The HSPG Glypican Regulates Experience-Dependent Synaptic and Behavioral Plasticity by Modulating the Non-Canonical BMP Pathway

Kamimura, Kazuo; Odajima, Aiko; Ikegawa, Yuko; Maru, Chikako; Maeda, Nobuaki

doi:10.1016/j.celrep.2019.08.032

Cited by 17 publications

(9 citation statements)

References 61 publications

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“…Later in neurodevelopment, secreted trans -synaptic BMP signaling regulates synaptic structure and function at the Drosophila larval glutamatergic NMJ ( Figure 1 ), including motoneuron terminal growth ( Sulkowski et al, 2016 ; Kamimura et al, 2019 ), neurotransmission strength ( Kamimura et al, 2019 ; Politano et al, 2019 ), and maintained homeostasis ( Chou et al, 2020 ). Three known BMP ligands Decapentaplegic (Dpp), Glass-bottom boat (Gbb), and Screw (Scw) ( Upadhyay et al, 2017 ) are secreted from either presynaptic boutons or postsynaptic muscles to activate BMP type I receptors Thick veins (Tkv) and Saxophone (Sax), and either of two the type II receptors Wishful thinking (Wit) or Punt (Put) ( Kim and O’Connor, 2014 ; Upadhyay et al, 2017 ).…”

Section: Part 1: Bmp Signaling In Fxsmentioning

confidence: 99%

“…Nevertheless, the GluRIIA accumulation in the Drosophila FXS model ( Pan and Broadie, 2007 ) is well explained by the postsynaptic FMRP-Stau-Cora regulative pathway, which activates phosphorylation of presynaptic Mothers against Decapentaplegic (Mad) to drive NMJ bouton overgrowth ( Figure 1 ; Song et al, 2022 ). Interestingly, Coracle overexpression and RNAi phenocopy ( Song et al, 2022 ), as in other neurodevelopmental contexts ( Landsverk et al, 2007 ; Tokuda et al, 2014 ; Fulterer et al, 2018 ), and GluRIIA-induced pMad production does not involve BMP ligands ( Friedman et al, 2013 ; Sulkowski et al, 2016 ; Kamimura et al, 2019 ), but does depend on BMP receptors Wit and Sax ( Sulkowski et al, 2016 ; Kamimura et al, 2019 ). GluRIIA is thought to interact with Wit through the transmembrane GluR-clustering protein Neto ( Chou et al, 2020 ), but the mechanism of this FMRP-dependent noncanonical trans -synaptic BMP signaling remains to be fully elucidated.…”

Section: Part 1: Bmp Signaling In Fxsmentioning

confidence: 99%

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Dysregulation of BMP, Wnt, and Insulin Signaling in Fragile X Syndrome

Song

Broadie²

2022

Front. Cell Dev. Biol.

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Drosophila models of neurological disease contribute tremendously to research progress due to the high conservation of human disease genes, the powerful and sophisticated genetic toolkit, and the rapid generation time. Fragile X syndrome (FXS) is the most prevalent heritable cause of intellectual disability and autism spectrum disorders, and the Drosophila FXS disease model has been critical for the genetic screening discovery of new intercellular secretion mechanisms. Here, we focus on the roles of three major signaling pathways: BMP, Wnt, and insulin-like peptides. We present Drosophila FXS model defects compared to mouse models in stem cells/embryos, the glutamatergic neuromuscular junction (NMJ) synapse model, and the developing adult brain. All three of these secreted signaling pathways are strikingly altered in FXS disease models, giving new mechanistic insights into impaired cellular outcomes and neurological phenotypes. Drosophila provides a powerful genetic screening platform to expand understanding of these secretory mechanisms and to test cellular roles in both peripheral and central nervous systems. The studies demonstrate the importance of exploring broad genetic interactions and unexpected regulatory mechanisms. We discuss a number of research avenues to pursue BMP, Wnt, and insulin signaling in future FXS investigations and the development of potential therapeutics.

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Section: Part 1: Bmp Signaling In Fxsmentioning

confidence: 99%

Section: Part 1: Bmp Signaling In Fxsmentioning

confidence: 99%

Dysregulation of BMP, Wnt, and Insulin Signaling in Fragile X Syndrome

Song

Broadie²

2022

Front. Cell Dev. Biol.

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“…Most basically, the brain’s ECM biomacromolecule composition consists of: (i) glycosaminoglycans (GAGs)–hyaluronic acid (HA) [ 17 , 22 , 25 ]; (ii) proteoglycans (PGs)–chondroitin sulfate proteoglycans (brevican, versican, neurocan, and phosphacan) [ 22 , 26 , 27 , 28 , 29 , 30 ], and heparan sulfate proteoglycans (syndecan, glypican, agrin, and perlecan) [ 25 , 31 , 32 , 33 ] and (iii) glycoproteins—link proteins, tenascin-R, collagens, fibronectins, laminins, and nidogens [ 3 , 17 , 32 , 34 , 35 , 36 , 37 , 38 ] ( Figure 2 ). The scaffolding for the ECM structure is made up of GAGs, namely HA polymers.…”

Section: Composition and Biological Meaning Of Brain’s Extracellular ...mentioning

confidence: 99%

“…In the central nervous system (CNS), the two primary types of PGs are chondroitin sulfate proteoglycans and heparin sulfate proteoglycans [ 25 , 31 ]. The most prevalent chondroitin sulfate proteoglycans are lecticans, which are involved in gliogenesis in the developing brain, tissue repair after brain injury or in brain tumors, neuronal adhesion, axonal growth, development of the nervous system, and inhibition of neurite outgrowth [ 25 , 31 , 32 , 33 ].The other type of PGs are involved in binding different proteins, basement membrane association, signaling, structural functions, growth factor signaling and sensitivity, binding proteins during neuronal development, and organization of the basement membrane [ 25 , 31 , 32 , 33 ]. Glycoproteins are engaged in interactions between HA and aggrecan, formation of lectin complexes, antiadhesive and adhesive functions dependent on cell type, expression in tumors, vascular basement membrane, cell development and differentiation, and creation of strong complexes [ 3 , 17 , 22 , 32 , 34 , 35 , 36 , 37 , 38 ].…”

Section: Composition and Biological Meaning Of Brain’s Extracellular ...mentioning

confidence: 99%

Mechanical Properties of the Extracellular Environment of Human Brain Cells Drive the Effectiveness of Drugs in Fighting Central Nervous System Cancers

et al. 2022

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The evaluation of nanomechanical properties of tissues in health and disease is of increasing interest to scientists. It has been confirmed that these properties, determined in part by the composition of the extracellular matrix, significantly affect tissue physiology and the biological behavior of cells, mainly in terms of their adhesion, mobility, or ability to mutate. Importantly, pathophysiological changes that determine disease development within the tissue usually result in significant changes in tissue mechanics that might potentially affect the drug efficacy, which is important from the perspective of development of new therapeutics, since most of the currently used in vitro experimental models for drug testing do not account for these properties. Here, we provide a summary of the current understanding of how the mechanical properties of brain tissue change in pathological conditions, and how the activity of the therapeutic agents is linked to this mechanical state.

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“…Synaptic signaling is also regulated by heparan sulfate proteoglycans (HSPGs) such as Dallylike (Dlp) and Syndecan (Sdc), which impact multiple pathways including Wnt/Wg and BMP [254,255]. Dlp acts as a negative brake on the positive feedback loop between GluRIIA and presynaptic pMad that is itself inhibited by presence of Octopamine, the Drosophila analog of nonadrenaline [256]. Additionally, Dlp and Sdc regulate the RPTP LAR, with effects on presynaptic neuronal morphology and AZ assembly [31,120].…”

Section: Trans-synaptic Communication Between Compartmentsmentioning

confidence: 99%

Synapse development and maturation at the drosophila neuromuscular junction

2020

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Synapses are the sites of neuron-to-neuron communication and form the basis of the neural circuits that underlie all animal cognition and behavior. Chemical synapses are specialized asymmetric junctions between a presynaptic neuron and a postsynaptic target that form through a series of diverse cellular and subcellular events under the control of complex signaling networks. Once established, the synapse facilitates neurotransmission by mediating the organization and fusion of synaptic vesicles and must also retain the ability to undergo plastic changes. In recent years, synaptic genes have been implicated in a wide array of neurodevelopmental disorders; the individual and societal burdens imposed by these disorders, as well as the lack of effective therapies, motivates continued work on fundamental synapse biology. The properties and functions of the nervous system are remarkably conserved across animal phyla, and many insights into the synapses of the vertebrate central nervous system have been derived from studies of invertebrate models. A prominent model synapse is the Drosophila melanogaster larval neuromuscular junction, which bears striking similarities to the glutamatergic synapses of the vertebrate brain and spine; further advantages include the simplicity and experimental versatility of the fly, as well as its century-long history as a model organism. Here, we survey findings on the major events in synaptogenesis, including target specification, morphogenesis, and the assembly and maturation of synaptic specializations, with a emphasis on work conducted at the Drosophila neuromuscular junction.

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The HSPG Glypican Regulates Experience-Dependent Synaptic and Behavioral Plasticity by Modulating the Non-Canonical BMP Pathway

Cited by 17 publications

References 61 publications

Dysregulation of BMP, Wnt, and Insulin Signaling in Fragile X Syndrome

Dysregulation of BMP, Wnt, and Insulin Signaling in Fragile X Syndrome

Mechanical Properties of the Extracellular Environment of Human Brain Cells Drive the Effectiveness of Drugs in Fighting Central Nervous System Cancers

Synapse development and maturation at the drosophila neuromuscular junction

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