized by bone fibrous dysplasia and intramuscular myxomas. We report here two new cases of Mazabraud syndrome. One of our patients (Patient 1) also had café-au-lait spots and multinodular goiter suggestive of McCune-Albright syndrome. We review the 37 previously reported cases with Mazabraud syndrome and discuss the 6/37 patients with criteria of Mazabraud and McCune-Albright syndromes. Based on the clinical overlap between the two syndromes, we tested the GNAS1 gene in blood leukocytes and skin fibroblasts of Patient 1, but found no evidence of an activating mutation in the GNAS1 gene. © 2001 Wiley-Liss, Inc.

Published
2001
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7. Dystrophie Musculaire Facio-Scapulo-Humérale (DMFSH) associée au syndrome de délétion du chromosome 18 (18p-)

Author

Capet, Nicolas, Dimitri, Renard, Feasson, Leonard, Manel, Véronique, Echaniz-Laguna, Andoni, Kien, Philippe Khau Van, and Sacconi, Sabrina

Abstract

La DMFSH est causée par une dépression génétique et épigénétique du locus D4Z4 due à la présence d’une contraction pathologique en 4q, ou à une mutation dans le gène SMCHD1 localisé en 18p.

Published
2017
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