A kinome-wide RNAi screen identifies ERK2 as a druggable regulator of Shank3 stability

Wang, Li; Adamski, Carolyn J.; Bondar, Vitaliy V.; Craigen, Evelyn; Collette, John R.; Pang, Kaifang; Han, Ki-Hoon; Jain, Antrix; Jung, Sung Yun; Liu, Zhandong; Sifers, Richard N.; Holder, J. Lloyd; Zoghbi, Huda Y.

doi:10.1038/s41380-018-0325-9

Cited by 23 publications

(22 citation statements)

References 33 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Studies in mice have shown that Shank3 is essential for proper synaptic function and mutations in this gene lead to impaired motor coordination, repetitive behavior and altered social interactions ( Uchino and Waga, 2015 ; Amal et al, 2018 ; Wang et al, 2019 ). At least five mutant Shank3 lines altering different regions of the protein have been created in mice ( Jiang and Ehlers, 2013 ).…”

Section: Knock-out Versus Knock-downmentioning

confidence: 99%

Using Zebrafish to Model Autism Spectrum Disorder: A Comparison of ASD Risk Genes Between Zebrafish and Their Mammalian Counterparts

Rea

Raay

2020

Front. Mol. Neurosci.

View full text Add to dashboard Cite

Autism spectrum disorders (ASDs) are a highly variable and complex set of neurological disorders that alter neurodevelopment and cognitive function, which usually presents with social and learning impairments accompanied with other comorbid symptoms like hypersensitivity or hyposensitivity, or repetitive behaviors. Autism can be caused by genetic and/or environmental factors and unraveling the etiology of ASD has proven challenging, especially given that different genetic mutations can cause both similar and different phenotypes that all fall within the autism spectrum. Furthermore, the list of ASD risk genes is ever increasing making it difficult to synthesize a common theme. The use of rodent models to enhance ASD research is invaluable and is beginning to unravel the underlying molecular mechanisms of this disease. Recently, zebrafish have been recognized as a useful model of neurodevelopmental disorders with regards to genetics, pharmacology and behavior and one of the main foundations supporting autism research (SFARI) recently identified 12 ASD risk genes with validated zebrafish mutant models. Here, we describe what is known about those 12 ASD risk genes in human, mice and zebrafish to better facilitate this research. We also describe several non-genetic models including pharmacological and gnotobiotic models that are used in zebrafish to study ASD.

show abstract

Section: Knock-out Versus Knock-downmentioning

confidence: 99%

Using Zebrafish to Model Autism Spectrum Disorder: A Comparison of ASD Risk Genes Between Zebrafish and Their Mammalian Counterparts

Rea

Raay

2020

Front. Mol. Neurosci.

View full text Add to dashboard Cite

show abstract

“…As SHANK3 is critically involved in regulating synaptic structure and function, neurons are sensitive to altered gene dosage, which has been pointed out by several studies (Bozdagi et al, 2010; Durand et al, 2007; Wang, Adamski, et al, 2019; Yi et al, 2016). Of note, albeit both mutations are located within the SPN domain, they had distinct effects on SHANK3 folding and residing time as well as localization at the synapse, suggesting that each point mutation might cause synaptic dysfunction by different mechanisms.…”

Section: Discussionmentioning

confidence: 96%

Autism associatedSHANK3missense point mutations impact conformational fluctuations and protein turnover at synapses

Bucher

Niebling

Han

et al. 2021

Preprint

View full text Add to dashboard Cite

Members of the SH3- and ankyrin-rich repeat (SHANK) protein family are considered as master scaffolds of the post-synaptic density of glutamatergic synapses. Several missense mutations within the canonical SHANK3 isoform have been proposed as causative for the development of autism spectrum disorders (ASDs). However, there is a surprising paucity of data linking missense mutation-induced changes in protein structure and dynamics to the occurrence of ASD-related synaptic phenotypes. In this work, we focus on two ASD-associated point mutations, both located within the same domain of SHANK3. In a proof-of-principle study we demonstrate that both mutant proteins show indeed distinct changes in secondary and tertiary structure as well as higher conformational fluctuations. Local and surprisingly also distal structural disturbances of protein folding result in altered synaptic targeting and changes of protein turnover at synaptic sites.

show abstract

“…Mutations in the SHANK3 gene have been associated with various brain disorders, including autism spectrum disorders (ASD), Phelan-McDermid Syndrome (PMS), schizophrenia, intellectual disability, and mania (Wilson et al, 2003; Gauthier et al, 2010; Bonaglia et al, 2011; Hamdan et al, 2011; Phelan and McDermid, 2012; Boccuto et al, 2013; Han et al, 2013; Guilmatre et al, 2014; Leblond et al, 2014; Cochoy et al, 2015). Mechanisms underlying the development of Shank3-related brain dysfunctions have been suggested through studies of a large number of Shank3 -mutant mice (Bozdagi et al, 2010; Peca et al, 2011; Wang X. et al, 2011; Yang et al, 2012; Han et al, 2013; Jiang and Ehlers, 2013; Kouser et al, 2013; Duffney et al, 2015; Lee et al, 2015; Sala et al, 2015; Speed et al, 2015; Jaramillo et al, 2016, 2017; Mei et al, 2016; Wang et al, 2016, 2019a,b; Zhou et al, 2016; Monteiro and Feng, 2017; Vicidomini et al, 2017; Bey et al, 2018; Drapeau et al, 2018; Qin et al, 2018; Yoo et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

Shank3 Exons 14–16 Deletion in Glutamatergic Neurons Leads to Social and Repetitive Behavioral Deficits Associated With Increased Cortical Layer 2/3 Neuronal Excitability

Yoo

Cho

Park

et al. 2019

Front. Cell. Neurosci.

View full text Add to dashboard Cite

Shank3, an abundant excitatory postsynaptic scaffolding protein, has been associated with multiple brain disorders, including autism spectrum disorders (ASD) and Phelan-McDermid syndrome (PMS). However, how cell type-specific Shank3 deletion affects disease-related neuronal and brain functions remains largely unclear. Here, we investigated the impacts of Shank3 deletion in glutamatergic neurons on synaptic and behavioral phenotypes in mice and compared results with those previously obtained from mice with global Shank3 mutation and GABAergic neuron-specific Shank3 mutation. Neuronal excitability was abnormally increased in layer 2/3 pyramidal neurons in the medial prefrontal cortex (mPFC) in mice with a glutamatergic Shank3 deletion, similar to results obtained in mice with a global Shank3 deletion. In addition, excitatory synaptic transmission was abnormally increased in layer 2/3 neurons in mice with a global, but not a glutamatergic, Shank3 deletion, suggesting that Shank3 in glutamatergic neurons are important for the increased neuronal excitability, but not for the increased excitatory synaptic transmission. Neither excitatory nor inhibitory synaptic transmission was altered in the dorsal striatum of Shank3-deficient glutamatergic neurons, a finding that contrasts with the decreased excitatory synaptic transmission in global and Shank3-deficient GABAergic neurons. Behaviorally, glutamatergic Shank3-deficient mice displayed abnormally increased direct social interaction and repetitive self-grooming, similar to global and GABAergic Shank3-deficient mice. These results suggest that glutamatergic and GABAergic Shank3 deletions lead to distinct synaptic and neuronal changes in cortical layer 2/3 and dorsal striatal neurons, but cause similar social and repetitive behavioral abnormalities likely through distinct mechanisms.

show abstract

A kinome-wide RNAi screen identifies ERK2 as a druggable regulator of Shank3 stability

Cited by 23 publications

References 33 publications

Using Zebrafish to Model Autism Spectrum Disorder: A Comparison of ASD Risk Genes Between Zebrafish and Their Mammalian Counterparts

Using Zebrafish to Model Autism Spectrum Disorder: A Comparison of ASD Risk Genes Between Zebrafish and Their Mammalian Counterparts

Autism associatedSHANK3missense point mutations impact conformational fluctuations and protein turnover at synapses

Shank3 Exons 14–16 Deletion in Glutamatergic Neurons Leads to Social and Repetitive Behavioral Deficits Associated With Increased Cortical Layer 2/3 Neuronal Excitability

Contact Info

Product

Resources

About