Investigating social orienting in children with Phelan-McDermid syndrome and ‘idiopathic’ autism

San José Cáceres, Antonia, Wilkinson, Emma, Cooke, Jennifer, Baskett, Victoria, Blackmore, Charlotte, Crawley, Daisy Victoria, Durkin, Allison, Halpern, Danielle, Núñez, María, Siper, Page, Murphy, Declan G., Foss-Feig, Jennifer, Kolevzon, Alexander and Loth, Eva (2024) Investigating social orienting in children with Phelan-McDermid syndrome and ‘idiopathic’ autism. Journal of Neurodevelopmental Disorders, 16 (1): 64. pp. 1-11.
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Background: Phelan-McDermid syndrome (PMS) is a rare genetic syndrome characterized by developmental delay/intellectual disability, absent or delayed speech, physical dysmorphic features and high rates of autistic features. However, it is currently unknown whether people with PMS have similar neurocognitive atypicalities to those previously identified in idiopathic autism. Disruption in social orienting has previously been suggested as an early hallmark feature of idiopathic autism that impacts social learning and social interaction. Methods: This study used a semi-naturalistic task to explore orienting to social versus non-social stimuli and its relation to clinical features in individuals diagnosed with PMS, autism, and neurotypical children recruited in the United States and the United Kingdom. Results: At the group level, autistic and neurotypical children responded on average more often to social than non-social stimuli, while children with PMS responded similarly to both stimulus types. Both clinical groups responded significantly less often to social stimuli than neurotypical children. In addition, we found considerable variability in orienting responses within each group that were of clinical relevance. In the autism group, non-social orienting was associated with mental age, while in the PMS group social and non-social orienting were related to strength of autistic features. Conclusions: These findings do not support specific social motivation difficulties in either clinical group. Instead, they highlight the importance of exploring individual differences in orienting responses in Phelan-McDermid Syndrome in relation to autistic features. Trial registration: NA.


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