Autism Clinical Trial
Official title:
Neuropsychopathological Study of Autism: From Clinical, Neurocognitive, to Genetic Studies and Animal Models
Autism or autism spectrum disorder (ASD) is a relatively common (0.3% in Taiwan), multi-factorial, genetically and clinically heterogeneous, childhood-onset neurodevelopmental disorder. Due to its high heritability and severe long-term impairment without available laboratory diagnosis, effective prevention or treatment, this disastrous disease has been prioritized for molecular genetic studies. Recent CNVs investigation to identify rare variants and GWA study with endophenotype approaches are promising strategies to identify common genetic variants. In addition to intermediate phenotypes such as head circumstance, speech delay, social impairments and stereotyped behaviors, evidence has demonstrated that neuropsychology and neuroimages may be useful endophenotypes for autism. Dlgap2, Fbxo25, and Arhgef10 knoutout mice generated from our previous CNV results will be characterized.
The specific aims of the study aree:
1. To collect complete environmental, developmental, clinical, neuropsychological, and
genetic data of 350 probands with autism (800 in total, 450 from [96HD008]) and their
families;
2. To re-sequence promoter region, all the exons, and the 3'UTR region of the DLGAP2,
CLN8, ARHGEF10, FBXO25, and GABRB3 genes (one gene per year);
3. To conduct fine-mapping and replication studies for selected candidate genes from GWA
study[96HD008];
4. To validate social impairment and speech delay as intermediate phenotypes and the
executive functions as effective cognitive endophenotypes by first demonstrating the
differences in these measures among probands, their unaffected siblings and
neurotypicals, followed by different genetic risks (e.g., neurexin, neuroligin,
CNTNAP2, SHANK3, MET, PTEN, WNT2, FOXP2, DLGAP2, CLN8, ARHGEF10, FBXO25, and GABRB3);
5. To validate the structural and functional connectivity as effective imaging
endophenotypes by demonstrating the differences between probands with autism, their
siblings, and matched neurotypicals; and
6. To characterize the phenotypes of and to explore the possible function of other
autism-related genes found by using GWAS, and to explore the possible drug targets for
the treatment for Dlgap2, Fbxo25, and Arhgef10 mutant mice.
The investigators will recruit 350 probands with clinical diagnosis of autism confirmed by
the ADI-R and ADOS, and their families. The probands and their siblings will also be
assessed for other psychiatric disorders (K-SADS-E); autistic symptom dimensions (SRS, SCQ,
CAST, ABC), other behavioral symptoms (CBCL, SNAP-IV), and perinatal/environmental risk
factors. The direct tests include intelligence (CPM/SPM, WISC-III, WPPSI-R) and
neuropsychological tests (CPT, WCST, CANTAB). The parents will be assessed for DSM-IV
psychiatric disorders (ASRI-4) and autistic features (AQ, SRS). The investigators will
collect blood samples from all the subjects. Probands with previous CNVs findings (n = 20)
and high-functioning autism (n=30) will receive the MRI assessments (Diffusion Spectrum
Imaging, resting-state fMRI) as compared to 50 age-, sex-, and handedness-matched
neurotypicals.
The investigators will (1) characterize the behavioral, structural, electrophysiological and
biochemical phenotypes of Dlgap2, and Arhgef10 mice at 4 weeks, 8 weeks, 12 weeks and 16
weeks of ages; (2) explore the possible function of other autism-related genes found by GWAS
analysis; and (3) explore the possible drug targets for the treatment of autism from KO
mice. While the potential target is recognized, existing compounds of this target can be
tested.
The investigators anticipate to establishing a representative cohort of 800 patients with
autism and their families from this study and [96HD008] with comprehensive clinical and
genetic data. This well-characterized cohort will contribute to validation of intermediate
phenotypes and cognitive and imaging endophenotypes for autism in this study, and will be
used to search for rare variants by CNVs analysis and common variants by GWAS analysis in
future study, and will pave the way to have 2-3 lines of well-characterized transgenic
animal models of autism (e.g., Dlgap2). In addition, a wealth of data from this cohort will
benefit to current and future investigation on autism and will be the basis for future
international collaboration. The investigators also anticipated to publication of 20 SCI
papers (4 per year) and presentation of our work in peer-reviewed scientific conferences by
more than 40 posters or oral communications.
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Observational Model: Family-Based
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