FARP‐1 deletion is associated with lack of response to autism treatment by early start denver model in a multiplex family

Francesca Cucinotta; Arianna Ricciardello; Laura Turriziani; Giorgia Calabrese; Marilena Briguglio; Maria Boncoddo; Fabiana Bellomo; Pasquale Tomaiuolo; Silvia Martines; Marianna Bruschetta; Francesca La Fauci Belponer; Tiziana Di Bella; Costanza Colombi; Marco Baccarin; Chiara Picinelli; Paola Castronovo; Carla Lintas; Roberto Sacco; Thomas Biederer; Barbara Kellam; Stephen W. Scherer; Antonio M. Persico

doi:10.1002/mgg3.1373

Molecular Genetics & Genomic Medicine (Sep 2020)

FARP‐1 deletion is associated with lack of response to autism treatment by early start denver model in a multiplex family

Francesca Cucinotta,
Arianna Ricciardello,
Laura Turriziani,
Giorgia Calabrese,
Marilena Briguglio,
Maria Boncoddo,
Fabiana Bellomo,
Pasquale Tomaiuolo,
Silvia Martines,
Marianna Bruschetta,
Francesca La Fauci Belponer,
Tiziana Di Bella,
Costanza Colombi,
Marco Baccarin,
Chiara Picinelli,
Paola Castronovo,
Carla Lintas,
Roberto Sacco,
Thomas Biederer,
Barbara Kellam,
Stephen W. Scherer,
Antonio M. Persico

Affiliations

Francesca Cucinotta: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Arianna Ricciardello: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Laura Turriziani: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Giorgia Calabrese: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Marilena Briguglio: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Maria Boncoddo: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Fabiana Bellomo: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Pasquale Tomaiuolo: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Silvia Martines: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Marianna Bruschetta: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Francesca La Fauci Belponer: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Tiziana Di Bella: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy
Costanza Colombi: Department of Psychiatry University of Michigan Ann Arbor MI USA
Marco Baccarin: Mafalda Luce Center for Pervasive Developmental Disorders Milan Italy
Chiara Picinelli: Mafalda Luce Center for Pervasive Developmental Disorders Milan Italy
Paola Castronovo: Mafalda Luce Center for Pervasive Developmental Disorders Milan Italy
Carla Lintas: Service for Neurodevelopmental Disorders & Laboratory of Molecular Psychiatry and Neurogenetics University “Campus Bio‐Medico” Rome Italy
Roberto Sacco: Service for Neurodevelopmental Disorders & Laboratory of Molecular Psychiatry and Neurogenetics University “Campus Bio‐Medico” Rome Italy
Thomas Biederer: Department of Neurology Yale University School of Medicine New Haven CT USA
Barbara Kellam: Genetics & Genome Biology Program Toronto Canada
Stephen W. Scherer: Genetics & Genome Biology Program Toronto Canada
Antonio M. Persico: Interdepartmental Program "Autism 0‐90" "G. Martino" University Hospital of Messina Messina Italy

DOI: https://doi.org/10.1002/mgg3.1373
Journal volume & issue: Vol. 8, no. 9
pp. n/a – n/a

Abstract

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Abstract Background Children with autism spectrum disorder (ASD) display impressive clinical heterogeneity, also involving treatment response. Genetic variants can contribute to explain this large interindividual phenotypic variability. Methods Array‐CGH (a‐CGH) and whole genome sequencing (WGS) were performed on a multiplex family with two small children diagnosed with ASD at 17 and 18 months of age. Both brothers received the same naturalistic intervention for one year according to the Early Start Denver Model (ESDM), applied by the same therapists, yielding dramatically different treatment outcomes. Results The older sibling came out of the autism spectrum, while the younger sibling displayed very little, in any, improvement. This boy was subsequently treated applying a structured Early Intensive Behavioral Intervention paired with Augmentative Alternative Communication, which yielded a partial response within another year. The ESDM nonresponsive child carries a novel maternally inherited 65 Kb deletion at chr. 13q32.2 spanning FARP1. Farp1 is a synaptic scaffolding protein, which plays a significant role in neural plasticity. Conclusion These results represent a paradigmatic example of the heuristic potential of genetic markers in predicting treatment response and possibly in supporting the targeted prescription of specific early intervention approaches.

Published in Molecular Genetics & Genomic Medicine

ISSN: 2324-9269 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Science: Biology (General): Genetics
Website: https://onlinelibrary.wiley.com/journal/23249269

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