Fragile X mental retardation protein (FMRP) interacting proteins exhibit different expression patterns during development

Bonaccorso, C.; Spatuzza, Michela; Marco, Barbara Di; Gloria, Angelo; Barrancotto, G.; Cupo, A.; Musumeci, S; D’Antoni, Simona; Bardoni, Barbara; Catania, Maria Vincenza

doi:10.1016/j.ijdevneu.2015.02.004

Cited by 47 publications

(54 citation statements)

References 53 publications

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“…Disruption of FMRP expression and function leads to dysregulation of activity-dependent local translation, and affects neuronal mechanisms of plasticity (Wang et al, 2014, Yun and Trommer, 2011). While the importance of FMRP during development has been well established, a potential role for FMRP in mediating alterations in translation in response to chronic ethanol exposure is not known (Saffary and Xie, 2011, Fernandez et al, 2013, Bonaccorso et al, 2015). The goal of the current study was to gain a better understand the role of FMRP in regulating ethanol-induced changes in protein expression at glutamatergic synapses.…”

Section: Introductionmentioning

confidence: 99%

FMRP Mediates Chronic Ethanol‐Induced Changes in NMDA, Kv4.2, and KChIP3 Expression in the Hippocampus

Spencer

Mulholland

Chandler

2016

Alcoholism Clin & Exp Res

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Background Exposure to chronic ethanol results in changes in expression of proteins that regulate neuronal excitability. The present study examined whether chronic ethanol alters the hippocampal expression and function of Fragile-X mental retardation protein (FMRP), and the role of FMRP in the modulation of chronic ethanol-induced changes in expression of NMDA receptors and Kv4.2 channels. Methods For in-vivo studies, C57Bl6/J mice underwent a chronic intermittent ethanol (CIE) vapor exposure procedure. After CIE, hippocampal tissue was collected and subjected to immunoblot blot analysis of NMDA receptor subunits (GluN1, GluN2B), Kv4.2 and its accessory protein KChIP3. For in-vitro studies, hippocampal slice cultures were exposed to 75 mM ethanol for 8 days. Following ethanol exposure, mRNAs bound to FMRP was measured. In a separate set of studies, cultures were exposed to an inhibitor of S6K1 (PF-4708671, 6 μM) in order to assess whether ethanol-induced homeostatic changes in protein expression depend upon changes in FMRP activity. Results Immunoblot blot analysis revealed increases in GluN1 and GluN2B but reductions in Kv4.2 and KChIP3. Analysis of mRNAs bound to FMRP revealed a similar bidirectional change observed as reduction of GluN2B and increase in Kv4.2 and KChiP3 mRNA transcripts. Analysis of FMRP further revealed that while chronic ethanol did not alter the expression of FMRP, it significantly increased phosphorylation of FMRP at the S499 residue that is known to critically regulate its activity. Inhibition of S6K1 prevented the chronic ethanol-induced increase in phospho-FMRP and changes in NMDA subunits, Kv4.2 and KChiP3. In contrast, PF-4708671 had no effect in the absence of alcohol, indicating it was specific for the chronic ethanol-induce changes. Conclusions These findings demonstrate that chronic ethanol exposure enhances translational control of plasticity related proteins by FMRP, and that S6K1 and FMRP activity are required for expression of chronic ethanol-induced homeostatic plasticity at glutamatergic synapses in the hippocampus.

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Section: Introductionmentioning

confidence: 99%

FMRP Mediates Chronic Ethanol‐Induced Changes in NMDA, Kv4.2, and KChIP3 Expression in the Hippocampus

Spencer

Mulholland

Chandler

2016

Alcoholism Clin & Exp Res

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“…Some findings from other laboratories are in line with our results. Indeed, (i) while both CYFIP1 and CYFIP2 interact with FMRP, only CYFIP2 interacts with FXR1P and FXR2P, the two paralogs and interactors of FMRP (Schenck et al, 2001); (ii) the expression of the two proteins appears differently modulated in different brain regions during post-natal brain development, while the three FXR proteins have the same expression pattern during development (Bonaccorso et al, 2015); (iii) depletion of CYFIP1 in epithelial cancer cells interferes with the morphology of the cells and induces invasion (Silva et al, 2009). This phenotype is also present when WAVE1 or NAP1 are knocked down.…”

Section: Discussionmentioning

confidence: 99%

“…CYFIP1 and CYFIP2 are members of a family of proteins interacting with the Fragile X mental retardation protein (FMRP, encoded by FMR1 ) in mammals, as well as in the fly (Abekhoukh and Bardoni, 2014; Schenck et al, 2001, 2003). They have different patterns of expression during brain development (Bonaccorso et al, 2015) and while CYFIP1 interacts only with FMRP, CYFIP2 is also a partner of the two other members of the Fragile X-related protein (FXR) family, namely FXR1P and FXR2P. CYFIP1 is involved in translational regulation by interacting not only with FMRP (Schenck et al, 2001), but also with the translation initiation factor 4E (Napoli et al, 2008; Beggs et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

“…While a few studies have linked the CYFIP family genes to carcinogenesis (Silva et al, 2009), a large number of studies focused on the role of these proteins both within neurons and during neuronal development (Abekhoukh and Bardoni, 2014; Bonaccorso et al, 2015) because of the functional links of these proteins to neurodevelopmental disorders such as ID, autism, schizophrenia or epilepsy (Schenck et al, 2001, 2003; Madrigal et al, 2012; Wang et al, 2015; Waltes et al, 2014; De Rubeis et al, 2013; Huang, 2016). CYFIP1 is localized in the BP1-BP2 region of human chromosome 15q11.2 (Abekhoukh and Bardoni, 2014) and deletion of this region (including the NIPA1 , NIPA2 , TUBGCP5 and WHAM genes) leads to the Burnside-Butler (BP1-BP2 microdeletion) syndrome, characterized by developmental and language delay, neurobehavioral disturbances and psychiatric problems, autism, seizures, schizophrenia and mild dysmorphic features (Cox and Butler, 2015).…”

Section: Introductionmentioning

confidence: 99%

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New insights into the regulatory function of CYFIP1 in the context of WAVE- and FMRP-containing complexes

Abekhoukh

Sahin

Grossi

et al. 2017

Disease Models &Amp; Mechanisms

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Cytoplasmic FMRP interacting protein 1 (CYFIP1) is a candidate gene for intellectual disability (ID), autism, schizophrenia and epilepsy. It is a member of a family of proteins that is highly conserved during evolution, sharing high homology with its Drosophila homolog, dCYFIP. CYFIP1 interacts with the Fragile X mental retardation protein (FMRP, encoded by the FMR1 gene), whose absence causes Fragile X syndrome, and with the translation initiation factor eIF4E. It is a member of the WAVE regulatory complex (WRC), thus representing a link between translational regulation and the actin cytoskeleton. Here, we present data showing a correlation between mRNA levels of CYFIP1 and other members of the WRC. This suggests a tight regulation of the levels of the WRC members, not only by post-translational mechanisms, as previously hypothesized. Moreover, we studied the impact of loss of function of both CYFIP1 and FMRP on neuronal growth and differentiation in two animal models – fly and mouse. We show that these two proteins antagonize each other's function not only during neuromuscular junction growth in the fly but also during new neuronal differentiation in the olfactory bulb of adult mice. Mechanistically, FMRP and CYFIP1 modulate mTor signaling in an antagonistic manner, likely via independent pathways, supporting the results obtained in mouse as well as in fly at the morphological level. Collectively, our results illustrate a new model to explain the cellular roles of FMRP and CYFIP1 and the molecular significance of their interaction.

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“…In addition to low IQ and learning disabilities, FXS patients exhibit hypersensitivity to multiple sensory modalities [1], and up to 20% comorbidity for childhood epilepsy [3]. Fragile X Mental Retardation Protein (FMRP) expression delineates early-use critical periods of neural circuit optimization in FXS disease models [4,5]. FMRP is proposed to function within the activity sensor mechanism, mediating activity-dependent synaptic remodeling based on early sensory experience [6,7].…”

Section: Introductionmentioning

confidence: 99%

Fragile X Mental Retardation Protein Requirements in Activity-Dependent Critical Period Neural Circuit Refinement

2017

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Summary Activity-dependent synaptic remodeling occurs during early-use critical periods, when naïve juveniles experience sensory input. Fragile X Mental Retardation Protein (FMRP) sculpts synaptic refinement in an activity sensor mechanism based on sensory cues, with FMRP loss causing the most common heritable autism spectrum disorder (ASD), Fragile X syndrome (FXS). In the well-mapped Drosophila olfactory circuitry, projection neurons (PN) relay peripheral sensory information to the central brain mushroom body (MB) learning/memory center. FMRP-null PNs reduce synaptic branching and enlarge boutons, with ultrastructural and synaptic reconstitution MB connectivity defects. Critical period activity modulation via odorant stimuli, optogenetics and transgenic tetanus toxin neurotransmission block show elevated PN activity phenocopies FMRP-null defects, while PN silencing causes opposing changes. FMRP-null PNs lose activity-dependent synaptic modulation, with impairments restricted to the critical period. We conclude FMRP is absolutely required for experience-dependent changes in synaptic connectivity during the developmental critical period of neural circuit optimization for sensory input.

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Fragile X mental retardation protein (FMRP) interacting proteins exhibit different expression patterns during development

Cited by 47 publications

References 53 publications

FMRP Mediates Chronic Ethanol‐Induced Changes in NMDA, Kv4.2, and KChIP3 Expression in the Hippocampus

FMRP Mediates Chronic Ethanol‐Induced Changes in NMDA, Kv4.2, and KChIP3 Expression in the Hippocampus

New insights into the regulatory function of CYFIP1 in the context of WAVE- and FMRP-containing complexes

Fragile X Mental Retardation Protein Requirements in Activity-Dependent Critical Period Neural Circuit Refinement

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