Prader-Willi syndrome: intellectual abilities and behavioural features by genetic subtype
Prader-Willi syndrome: intellectual abilities and behavioural features by genetic subtype
Background: Studies of chromosome 15 abnormality have implicated over-expression of paternally imprinted genes in the 15q11–13 region in the aetiology of autism. To test this hypothesis we compared individuals with Prader-Willi syndrome (PWS) due to uniparental disomy (UPD – where paternally imprinted genes are over-expressed) to individuals with the 15q11–13 deletion form of the syndrome (where paternally imprinted genes are not over-expressed). We also tested reports that PWS cases due to the larger type I (TI) form of deletion show differences to cases with the smaller type II (TII) deletion.
Method: Ninety-six individuals with PWS were recruited from genetic centres and the PWS association. Forty-nine individuals were confirmed as having maternal UPD of chromosome 15 and were age and sex matched to 47 individuals with a deletion involving 15q11–13 (32 had the shorter (T II) deletion, and 14 had the longer (TI) deletion). Behavioural assessments were carried out blind to genetic status, using the Autism Diagnostic Observation Schedule (ADOS), the Autism Diagnostic Interview (ADI), the Autism Screening Questionnaire (ASQ), the Children's Yale-Brown Obsessive-Compulsive Scale (CY-BOCS), the Vineland Adaptive Behaviour Scales (VABS), and measurements of intellectual ability, including the Wechsler and Mullen Scales and Raven's Matrices.
Results: UPD cases exhibited significantly more autistic-like impairments in reciprocal social interaction on questionnaire, interview and standardised observational measures. Comparison of TI and TII deletion cases revealed few differences, but ability levels tended to be lower in the TI deletion cases.
Conclusions: Findings from a large study comparing deletion and UPD forms of Prader-Willi syndrome were consistent with other evidence in indicating that paternally imprinted genes in the 15q11–13 region constitute a genetic risk factor for aspects of autistic symptomatology. These genes may therefore play a role in the aetiology of autism. By contrast with another report, there was no clear-cut relationship between the size of the deletion and the form of cognitive and behavioural phenotype.
1089-1096
Milner, Katja M.
3c868f73-2778-44b0-a87d-963c2dfd9c84
Craig, Ellen E.
f33f423e-3d96-49f7-b5d7-86e10aa2727d
Thompson, Russell J.
4f73d649-4980-45c7-9c05-0090683ebb20
Veltman, Marijcke W.M.
c7058408-7866-49ce-9807-e1b3eecfb4a6
Thomas, N. Simon
1a601957-288d-4f12-a9f7-4f4279b7f9b3
Roberts, Sian
baaf7d9f-4a23-493f-858b-5a61c09ba7e0
Bellamy, Margaret
48894d5e-2d9e-4ad3-8ce7-fadc3d5821e9
Curran, Sarah R.
6abd872b-d266-430f-b6e7-18fc9ee206f5
Sporikou, Caroline M.J.
dadbc9ce-73b3-4d37-9924-233e3b58a1bd
Bolton, Patrick F.
2f8d64d8-1977-4020-9add-d571cb96f826
2005
Milner, Katja M.
3c868f73-2778-44b0-a87d-963c2dfd9c84
Craig, Ellen E.
f33f423e-3d96-49f7-b5d7-86e10aa2727d
Thompson, Russell J.
4f73d649-4980-45c7-9c05-0090683ebb20
Veltman, Marijcke W.M.
c7058408-7866-49ce-9807-e1b3eecfb4a6
Thomas, N. Simon
1a601957-288d-4f12-a9f7-4f4279b7f9b3
Roberts, Sian
baaf7d9f-4a23-493f-858b-5a61c09ba7e0
Bellamy, Margaret
48894d5e-2d9e-4ad3-8ce7-fadc3d5821e9
Curran, Sarah R.
6abd872b-d266-430f-b6e7-18fc9ee206f5
Sporikou, Caroline M.J.
dadbc9ce-73b3-4d37-9924-233e3b58a1bd
Bolton, Patrick F.
2f8d64d8-1977-4020-9add-d571cb96f826
Milner, Katja M., Craig, Ellen E., Thompson, Russell J., Veltman, Marijcke W.M., Thomas, N. Simon, Roberts, Sian, Bellamy, Margaret, Curran, Sarah R., Sporikou, Caroline M.J. and Bolton, Patrick F.
(2005)
Prader-Willi syndrome: intellectual abilities and behavioural features by genetic subtype.
Journal of Child Psychology and Psychiatry, 46 (10), .
(doi:10.1111/j.1469-7610.2005.01520.x).
Abstract
Background: Studies of chromosome 15 abnormality have implicated over-expression of paternally imprinted genes in the 15q11–13 region in the aetiology of autism. To test this hypothesis we compared individuals with Prader-Willi syndrome (PWS) due to uniparental disomy (UPD – where paternally imprinted genes are over-expressed) to individuals with the 15q11–13 deletion form of the syndrome (where paternally imprinted genes are not over-expressed). We also tested reports that PWS cases due to the larger type I (TI) form of deletion show differences to cases with the smaller type II (TII) deletion.
Method: Ninety-six individuals with PWS were recruited from genetic centres and the PWS association. Forty-nine individuals were confirmed as having maternal UPD of chromosome 15 and were age and sex matched to 47 individuals with a deletion involving 15q11–13 (32 had the shorter (T II) deletion, and 14 had the longer (TI) deletion). Behavioural assessments were carried out blind to genetic status, using the Autism Diagnostic Observation Schedule (ADOS), the Autism Diagnostic Interview (ADI), the Autism Screening Questionnaire (ASQ), the Children's Yale-Brown Obsessive-Compulsive Scale (CY-BOCS), the Vineland Adaptive Behaviour Scales (VABS), and measurements of intellectual ability, including the Wechsler and Mullen Scales and Raven's Matrices.
Results: UPD cases exhibited significantly more autistic-like impairments in reciprocal social interaction on questionnaire, interview and standardised observational measures. Comparison of TI and TII deletion cases revealed few differences, but ability levels tended to be lower in the TI deletion cases.
Conclusions: Findings from a large study comparing deletion and UPD forms of Prader-Willi syndrome were consistent with other evidence in indicating that paternally imprinted genes in the 15q11–13 region constitute a genetic risk factor for aspects of autistic symptomatology. These genes may therefore play a role in the aetiology of autism. By contrast with another report, there was no clear-cut relationship between the size of the deletion and the form of cognitive and behavioural phenotype.
This record has no associated files available for download.
More information
Published date: 2005
Identifiers
Local EPrints ID: 24866
URI: http://eprints.soton.ac.uk/id/eprint/24866
ISSN: 0021-9630
PURE UUID: 923d0d94-42a4-49a4-b599-2ecae5b1fdca
Catalogue record
Date deposited: 03 Apr 2006
Last modified: 15 Mar 2024 06:59
Export record
Altmetrics
Contributors
Author:
Katja M. Milner
Author:
Ellen E. Craig
Author:
Russell J. Thompson
Author:
Marijcke W.M. Veltman
Author:
N. Simon Thomas
Author:
Sian Roberts
Author:
Margaret Bellamy
Author:
Sarah R. Curran
Author:
Caroline M.J. Sporikou
Author:
Patrick F. Bolton
Download statistics
Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.
View more statistics