Early identification and diagnosis of autism spectrum disorder (ASD) is necessary to promote access to early treatment. Despite the high incidence, in Italy it is estimated that 1 in 77 children (age 7-9 years) (Narzisi et al., 2018), the diagnosis and the choice of rehabilitation treatment for patients with Autism Spectrum Disorder (ASD) are still based on clinical observation. In the absence of targeted pharmacological therapies, early surveillance and evaluation aimed at timely intervention represent the only successful strategy to reduce the severity of symptoms (Palomo R et al., 2006) and improve the quality of life of children affected by ASD and their families, thus also leading to a reduction in costs for the National Health Service (Ganz ML. 2007). However, compared to the great advances in neuroscience, the clinical management of autistic individuals is seriously lagging behind, and the disorder is often diagnosed after 3-4 years of age despite the presence of deficits starting from the very first months of life (Zwaigenbaum L et al. al., 2013). The aim of this project is to bridge the gap between research and clinic, thanks to the convergence of multiple biological and clinical data.
The purpose of this project is to combine multiple biological levels of information and their matching with the clinical phenotype and personal/family anamnesis of the single individual. In fact, by stratifying multiple levels of biomarkers, including behavioral (eye tracking), clinical and neuropsychological variables, parameters taken from transcriptomics (RNAseq), the goal is to identify a panel of intermediate biomarkers capable of (a) distinguishing autistic subjects from typically developing brothers/sisters, (b) to distinguish autistic subjects from typically developing subjects, (c) to stratify autistic patients into a limited number of homogeneous subgroups by physiopathology, in order to allow personalized pharmacology and improve their management clinic.
Study Type
OBSERVATIONAL
Enrollment
28
Collection of saliva via swab for miRNA processing
Administration of eye-tracking session recording Saccadic Eye Movements, fixation duration and pupillary response.
Administration of neuropsychological tests and collected patient medical history
IRCCS Centro Neurolesi Bonino Pulejo
Messina, Italy
RECRUITINGSalivary miRNA profile
Measures of salivary miRNA profile - identify the microRNAs differentially expressed in patients with autism spectrum disorder compared to sibling and healthy controls.
Time frame: At time of enrollment
eye-gaze path characteristics - Saccadic Eye Movements
Saccadic eye movement assessments measure the speed and accuracy of a participant's saccadic eye movements in response to various stimuli.
Time frame: At time of enrollment
eye-gaze path characteristics - fixation time
Total fixation duration measurements in pre-selected areas (areas of interest)
Time frame: At time of enrollment
eye-gaze path characteristics - pupillary response
pupillary response measurements assess the changes of mean pupil diameters for the left and right eyes after exposition to pre-selected immages (areas of interest)
Time frame: At time of enrollment
Autism Diagnostic Observation Schedule 2 (ASD patients only)
Ados2 is a semi-structured, standardised assessment to measure autistic behaviors.
Time frame: At time of enrollment
Vineland Adaptive Behavior Scales (VABS) II (ASD patients only)
The VABS II is a standardized semi-structured interview to measure adaptive behavior.
Time frame: At time of enrollment
Intellectual Quotient (ASD patients only)
Intellectual quotient measured using one cognitive test per subject, chosen depending on age and language development (either Griffiths Developmental Rating Scales, Wechsler Intelligence Scale for Children - Fourth Edition, or Leiter III).
Time frame: At time of enrollment
IRCCS Centro Neurolesi Bonino Pulejo Bio-parco delle intelligenze e delle neuro-fragilità
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