Characterization of a Clinically and Biologically Defined Subgroup of Patients with Autism Spectrum Disorder and Identification of a Tailored Combination Treatment
Laura Pérez-Cano,
Luigi Boccuto,
Francesco Sirci,
Jose Manuel Hidalgo,
Samuel Valentini,
Mattia Bosio,
Xavier Liogier D’Ardhuy,
Cindy Skinner,
Lauren Cascio,
Sujata Srikanth,
Kelly Jones,
Caroline B. Buchanan,
Steven A. Skinner,
Baltazar Gomez-Mancilla,
Jean-Marc Hyvelin,
Emre Guney,
Lynn Durham
Affiliations
Laura Pérez-Cano
Discovery and Data Science (DDS) Unit, STALICLA SL, Moll de Barcelona, s/n, Edif Este, 08039 Barcelona, Spain
Luigi Boccuto
JC Self Research Institute, Greenwood Genetic Center, Greenwood, SC 29649, USA
Francesco Sirci
Discovery and Data Science (DDS) Unit, STALICLA SL, Moll de Barcelona, s/n, Edif Este, 08039 Barcelona, Spain
Jose Manuel Hidalgo
Discovery and Data Science (DDS) Unit, STALICLA SL, Moll de Barcelona, s/n, Edif Este, 08039 Barcelona, Spain
Samuel Valentini
Discovery and Data Science (DDS) Unit, STALICLA SL, Moll de Barcelona, s/n, Edif Este, 08039 Barcelona, Spain
Mattia Bosio
Discovery and Data Science (DDS) Unit, STALICLA SL, Moll de Barcelona, s/n, Edif Este, 08039 Barcelona, Spain
Xavier Liogier D’Ardhuy
Drug Development Unit (DDU), STALICLA SA, Avenue de Sécheron 15, 1202 Geneva, Switzerland
Cindy Skinner
JC Self Research Institute, Greenwood Genetic Center, Greenwood, SC 29649, USA
Lauren Cascio
JC Self Research Institute, Greenwood Genetic Center, Greenwood, SC 29649, USA
Sujata Srikanth
JC Self Research Institute, Greenwood Genetic Center, Greenwood, SC 29649, USA
Kelly Jones
JC Self Research Institute, Greenwood Genetic Center, Greenwood, SC 29649, USA
Caroline B. Buchanan
JC Self Research Institute, Greenwood Genetic Center, Greenwood, SC 29649, USA
Steven A. Skinner
JC Self Research Institute, Greenwood Genetic Center, Greenwood, SC 29649, USA
Baltazar Gomez-Mancilla
Drug Development Unit (DDU), STALICLA SA, Avenue de Sécheron 15, 1202 Geneva, Switzerland
Jean-Marc Hyvelin
Drug Development Unit (DDU), STALICLA SA, Avenue de Sécheron 15, 1202 Geneva, Switzerland
Emre Guney
Discovery and Data Science (DDS) Unit, STALICLA SL, Moll de Barcelona, s/n, Edif Este, 08039 Barcelona, Spain
Lynn Durham
Discovery and Data Science (DDS) Unit, STALICLA SL, Moll de Barcelona, s/n, Edif Este, 08039 Barcelona, Spain
Autism spectrum disorder (ASD) is a heterogeneous group of neurodevelopmental disorders (NDDs) with a high unmet medical need. The diagnosis of ASD is currently based on behavior criteria, which overlooks the diversity of genetic, neurophysiological, and clinical manifestations. Failure to acknowledge such heterogeneity has hindered the development of efficient drug treatments for ASD and other NDDs. DEPI® (Databased Endophenotyping Patient Identification) is a systems biology, multi-omics, and machine learning-driven platform enabling the identification of subgroups of patients with NDDs and the development of patient-tailored treatments. In this study, we provide evidence for the validation of a first clinically and biologically defined subgroup of patients with ASD identified by DEPI, ASD Phenotype 1 (ASD-Phen1). Among 313 screened patients with idiopathic ASD, the prevalence of ASD-Phen1 was observed to be ~24% in 84 patients who qualified to be enrolled in the study. Metabolic and transcriptomic alterations differentiating patients with ASD-Phen1 were consistent with an over-activation of NF-κB and NRF2 transcription factors, as predicted by DEPI. Finally, the suitability of STP1 combination treatment to revert such observed molecular alterations in patients with ASD-Phen1 was determined. Overall, our results support the development of precision medicine-based treatments for patients diagnosed with ASD.
