The Cognitive and Behavioral Phenotype of the 16p11.2 Deletion in a Clinically Ascertained Population

Hanson, Ellen; Bernier, Raphael; Porche, Ken; Jackson, Frank I.; Goin‐Kochel, Robin P.; Snyder, LeeAnne Green; Snow, Anne; Wallace, Arianne S.; Campe, Katherine L.; Zhang, Yuan; Chen, Qixuan; D’Angelo, Debra; Moreno-De-Luca, Andrés; Orr, Patrick T.; Boomer, K. B.; Evans, David W.; Kanne, Stephen M.; Berry, Leandra N.; Miller, Fiona K.; Olson, Jennifer; Sherr, Elliot; Martin, Christa Lese; Ledbetter, David H.; Spiro, John E.; Chung, Wendy K.

doi:10.1016/j.biopsych.2014.04.021

Cited by 213 publications

(230 citation statements)

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“…A good example of this is that reciprocal deletions and duplications of »600kb region at 16p11.2 are strongly associated with behavioral disorders, cognitive deficits and brain volume. 16p11.2 deletions are associated with speech/language and motor deficits, intellectual impairment, restrictive and repetitive behavior and macrocephaly, 28,29 whereas duplications are associated with ADHD, schizophrenia and microcephaly. 28,30 Decreased neurogenesis in the Ulk4 mutants has provided a cellular mechanism for its association with neurodevelopmental disorders.…”

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confidence: 99%

Multiple roles of Ulk4 in neurogenesis and brain function

Liu

O’Brien

et al. 2017

Neurogenesis

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confidence: 99%

Multiple roles of Ulk4 in neurogenesis and brain function

Liu

O’Brien

et al. 2017

Neurogenesis

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“…Contextual and cued fear conditioning were normal in +/2. These cognitive phenotypes may be relevant to some aspects of cognitive impairments in humans with 16p11.2 deletion, and support the use of 16p11.2+/2 mice as a model system for discovering treatments for cognitive impairments in 16p11.2 deletion syndrome.Recurrent heterozygous deletions of a 600-kb segment on human chromosome 16 is found in 0.4% of individuals with intellectual disability (Bijlsma et al 2009;Hanson et al 2015) and 0.6% of individuals with autism (Marshall et al 2008;Weiss et al 2008;Walsh and Bracken 2011). 16p11.2 deletion syndrome presents with a range of mild-to-severe cognitive impairments, with IQ scores averaging 2 SDs lower than controls, and a confirmed diagnosis of autism in 15% of affected individuals (Hanson et al…”

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16p11.2 Deletion mice display cognitive deficits in touchscreen learning and novelty recognition tasks

et al. 2015

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Chromosomal 16p11.2 deletion syndrome frequently presents with intellectual disabilities, speech delays, and autism. Here we investigated the Dolmetsch line of 16p11.2 heterozygous (+/2) mice on a range of cognitive tasks with different neuroanatomical substrates. Robust novel object recognition deficits were replicated in two cohorts of 16p11.2+/2 mice, confirming previous findings. A similarly robust deficit in object location memory was discovered in +/2, indicating impaired spatial novelty recognition. Generalizability of novelty recognition deficits in +/2 mice extended to preference for social novelty. Robust learning deficits and cognitive inflexibility were detected using Bussey-Saksida touchscreen operant chambers. During acquisition of pairwise visual discrimination, +/2 mice required significantly more training trials to reach criterion than wild-type littermates (+/+), and made more errors and correction errors than +/+. In the reversal phase, all +/+ reached criterion, whereas most +/2 failed to reach criterion by the 30-d cutoff. Contextual and cued fear conditioning were normal in +/2. These cognitive phenotypes may be relevant to some aspects of cognitive impairments in humans with 16p11.2 deletion, and support the use of 16p11.2+/2 mice as a model system for discovering treatments for cognitive impairments in 16p11.2 deletion syndrome.Recurrent heterozygous deletions of a 600-kb segment on human chromosome 16 is found in 0.4% of individuals with intellectual disability (Bijlsma et al. 2009;Hanson et al. 2015) and 0.6% of individuals with autism (Marshall et al. 2008;Weiss et al. 2008;Walsh and Bracken 2011). 16p11.2 deletion syndrome presents with a range of mild-to-severe cognitive impairments, with IQ scores averaging 2 SDs lower than controls, and a confirmed diagnosis of autism in 15% of affected individuals (Hanson et al.

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“…This 593-kb segment encompasses 25 genes and accounts for approximately 1% of cases of ASD [98,102]. Both deletions and duplications are associated with language delays, ASD, behavioral problems, congenital anomalies, and seizures [129][130][131], although the deletion may appear more commonly in autism [102,132], and the duplication appears to be more common in schizophrenia [112]. Contrasting phenotypes are observed: deletions are associated with increased brain volume/macrocephaly and increased body mass index/obesity, while duplications are associated with decreased brain volume/microcephaly and decreased body mass index [129,133,134].…”

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confidence: 99%

Discovery of Rare Mutations in Autism: Elucidating Neurodevelopmental Mechanisms

et al. 2015

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Autism spectrum disorder (ASD) is a group of highly genetic neurodevelopmental disorders characterized by language, social, cognitive, and behavioral abnormalities. ASD is a complex disorder with a heterogeneous etiology. The genetic architecture of autism is such that a variety of different rare mutations have been discovered, including rare monogenic conditions that involve autistic symptoms. Also, de novo copy number variants and single nucleotide variants contribute to disease susceptibility. Finally, autosomal recessive loci are contributing to our understanding of inherited factors. We will review the progress that the field has made in the discovery of these rare genetic variants in autism. We argue that mutation discovery of this sort offers an important opportunity to identify neurodevelopmental mechanisms in disease. The hope is that these mechanisms will show some degree of convergence that may be amenable to treatment intervention.

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The Cognitive and Behavioral Phenotype of the 16p11.2 Deletion in a Clinically Ascertained Population

Cited by 213 publications

References 45 publications

Multiple roles of Ulk4 in neurogenesis and brain function

Multiple roles of Ulk4 in neurogenesis and brain function

16p11.2 Deletion mice display cognitive deficits in touchscreen learning and novelty recognition tasks

Discovery of Rare Mutations in Autism: Elucidating Neurodevelopmental Mechanisms

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