Regulation of Neuronal Gene Expression by Local Axonal Translation

Korsak, Lulu I T.; Mitchell, Molly E; Shepard, Katherine A.; Akins, Michael R.

doi:10.1007/s40142-016-0085-2

Cited by 24 publications

(21 citation statements)

References 91 publications

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“…Because neurons are so highly polarized, transport of mRNAs along the axon and dendrites to undergo local, on-site protein synthesis is key for maintaining proper structural and functional polarity (Bramham, 2008;Cioni et al, 2018;Rangaraju et al, 2017;Tom Dieck et al, 2014). In these subcompartments, FMRP and its homologs, the fragile X-related proteins FXR1P and FXR2P, assemble with other RNA-binding proteins and coding and noncoding RNAs to form large ribonucleoprotein particles or granules that tightly regulate mRNA transport, translation, stability, and degradation (Akins et al, 2012;Korsak et al, 2016;Bagni, 2014a, 2014b). In axons and dendrites, fragile X granules are transported along microtubules in a translationallyquiescent manner through interactions with kinesin, myosin, and dynein motor proteins (Kanai et al, 2004).…”

Section: Fmrp At Synapsesmentioning

confidence: 99%

A Synaptic Perspective of Fragile X Syndrome and Autism Spectrum Disorders

Bagni

Zukin

2019

Neuron

270

258

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Altered synaptic structure and function is a major hallmark of fragile X syndrome (FXS), autism spectrum disorders (ASDs), and other intellectual disabilities (IDs), which are therefore classified as synaptopathies. FXS and ASDs, while clinically and genetically distinct, share significant comorbidity, suggesting that there may be a common molecular and/or cellular basis, presumably at the synapse. In this article, we review brain architecture and synaptic pathways that are dysregulated in FXS and ASDs, including spine architecture, signaling in synaptic plasticity, local protein synthesis, (m)RNA modifications, and degradation. mRNA repression is a powerful mechanism for the regulation of synaptic structure and efficacy. We infer that there is no single pathway that explains most of the etiology and discuss new findings and the implications for future work directed at improving our understanding of the pathogenesis of FXS and related ASDs and the design of therapeutic strategies to ameliorate these disorders. ASDs and FXS: Causes and Clinical Features Approximately 1%-3% of the general population is affected by intellectual disabilities (IDs). IDs are neurodevelopmental disorders defined by significant limitations in intellectual functioning and adaptive behaviors and often exhibit comorbidity with autism (Mefford et al., 2012). Autism spectrum disorders (ASDs) are characterized by high phenotypic heterogeneity, comprising deficits in social interaction and communication as well as repetitive and stereotyped behaviors (

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Section: Fmrp At Synapsesmentioning

confidence: 99%

A Synaptic Perspective of Fragile X Syndrome and Autism Spectrum Disorders

Bagni

Zukin

2019

Neuron

270

258

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“…One conceptually attractive solution to this challenge is the local translation of mRNAs in the axon. Translation in developing and regenerating axons is well documented (2,3), and recent evidence suggests that CNS axons in the mammalian brain may also utilize this mechanism (4,5). However the extent to which endogenous ribosomes, mRNA and translational regulators localize to adult brain axons that are integrated into mature circuitry is unknown (6,7).…”

Section: Introductionmentioning

confidence: 99%

Axonal ribosomes and mRNAs associate with fragile X granules in adult rodent and human brains

et al. 2017

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Local mRNA translation in growing axons allows for rapid and precise regulation of protein expression in response to extrinsic stimuli. However, the role of local translation in mature CNS axons is unknown. Such a mechanism requires the presence of translational machinery and associated mRNAs in circuit-integrated brain axons. Here we use a combination of genetic, quantitative imaging and super-resolution microscopy approaches to show that mature axons in the mammalian brain contain ribosomes, the translational regulator FMRP and a subset of FMRP mRNA targets. This axonal translational machinery is associated with Fragile X granules (FXGs), which are restricted to axons in a stereotyped subset of brain circuits. FXGs and associated axonal translational machinery are present in hippocampus in humans as old as 57 years. This FXGassociated axonal translational machinery is present in adult rats, even when adult neurogenesis is blocked. In contrast, in mouse this machinery is only observed in juvenile hippocampal axons. This differential developmental expression was specific to the hippocampus, as both mice and rats exhibit FXGs in mature axons in the adult olfactory system. Experiments in Fmr1 null mice show that FMRP regulates axonal protein expression but is not required for axonal transport of ribosomes or its target mRNAs. Axonal translational machinery is thus a feature of adult CNS neurons. Regulation of this machinery by FMRP could support complex behaviours in humans throughout life.

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“…One important mechanism for such spatiotemporal control is local protein synthesis where mRNAs are targeted to specific domains and can be rapidly translated in response to nearby cues. This process has long been appreciated in dendrites (Holt and Schuman 2013;; Sutton and Schuman 2006) and recent evidence indicates that analogous translational machinery is also present in axons (Zheng et al, 2001;; Christie et al, 2009;; Taylor et al, 2009;; Korsak et al, 2016;; Shigeoka et al, 2016;; Akins et al, 2017;; Batista et al, 2017). Local protein synthesis is in part controlled by RNA binding proteins (RBPs) that can influence transcript fate through regulation of RNA biogenesis, localization, translation and degradation (Kapeli & Yeo, 2012;; Darnell, 2013;; Calabretta and Richard, 2015).…”

Section: Summary Statementmentioning

confidence: 99%