Dissecting the Extracellular Complexity of Neuromuscular Junction Organizers

Guarino, Salvatore; Canciani, Anselmo; Forneris, Federico

doi:10.3389/fmolb.2019.00156

Cited by 27 publications

(25 citation statements)

References 209 publications

(337 reference statements)

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“…While many additional signalling pathways have been identified that play a role in synapse specialization, including neuregulin/ErbB, Wnt/β-catenin, and Hippo/Yes-associated protein signalling cascades [40] , the remainder of this section will emphasize molecules that have been examined in the DMD context and how they develop, maintain, and remodel synaptic structure and function. Readers interested in much more comprehensive surveys of NMJ maturation are enthusiastically referred to these recent, expert reviews [ 20 , 22 , 23 , 37 , 40 , 41 ].…”

Section: Development Maintenance and Plasticity Of The Nmjmentioning

confidence: 99%

Recent insights into neuromuscular junction biology in Duchenne muscular dystrophy: Impacts, challenges, and opportunities

Ljubicic

2020

EBioMedicine

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Duchenne muscular dystrophy (DMD) is the most common and relentless form of muscular dystrophy. The pleiotropic effects of dystrophin deficiency include remarkable impacts on neuromuscular junction (NMJ) structure and function. Some of these alterations contribute to the severe muscle wasting and weakness that distinguish DMD, while others attempt to compensate for them. Experimental approaches that correct NMJ biology in pre-clinical models of DMD attenuate disease progression and improve functional outcomes, which suggests that targeting the NMJ may be an effective therapeutic strategy for DMD patients. The objectives of this review are to 1) survey the distinctions in NMJ structure, function, and gene expression in the dystrophic context as compared to the healthy condition, and 2) summarize the efforts, opportunities and challenges to correct NMJ biology in DMD. This information will expand our basic understanding of neuromuscular biology and may be useful for designing novel NMJ-targeted drug or behavioural strategies to mitigate the dystrophic pathology and other disorders of the neuromuscular system.

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Section: Development Maintenance and Plasticity Of The Nmjmentioning

confidence: 99%

Recent insights into neuromuscular junction biology in Duchenne muscular dystrophy: Impacts, challenges, and opportunities

Ljubicic

2020

EBioMedicine

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“…It involves the neuron-secreted proteoglycan agrin with its receptor, the lipoprotein receptor-related protein 4 (LRP4), the muscle-specific kinase (MuSK) and the regulatory soluble synapse-specific protease Neurotrypsin. Since MuSK is not able to directly bind Agrin, LRP4 mediates the process by forming a stable receptor/co-receptor assembly (for a complete review see [ 1 ]). The complex interplay between motor axons, terminal Schwann cells and the muscle fibers of the peripheral nervous system (PNS), is reminiscent of the tripartite synapse in the central nervous system (CNS) where pre- and post-synaptic neurons and astrocytes interact ( Figure 1 ).…”

Section: Nmj Structural Architecture and Peculiaritiesmentioning

confidence: 99%

How to Build and to Protect the Neuromuscular Junction: The Role of the Glial Cell Line-Derived Neurotrophic Factor

Stanga

Boido

Kienlen‐Campard

2020

IJMS

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The neuromuscular junction (NMJ) is at the crossroad between the nervous system (NS) and the muscle. Following neurotransmitter release from the motor neurons (MNs), muscle contraction occurs and movement is generated. Besides eliciting muscle contraction, the NMJ represents a site of chemical bidirectional interplay between nerve and muscle with the active participation of Schwann cells. Indeed, signals originating from the muscle play an important role in synapse formation, stabilization, maintenance and function, both in development and adulthood. We focus here on the contribution of the Glial cell line-Derived Neurotrophic Factor (GDNF) to these processes and to its potential role in the protection of the NMJ during neurodegeneration. Historically related to the maintenance and survival of dopaminergic neurons of the substantia nigra, GDNF also plays a fundamental role in the peripheral NS (PNS). At this level, it promotes muscle trophism and it participates to the functionality of synapses. Moreover, compared to the other neurotrophic factors, GDNF shows unique peculiarities, which make its contribution essential in neurodegenerative disorders. While describing the known structural and functional changes occurring at the NMJ during neurodegeneration, we highlight the role of GDNF in the NMJ–muscle cross-talk and we review its therapeutic potential in counteracting the degenerative process occurring in the PNS in progressive and severe diseases such as Alzheimer’s disease (AD), Amyotrophic Lateral Sclerosis (ALS) and Spinal Muscular Atrophy (SMA). We also describe functional 3D neuromuscular co-culture systems that have been recently developed as a model for studying both NMJ formation in vitro and its involvement in neuromuscular disorders.

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“…Lrp4 (Pink frame, Figure 1) which plays a pivotal role in mediating agrin (via green-limit, MuSK lg1/2, Figure 1)-and Wnt (via red-limit, MuSK CRD, Figure 1)-signalings for AChR clustering at the postsynaptic membrane and also serves the retrograde signaling from muscle to nerve (Barik et al, 2014a;Guarino et al, 2020). The molecular structure of Lrp4 consists of a large extracellular domain that contains eight low-density lipoprotein receptor domains class A (LDLa), EGF-like domains and four β-propeller domains; its N-terminal region (including the last few LDLa repeats and the first β-propeller domain) interacts with agrin (Zhang et al, 2011;Zong et al, 2012); in its third β-propeller domain, the edge part mediates the MuSK signaling and the central part mediates the Wnt signaling (Ohkawara et al, 2014).…”

Section: Anti-lrp4 Antibodiesmentioning

confidence: 99%

“…Wnt 11 (Wu et al, 2010;Zhang et al, 2012a), Wnt 9a (Zhang et al, 2012a), and Wnt4 (Strochlic et al, 2012;Zhang et al, 2012a) are derived from muscles. The binding of the Ig4 domain (CRD) of MuSK (red-limit in pink MuSK, Figure 1) with Wnts contributes to AChR clustering through the non-canonical pathway mediated by the Dishevelled protein (Dvl; Pink frame, Figure 1), leading to the formation of AChR microclusters at the early non-innervated stage, termed as the AChR prepatterning (Kummer et al, 2006) which forms the clusters at the central part of the muscle and guides the incoming axon (Gray frame, Figure 1; Luo et al, 2002;Jing et al, 2009;Stiegler et al, 2009;Wu et al, 2010;Gordon et al, 2012;Koles and Budnik, 2012;Barik et al, 2014b;Burden et al, 2018;Guarino et al, 2020). The motoneuron-derived Wnt7a and Wnt7b serve nerve terminal development (Shen et al, 2018).…”

Section: Wnt-mediating Signal Via Musk Contributes To Achr Cluster Prmentioning

confidence: 99%

Myasthenia Gravis: From the Viewpoint of Pathogenicity Focusing on Acetylcholine Receptor Clustering, Trans-Synaptic Homeostasis and Synaptic Stability

Takamori

2020

Front. Mol. Neurosci.

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Myasthenia gravis (MG) is a disease of the postsynaptic neuromuscular junction (NMJ) where nicotinic acetylcholine (ACh) receptors (AChRs) are targeted by autoantibodies. Search for other pathogenic antigens has detected the antibodies against musclespecific tyrosine kinase (MuSK) and low-density lipoprotein-related protein 4 (Lrp4), both causing pre-and post-synaptic impairments. Agrin is also suspected as a fourth pathogen. In a complex NMJ organization centering on MuSK: (1) the Wnt non-canonical pathway through the Wnt-Lrp4-MuSK cysteine-rich domain (CRD)-Dishevelled (Dvl, scaffold protein) signaling acts to form AChR prepatterning with axonal guidance; (2) the neural agrin-Lrp4-MuSK (Ig1/2 domains) signaling acts to form rapsyn-anchored AChR clusters at the innervated stage of muscle; (3) adaptor protein Dok-7 acts on MuSK activation for AChR clustering from "inside" and also on cytoskeleton to stabilize AChR clusters by the downstream effector Sorbs1/2; (4) the trans-synaptic retrograde signaling contributes to the presynaptic organization via: (i) Wnt-MuSK CRD-Dvl-β catenin-Slit 2 pathway; (ii) Lrp4; and (iii) laminins. The presynaptic Ca 2+ homeostasis conditioning ACh release is modified by autoreceptors such as M1-type muscarinic AChR and A2A adenosine receptors. The post-synaptic structure is stabilized by: (i) lamininnetwork including the muscle-derived agrin; (ii) the extracellular matrix proteins (including collagen Q/perlecan and biglycan which link to MuSK Ig1 domain and CRD); and (iii) the dystrophin-associated glycoprotein complex. The study on MuSK ectodomains (Ig1/2 domains and CRD) recognized by antibodies suggested that the MuSK antibodies were pathologically heterogeneous due to their binding to multiple functional domains. Focussing one of the matrix proteins, biglycan which functions in the manner similar to collagen Q, our antibody assay showed the negative result in MG patients. However, the synaptic stability may be impaired by antibodies against MuSK ectodomains because of the linkage of biglycan with MuSK Ig1 domain and CRD. The pathogenic diversity of MG is discussed based on NMJ signaling molecules.

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Dissecting the Extracellular Complexity of Neuromuscular Junction Organizers

Cited by 27 publications

References 209 publications

Recent insights into neuromuscular junction biology in Duchenne muscular dystrophy: Impacts, challenges, and opportunities

Recent insights into neuromuscular junction biology in Duchenne muscular dystrophy: Impacts, challenges, and opportunities

How to Build and to Protect the Neuromuscular Junction: The Role of the Glial Cell Line-Derived Neurotrophic Factor

Myasthenia Gravis: From the Viewpoint of Pathogenicity Focusing on Acetylcholine Receptor Clustering, Trans-Synaptic Homeostasis and Synaptic Stability

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