An integrated analysis of rare CNV and exome variation in Autism Spectrum Disorder using the Infinium PsychArray

Bacchelli, Elena; Cameli, Cinzia; Viggiano, Marta; Igliozzi, Roberta; Mancini, Alice; Tancredi, Raffaella; Battaglia, Agatino; Maestrini, Elena

doi:10.1038/s41598-020-59922-3

Cited by 51 publications

(50 citation statements)

References 58 publications

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“…ASD refers to a broad range of highly complex and heterogeneous neuropsychiatric conditions characterized by challenges with social skills, difficulty in communication and interaction with others, restricted interests, and repetitive behaviors. ADS individuals often suffer from other co-occurring conditions such as intellectual disability (ID), epilepsy, sleep disorders, motor deficits, and attention-deficit hyperactivity disorder (ADHD) [ 40 ]. Many of these ASD co-morbidities overlap with clinical features displayed by individuals affected with the above described WWOX related CNS disorders.…”

Section: Wwox-associated Cns Disordersmentioning

confidence: 99%

WWOX Loss of Function in Neurodevelopmental and Neurodegenerative Disorders

Aldaz

Hussain

2020

IJMS

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The WWOX gene was initially discovered as a putative tumor suppressor. More recently, its association with multiple central nervous system (CNS) pathologies has been recognized. WWOX biallelic germline pathogenic variants have been implicated in spinocerebellar ataxia type 12 (SCAR12; MIM:614322) and in early infantile epileptic encephalopathy (EIEE28; MIM:616211). WWOX germline copy number variants have also been associated with autism spectrum disorder (ASD). All identified germline genomic variants lead to partial or complete loss of WWOX function. Importantly, large-scale genome-wide association studies have also identified WWOX as a risk gene for common neurodegenerative conditions such as Alzheimer’s disease (AD) and multiple sclerosis (MS). Thus, the spectrum of CNS disorders associated with WWOX is broad and heterogeneous, and there is little understanding of potential mechanisms at play. Exploration of gene expression databases indicates that WWOX expression is comparatively higher in the human cerebellar cortex than in other CNS structures. However, RNA in-situ hybridization data from the Allen Mouse Brain Atlas show that specific regions of the basolateral amygdala (BLA), the medial entorhinal cortex (EC), and deep layers of the isocortex can be singled out as brain regions with specific higher levels of Wwox expression. These observations are in close agreement with single-cell RNA-seq data which indicate that neurons from the medial entorhinal cortex, Layer 5 from the frontal cortex as well as GABAergic basket cells and granule cells from cerebellar cortex are the specific neuronal subtypes that display the highest Wwox expression levels. Importantly, the brain regions and cell types in which WWOX is most abundantly expressed, such as the EC and BLA, are intimately linked to pathologies and syndromic conditions in turn associated with this gene, such as epilepsy, intellectual disability, ASD, and AD. Higher Wwox expression in interneurons and granule cells from cerebellum points to a direct link to the described cerebellar ataxia in cases of WWOX loss of function. We now know that total or partial impairment of WWOX function results in a wide and heterogeneous variety of neurodegenerative conditions for which the specific molecular mechanisms remain to be deciphered. Nevertheless, these observations indicate an important functional role for WWOX in normal development and function of the CNS. Evidence also indicates that disruption of WWOX expression at the gene or protein level in CNS has significant deleterious consequences.

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Section: Wwox-associated Cns Disordersmentioning

confidence: 99%

WWOX Loss of Function in Neurodevelopmental and Neurodegenerative Disorders

Aldaz

Hussain

2020

IJMS

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“…In addition to the fact that only sometimes the so-called common sequence variants (meaning that the minor allele frequency [MAF] is greater than 5% in the population) or their combinations are implied in the development of ASD, more important for the pathogenesis of ASD are rare (MAF < 1%) or very rare (MAF < 0.1%) single nucleotide variants (SNVs), as well as rare variations in the number of copies (copy number variation, CNV), especially deletions, but also duplications [ 148 , 149 , 150 , 151 , 152 ]. As of April 20, 2020, the Simons Foundation Autism Research Initiative (SFARI), the largest international database for ASD researchers, had a total of 835 genes whose changes or variants are associated with ASD ( ).…”

Section: Autism Spectrum Disorder (Asd)mentioning

confidence: 99%

Molecules, Mechanisms, and Disorders of Self-Domestication: Keys for Understanding Emotional and Social Communication from an Evolutionary Perspective

et al. 2020

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The neural crest hypothesis states that the phenotypic features of the domestication syndrome are due to a reduced number or disruption of neural crest cells (NCCs) migration, as these cells differentiate at their final destinations and proliferate into different tissues whose activity is reduced by domestication. Comparing the phenotypic characteristics of modern and prehistoric man, it is clear that during their recent evolutionary past, humans also went through a process of self-domestication with a simultaneous prolongation of the period of socialization. This has led to the development of social abilities and skills, especially language, as well as neoteny. Disorders of neural crest cell development and migration lead to many different conditions such as Waardenburg syndrome, Hirschsprung disease, fetal alcohol syndrome, DiGeorge and Treacher-Collins syndrome, for which the mechanisms are already relatively well-known. However, for others, such as Williams-Beuren syndrome and schizophrenia that have the characteristics of hyperdomestication, and autism spectrum disorders, and 7dupASD syndrome that have the characteristics of hypodomestication, much less is known. Thus, deciphering the biological determinants of disordered self-domestication has great potential for elucidating the normal and disturbed ontogenesis of humans, as well as for the understanding of evolution of mammals in general.

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“…For example, inCNV can be used to find de novo CNVs of a sample within the same family. 4 , 35 To this end, users can filter out common or known CNVs and explore whether the remaining CNVs of the proband are different from their parents. Moreover, we can use inCNV to determine whether the sample has potential to develop a specific disease by the following steps: (1) Integrate the CNVs of the sample of interest with the CNVs of a sample set of the same disease; (2) Search for genes that are specifically related to the disease; (3) Search for the sample of interest; (4) Sort the results by the number of overlapping samples.…”

Section: Resultsmentioning

confidence: 99%

“…In particular, the study of CNV on whole-exome sequencing (WES) is much more popular 1 and affordable 2 than the study on whole-genome sequencing (WGS). The study of CNVs on WES provides insights into human genome diversity and predisposition to diseases, 3 such as autism, 4 schizophrenia, 5 type-2 diabetes, 6 congenital heart disease (CHD), 7 non-syndromic hearing loss 8 , 9 and inherited retinal degenerations, 10 among others. Nevertheless, issues with the accuracy and complexity of captured CNVs as well as their interpretation still exist.…”

Section: Introductionmentioning

confidence: 99%

inCNV: An Integrated Analysis Tool for Copy Number Variation on Whole Exome Sequencing

Chanwigoon

Piwluang

Wichadakul

2020

Evol Bioinform Online

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The detection of copy number variations (CNVs) on whole-exome sequencing (WES) represents a cost-effective technique for the study of genetic variants. This approach, however, has encountered an obstacle with high false-positive rates due to biases from exome sequencing capture kits and GC contents. Although plenty of CNV detection tools have been developed, they do not perform well with all types of CNVs. In addition, most tools lack features of genetic annotation, CNV visualization, and flexible installation, requiring users to put much effort into CNV interpretation. Here, we present “inCNV,” a web-based application that can accept multiple CNV-tool results, then integrate and prioritize them with user-friendly interfaces. This application helps users analyze the importance of called CNVs by generating CNV annotations from Ensembl, Database of Genomic Variants (DGV), ClinVar, and Online Mendelian Inheritance in Man (OMIM). Moreover, users can select and export CNVs of interest including their flanking sequences for primer design and experimental verification. We demonstrated how inCNV could help users filter and narrow down the called CNVs to a potentially novel CNV, a common CNV within a group of samples of the same disease, or a de novo CNV of a sample within the same family. Besides, we have provided in CNV as a docker image for ease of installation ( https://github.com/saowwapark/inCNV ).

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An integrated analysis of rare CNV and exome variation in Autism Spectrum Disorder using the Infinium PsychArray

Cited by 51 publications

References 58 publications

WWOX Loss of Function in Neurodevelopmental and Neurodegenerative Disorders

WWOX Loss of Function in Neurodevelopmental and Neurodegenerative Disorders

Molecules, Mechanisms, and Disorders of Self-Domestication: Keys for Understanding Emotional and Social Communication from an Evolutionary Perspective

inCNV: An Integrated Analysis Tool for Copy Number Variation on Whole Exome Sequencing

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