WAC loss-of-function mutations cause a recognisable syndrome characterised by dysmorphic features, developmental delay and hypotonia and recapitulate 10p11.23 microdeletion syndrome

Cori De Santo; Kristin D'Aco; Gabriel C. Araujo; Nora Shannon; D. D.D. Study; Hilary Vernon; April Rahrig; Kristin G. Monaghan; Zhiyv Niu; Patrik Vitazka; Jonathan Dodd; Sha Tang; Linda Manwaring; Arelis Martir-Negron; Rhonda E. Schnur; Jane Juusola; Audrey Schroeder; Vivian Pan; Katherine L. Helbig; Bethany Friedman; Marwan Shinawi

doi:10.1136/jmedgenet-2015-103069

WAC loss-of-function mutations cause a recognisable syndrome characterised by dysmorphic features, developmental delay and hypotonia and recapitulate 10p11.23 microdeletion syndrome

Cori De Santo, Kristin D'Aco, Gabriel C. Araujo, Nora Shannon, D. D.D. Study, Hilary Vernon, April Rahrig, Kristin G. Monaghan, Zhiyv Niu, Patrik Vitazka, Jonathan Dodd, Sha Tang, Linda Manwaring, Arelis Martir-Negron, Rhonda E. Schnur, Jane Juusola, Audrey Schroeder, Vivian Pan, Katherine L. Helbig, Bethany FriedmanMarwan Shinawi

School of Medicine

Research output: Contribution to journal › Article › peer-review

20 Scopus citations

Abstract

Background Rare de novo mutations have been implicated as a significant cause of idiopathic intellectual disability. Large deletions encompassing 10p11.23 have been implicated in developmental delay, behavioural abnormalities and dysmorphic features, but the genotype-phenotype correlation was not delineated. Mutations in WAC have been recently reported in large screening cohorts of patients with intellectual disability or autism, but no full phenotypic characterisation was described. Methods Clinical and molecular characterisation of six patients with loss-of-function WAC mutations identified by whole exome sequencing was performed. Clinical data were obtained by retrospective chart review, parental interviews, direct patient interaction and formal neuropsychological evaluation. Results Five heterozygous de novo WAC mutations were identified in six patients. Three of the mutations were nonsense, and two were frameshift; all are predicted to cause loss of function either through nonsense-mediated mRNA decay or protein truncation. Clinical findings included developmental delay (6/6), hypotonia (6/6), behavioural problems (5/6), eye abnormalities (5/6), constipation (5/6), feeding difficulties (4/6), seizures (2/6) and sleep problems (2/6). All patients exhibited common dysmorphic features, including broad/prominent forehead, synophrys and/or bushy eyebrows, depressed nasal bridge and bulbous nasal tip. Posteriorly rotated ears, hirsutism, deep-set eyes, thin upper lip, inverted nipples, hearing loss and branchial cleft anomalies were also noted. Conclusions Our case series show that loss-of-function mutations in WAC cause a recognisable genetic syndrome characterised by a neurocognitive phenotype and facial dysmorphism. Our data highly suggest that WAC haploinsufficiency is responsible for most of the phenotypic features associated with deletions encompassing 10p11.23.

Original language	English (US)
Pages (from-to)	754-761
Number of pages	8
Journal	Journal of medical genetics
Volume	52
Issue number	11
DOIs	https://doi.org/10.1136/jmedgenet-2015-103069
State	Published - Aug 11 2015

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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De Santo, C., D'Aco, K., Araujo, G. C., Shannon, N., Study, D. D. D., Vernon, H., Rahrig, A., Monaghan, K. G., Niu, Z., Vitazka, P., Dodd, J., Tang, S., Manwaring, L., Martir-Negron, A., Schnur, R. E., Juusola, J., Schroeder, A., Pan, V., Helbig, K. L., ... Shinawi, M. (2015). WAC loss-of-function mutations cause a recognisable syndrome characterised by dysmorphic features, developmental delay and hypotonia and recapitulate 10p11.23 microdeletion syndrome. Journal of medical genetics, 52(11), 754-761. https://doi.org/10.1136/jmedgenet-2015-103069

WAC loss-of-function mutations cause a recognisable syndrome characterised by dysmorphic features, developmental delay and hypotonia and recapitulate 10p11.23 microdeletion syndrome. / De Santo, Cori; D'Aco, Kristin; Araujo, Gabriel C. et al.
In: Journal of medical genetics, Vol. 52, No. 11, 11.08.2015, p. 754-761.

Research output: Contribution to journal › Article › peer-review

De Santo, C, D'Aco, K, Araujo, GC, Shannon, N, Study, DDD, Vernon, H, Rahrig, A, Monaghan, KG, Niu, Z, Vitazka, P, Dodd, J, Tang, S, Manwaring, L, Martir-Negron, A, Schnur, RE, Juusola, J, Schroeder, A, Pan, V, Helbig, KL, Friedman, B & Shinawi, M 2015, 'WAC loss-of-function mutations cause a recognisable syndrome characterised by dysmorphic features, developmental delay and hypotonia and recapitulate 10p11.23 microdeletion syndrome', Journal of medical genetics, vol. 52, no. 11, pp. 754-761. https://doi.org/10.1136/jmedgenet-2015-103069

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title = "WAC loss-of-function mutations cause a recognisable syndrome characterised by dysmorphic features, developmental delay and hypotonia and recapitulate 10p11.23 microdeletion syndrome",

abstract = "Background Rare de novo mutations have been implicated as a significant cause of idiopathic intellectual disability. Large deletions encompassing 10p11.23 have been implicated in developmental delay, behavioural abnormalities and dysmorphic features, but the genotype-phenotype correlation was not delineated. Mutations in WAC have been recently reported in large screening cohorts of patients with intellectual disability or autism, but no full phenotypic characterisation was described. Methods Clinical and molecular characterisation of six patients with loss-of-function WAC mutations identified by whole exome sequencing was performed. Clinical data were obtained by retrospective chart review, parental interviews, direct patient interaction and formal neuropsychological evaluation. Results Five heterozygous de novo WAC mutations were identified in six patients. Three of the mutations were nonsense, and two were frameshift; all are predicted to cause loss of function either through nonsense-mediated mRNA decay or protein truncation. Clinical findings included developmental delay (6/6), hypotonia (6/6), behavioural problems (5/6), eye abnormalities (5/6), constipation (5/6), feeding difficulties (4/6), seizures (2/6) and sleep problems (2/6). All patients exhibited common dysmorphic features, including broad/prominent forehead, synophrys and/or bushy eyebrows, depressed nasal bridge and bulbous nasal tip. Posteriorly rotated ears, hirsutism, deep-set eyes, thin upper lip, inverted nipples, hearing loss and branchial cleft anomalies were also noted. Conclusions Our case series show that loss-of-function mutations in WAC cause a recognisable genetic syndrome characterised by a neurocognitive phenotype and facial dysmorphism. Our data highly suggest that WAC haploinsufficiency is responsible for most of the phenotypic features associated with deletions encompassing 10p11.23.",

author = "{De Santo}, Cori and Kristin D'Aco and Araujo, {Gabriel C.} and Nora Shannon and Study, {D. D.D.} and Hilary Vernon and April Rahrig and Monaghan, {Kristin G.} and Zhiyv Niu and Patrik Vitazka and Jonathan Dodd and Sha Tang and Linda Manwaring and Arelis Martir-Negron and Schnur, {Rhonda E.} and Jane Juusola and Audrey Schroeder and Vivian Pan and Helbig, {Katherine L.} and Bethany Friedman and Marwan Shinawi",

year = "2015",

month = aug,

day = "11",

doi = "10.1136/jmedgenet-2015-103069",

language = "English (US)",

volume = "52",

pages = "754--761",

journal = "Journal of medical genetics",

issn = "0022-2593",

publisher = "BMJ Publishing Group",

number = "11",

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TY - JOUR

T1 - WAC loss-of-function mutations cause a recognisable syndrome characterised by dysmorphic features, developmental delay and hypotonia and recapitulate 10p11.23 microdeletion syndrome

AU - De Santo, Cori

AU - D'Aco, Kristin

AU - Araujo, Gabriel C.

AU - Shannon, Nora

AU - Study, D. D.D.

AU - Vernon, Hilary

AU - Rahrig, April

AU - Monaghan, Kristin G.

AU - Niu, Zhiyv

AU - Vitazka, Patrik

AU - Dodd, Jonathan

AU - Tang, Sha

AU - Manwaring, Linda

AU - Martir-Negron, Arelis

AU - Schnur, Rhonda E.

AU - Juusola, Jane

AU - Schroeder, Audrey

AU - Pan, Vivian

AU - Helbig, Katherine L.

AU - Friedman, Bethany

AU - Shinawi, Marwan

PY - 2015/8/11

Y1 - 2015/8/11

N2 - Background Rare de novo mutations have been implicated as a significant cause of idiopathic intellectual disability. Large deletions encompassing 10p11.23 have been implicated in developmental delay, behavioural abnormalities and dysmorphic features, but the genotype-phenotype correlation was not delineated. Mutations in WAC have been recently reported in large screening cohorts of patients with intellectual disability or autism, but no full phenotypic characterisation was described. Methods Clinical and molecular characterisation of six patients with loss-of-function WAC mutations identified by whole exome sequencing was performed. Clinical data were obtained by retrospective chart review, parental interviews, direct patient interaction and formal neuropsychological evaluation. Results Five heterozygous de novo WAC mutations were identified in six patients. Three of the mutations were nonsense, and two were frameshift; all are predicted to cause loss of function either through nonsense-mediated mRNA decay or protein truncation. Clinical findings included developmental delay (6/6), hypotonia (6/6), behavioural problems (5/6), eye abnormalities (5/6), constipation (5/6), feeding difficulties (4/6), seizures (2/6) and sleep problems (2/6). All patients exhibited common dysmorphic features, including broad/prominent forehead, synophrys and/or bushy eyebrows, depressed nasal bridge and bulbous nasal tip. Posteriorly rotated ears, hirsutism, deep-set eyes, thin upper lip, inverted nipples, hearing loss and branchial cleft anomalies were also noted. Conclusions Our case series show that loss-of-function mutations in WAC cause a recognisable genetic syndrome characterised by a neurocognitive phenotype and facial dysmorphism. Our data highly suggest that WAC haploinsufficiency is responsible for most of the phenotypic features associated with deletions encompassing 10p11.23.

AB - Background Rare de novo mutations have been implicated as a significant cause of idiopathic intellectual disability. Large deletions encompassing 10p11.23 have been implicated in developmental delay, behavioural abnormalities and dysmorphic features, but the genotype-phenotype correlation was not delineated. Mutations in WAC have been recently reported in large screening cohorts of patients with intellectual disability or autism, but no full phenotypic characterisation was described. Methods Clinical and molecular characterisation of six patients with loss-of-function WAC mutations identified by whole exome sequencing was performed. Clinical data were obtained by retrospective chart review, parental interviews, direct patient interaction and formal neuropsychological evaluation. Results Five heterozygous de novo WAC mutations were identified in six patients. Three of the mutations were nonsense, and two were frameshift; all are predicted to cause loss of function either through nonsense-mediated mRNA decay or protein truncation. Clinical findings included developmental delay (6/6), hypotonia (6/6), behavioural problems (5/6), eye abnormalities (5/6), constipation (5/6), feeding difficulties (4/6), seizures (2/6) and sleep problems (2/6). All patients exhibited common dysmorphic features, including broad/prominent forehead, synophrys and/or bushy eyebrows, depressed nasal bridge and bulbous nasal tip. Posteriorly rotated ears, hirsutism, deep-set eyes, thin upper lip, inverted nipples, hearing loss and branchial cleft anomalies were also noted. Conclusions Our case series show that loss-of-function mutations in WAC cause a recognisable genetic syndrome characterised by a neurocognitive phenotype and facial dysmorphism. Our data highly suggest that WAC haploinsufficiency is responsible for most of the phenotypic features associated with deletions encompassing 10p11.23.

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WAC loss-of-function mutations cause a recognisable syndrome characterised by dysmorphic features, developmental delay and hypotonia and recapitulate 10p11.23 microdeletion syndrome

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