A 600 kb deletion syndrome at 16p11.2 leads to energy imbalance and neuropsychiatric disorders.
Détails
Télécharger: BIB_26004E3F396F.P001.pdf (326.09 [Ko])
Etat: Public
Version: Final published version
Licence: CC BY 4.0
Etat: Public
Version: Final published version
Licence: CC BY 4.0
ID Serval
serval:BIB_26004E3F396F
Type
Article: article d'un périodique ou d'un magazine.
Collection
Publications
Institution
Titre
A 600 kb deletion syndrome at 16p11.2 leads to energy imbalance and neuropsychiatric disorders.
Périodique
Journal of Medical Genetics
Collaborateur⸱rice⸱s
Simons VIP Consortium, 16p11.2 European Consortium
Contributeur⸱rice⸱s
Addor MC., Arveiler B., Belfiore M., Bena F., Bernardini L., Blanchet P., Bonneau D., Boute O., Callier P., Campion D., Chiesa J., Cordier MP., Cuisset JM., David A., de Leeuw N., de Vries B., Didelot G., Doco-Fenzy M., Bedu BD., Dubourg C., Dupuis-Girod S., Fagerberg CR., Faivre L., Fellmann F., Fernandez BA., Fisher R., Flori E., Goldenberg A., Heron D., Holder M., Hoyer J., Isidor B., Jaillard S., Jonveaux P., Joriot S., Journel H., Kooy F., le Caignec C., Leheup B., Lemaitre MP., Lewis S., Malan V., Mathieu-Dramard M., Metspalu A., Morice-Picard F., Mucciolo M., Oiglane-Shlik E., Ounap K., Pasquier L., Petit F., Philippe A., Plessis G., Prieur F., Puechberty J., Rajcan-Separovic E., Rauch A., Renieri A., Rieubland C., Rooryck C., Rötzer KM., Ruiter M., Sanlaville D., Selmoni S., Shen Y., Siffredi V., Thonney J., Vallée L., van Binsbergen E., Van der Aa N., van Haelst MM, Vigneron J., Vincent-Delorme C., Vittoria D., Vulto-van Silfhout AT, Witwicki RM., Zwolinski SA., Bowe A., Beaudet AL., Brewton CM., Chu Z., Dempsey AG., Evans YL., Garza S., Kanne SM., Laakman AL., Lasala MW., Llorens AV., Marzano G., Moss TJ., Nowell KP., Proud MB., Chen Q., Vaughan R., Berman J., Blaskey L., Hines K., Kessler S., Khan SY., Qasmieh S., Bibb AL., Paal AM., Page PZ., Smith-Packard B., Buckner R., Burko J., Cavanagh AL., Cerban B., Snow AV., Snyder LG., Keehn RM., Miller DT., Miller FK., Olson JE., Triantafallou C., Visyak N., Atwell C., Benedetti M., Fischbach GD., Greenup M., Packer A., Bukshpun P., Cheong M., Dale C., Gobuty SE., Hinkley L., Jeremy RJ., Lee H., Luks TL., Marco EJ., Martin AJ., McGovern KE., Nagarajan SS., Owen J., Paul BM., Pojman NJ., Sinha T., Swarnakar V., Wakahiro M., Alupay H., Aaronson B., Ackerman S., Ankenman K., Elgin J., Gerdts J., Johnson K., Reilly B., Shaw D., Stevens A., Ward T., Wenegrat J.
ISSN
1468-6244 (Electronic)
ISSN-L
0022-2593
Statut éditorial
Publié
Date de publication
2012
Peer-reviewed
Oui
Volume
49
Numéro
10
Pages
660-668
Langue
anglais
Notes
Publication types: Journal Article ; Research Support, Non-U.S. Gov't
Publication Status: ppublish
Publication Status: ppublish
Résumé
BACKGROUND: The recurrent ~600 kb 16p11.2 BP4-BP5 deletion is among the most frequent known genetic aetiologies of autism spectrum disorder (ASD) and related neurodevelopmental disorders.
OBJECTIVE: To define the medical, neuropsychological, and behavioural phenotypes in carriers of this deletion.
METHODS: We collected clinical data on 285 deletion carriers and performed detailed evaluations on 72 carriers and 68 intrafamilial non-carrier controls.
RESULTS: When compared to intrafamilial controls, full scale intelligence quotient (FSIQ) is two standard deviations lower in carriers, and there is no difference between carriers referred for neurodevelopmental disorders and carriers identified through cascade family testing. Verbal IQ (mean 74) is lower than non-verbal IQ (mean 83) and a majority of carriers require speech therapy. Over 80% of individuals exhibit psychiatric disorders including ASD, which is present in 15% of the paediatric carriers. Increase in head circumference (HC) during infancy is similar to the HC and brain growth patterns observed in idiopathic ASD. Obesity, a major comorbidity present in 50% of the carriers by the age of 7 years, does not correlate with FSIQ or any behavioural trait. Seizures are present in 24% of carriers and occur independently of other symptoms. Malformations are infrequently found, confirming only a few of the previously reported associations.
CONCLUSIONS: The 16p11.2 deletion impacts in a quantitative and independent manner FSIQ, behaviour and body mass index, possibly through direct influences on neural circuitry. Although non-specific, these features are clinically significant and reproducible. Lastly, this study demonstrates the necessity of studying large patient cohorts ascertained through multiple methods to characterise the clinical consequences of rare variants involved in common diseases.
OBJECTIVE: To define the medical, neuropsychological, and behavioural phenotypes in carriers of this deletion.
METHODS: We collected clinical data on 285 deletion carriers and performed detailed evaluations on 72 carriers and 68 intrafamilial non-carrier controls.
RESULTS: When compared to intrafamilial controls, full scale intelligence quotient (FSIQ) is two standard deviations lower in carriers, and there is no difference between carriers referred for neurodevelopmental disorders and carriers identified through cascade family testing. Verbal IQ (mean 74) is lower than non-verbal IQ (mean 83) and a majority of carriers require speech therapy. Over 80% of individuals exhibit psychiatric disorders including ASD, which is present in 15% of the paediatric carriers. Increase in head circumference (HC) during infancy is similar to the HC and brain growth patterns observed in idiopathic ASD. Obesity, a major comorbidity present in 50% of the carriers by the age of 7 years, does not correlate with FSIQ or any behavioural trait. Seizures are present in 24% of carriers and occur independently of other symptoms. Malformations are infrequently found, confirming only a few of the previously reported associations.
CONCLUSIONS: The 16p11.2 deletion impacts in a quantitative and independent manner FSIQ, behaviour and body mass index, possibly through direct influences on neural circuitry. Although non-specific, these features are clinically significant and reproducible. Lastly, this study demonstrates the necessity of studying large patient cohorts ascertained through multiple methods to characterise the clinical consequences of rare variants involved in common diseases.
Mots-clé
Adolescent, Adult, Body Mass Index, Child, Child Development Disorders, Pervasive/diagnosis, Child Development Disorders, Pervasive/genetics, Chromosome Deletion, Chromosomes, Human, Pair 16, Developmental Disabilities/diagnosis, Developmental Disabilities/genetics, Female, Gene Order, Heterozygote, Humans, Intelligence Tests, Male, Phenotype, Syndrome, Young Adult
Pubmed
Web of science
Open Access
Oui
Création de la notice
23/11/2012 21:39
Dernière modification de la notice
11/01/2024 7:14