Dystroglycan Mediates Clustering of Essential GABAergic Components in Cerebellar Purkinje Cells

Briatore, Federica; Pregno, Giulia; Angelantonio, Silvia Di; Frola, Elena; Stefano, Maria Egle De; Vaillend, Cyrille; Sassoè‐Pognetto, Marco; Patrizi, Annarita

doi:10.3389/fnmol.2020.00164

Cited by 26 publications

(35 citation statements)

References 65 publications

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“…In addition, α2- and γ2 -GABA A Rs and miniature IPSC frequency are normal in hippocampal cultures from the gephyrin knock-out [ 85 ]. Gephyrin-independent clustering of GABA A Rs has been observed in other brain areas, including α1-containing GABA A Rs on Purkinje cell somas [ 86 , 87 , 88 , 89 ], perisomatic α1-containing GABA A Rs on hippocampal Pyr cells [ 90 , 91 , 92 ], and α2/α3/α5/β3-containing GABA A Rs on sensory afferents [ 93 ]. Our data indicate that gephyrin may be a particularly unreliable marker for PV-type inhibitory synapses and suggest that other types of inhibitory inputs be carefully evaluated for gephyrin colocalization.…”

Section: Discussionmentioning

confidence: 99%

Gephyrin-Lacking PV Synapses on Neocortical Pyramidal Neurons

Kuljis

Ray

Wegner

et al. 2021

IJMS

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Gephyrin has long been thought of as a master regulator for inhibitory synapses, acting as a scaffold to organize γ-aminobutyric acid type A receptors (GABAARs) at the post-synaptic density. Accordingly, gephyrin immunostaining has been used as an indicator of inhibitory synapses; despite this, the pan-synaptic localization of gephyrin to specific classes of inhibitory synapses has not been demonstrated. Genetically encoded fibronectin intrabodies generated with mRNA display (FingRs) against gephyrin (Gephyrin.FingR) reliably label endogenous gephyrin, and can be tagged with fluorophores for comprehensive synaptic quantitation and monitoring. Here we investigated input- and target-specific localization of gephyrin at a defined class of inhibitory synapse, using Gephyrin.FingR proteins tagged with EGFP in brain tissue from transgenic mice. Parvalbumin-expressing (PV) neuron presynaptic boutons labeled using Cre- dependent synaptophysin-tdTomato were aligned with postsynaptic Gephyrin.FingR puncta. We discovered that more than one-third of PV boutons adjacent to neocortical pyramidal (Pyr) cell somas lack postsynaptic gephyrin labeling. This finding was confirmed using correlative fluorescence and electron microscopy. Our findings suggest some inhibitory synapses may lack gephyrin. Gephyrin-lacking synapses may play an important role in dynamically regulating cell activity under different physiological conditions.

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Section: Discussionmentioning

confidence: 99%

Gephyrin-Lacking PV Synapses on Neocortical Pyramidal Neurons

Kuljis

Ray

Wegner

et al. 2021

IJMS

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“…Clstn3 protein was localized to parallel-fiber synapses by immunoelectron microscopy (Hintsch et al, 2002). Moreover, other genetic manipulations that cause a decrease in inhibitory synaptic transmission in cerebellar cortex, such as deletions of Nlgn2 or of GABA A -receptors (Briatore et al, 2020; Fritschy et al, 2006; Meng et al, 2019; Zhang et al, 2015), do not induce an increase in excitatory parallel-fiber synapses. Finally and probably most importantly, although competition between synapses using the same transmitters is well-described (e.g., competition between glutamatergic parallel- and climbing-fiber synapses on Purkinje cells; Cesa and Strata, 2009; Miyazaki et al, 2012; Strata et al, 1997), no such competition has been observed between GABAergic and glutamatergic synapses, such that the decrease in one of them would lead to the increase of the other.…”

Section: Discussionmentioning

confidence: 99%

“…The interaction of presynaptic neurexins with cerebellins and postsynaptic GluD receptors plays a major role in shaping parallel-fiber synapses (Yuzaki and Aricescu, 2017), and the binding of C1ql1 to postsynaptic Bai3 has a prominent function in climbing-fiber synapses (Kakegawa et al, 2015; Sigoillot et al, 2015). Postsynaptic Nlgn2 and Nlgn3 are major contributors to the function of GABAergic synapses in Purkinje cells (Zhang et al, 2015), as is dystroglycan (Briatore et al, 2020). How can we envision the collaboration of various synaptic adhesion complexes in establishing and shaping the different types of synapses on Purkinje cells?…”

Section: Discussionmentioning

confidence: 99%

Calsyntenin-3, an atypical cadherin, suppresses inhibitory basket- and stellate-cell synapses but boosts excitatory parallel-fiber synapses in cerebellum

Liu

Jiang

Liakath‐Ali

et al. 2021

Preprint

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Cadherins contribute to the organization of nearly all tissues, but the functions of several evolutionarily conserved cadherins, including those of calsyntenins, remain enigmatic. Puzzlingly, two distinct, non-overlapping functions for calsyntenins were proposed: As postsynaptic neurexin ligands in synapse formation, or as presynaptic adaptors for kinesin-mediated vesicular transport. Here, we show that acute CRISPR-mediated deletion of calsyntenin-3 in cerebellar Purkinje cells in vivo causes a large decrease in inhibitory synapses, but a surprisingly robust increase in excitatory parallel-fiber synapses. No changes in the dendritic architecture of Purkinje cells or in climbing-fiber synapses were detected. Thus, by promoting formation of an excitatory type of synapses and decreasing formation of an inhibitory type of synapses in the same neuron, calsyntenin-3 functions as a postsynaptic adhesion molecule that regulates the excitatory/inhibitory balance in Purkinje cells. No similarly opposing function of a synaptic adhesion molecule was previously observed, suggesting a new paradigm of synaptic regulation.

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“…While this is the only demonstration, to our knowledge, of a complete recycling loop of an ECM molecule, many additional studies also add credence to the concept of ECM recycling at synapses. These include reports of ECM molecules that undergo internalization (e.g., Coopman et al, 1996 ; Tammi et al, 2001 ; Shi and Sottile, 2008 ; Lobert et al, 2010 ; Leonoudakis et al, 2014 ), demonstrations that ECM receptors are present at synapses (e.g., Kramár et al, 2002 ; Huang et al, 2006 ; Roszkowska et al, 2016 ; Izumi et al, 2017 ; Apóstolo et al, 2020 ; Briatore et al, 2020 ), and reports that synapses contain the machinery for trafficking recycling molecules in an activity-dependent manner (Tang, 2008 ; Gürth et al, 2020 ; Helm et al, 2021 ). Nevertheless, additional demonstrations of the recycling of ECM molecules in neurons are anticipated in the future.…”

Section: Recycling Of Synaptic Ecmmentioning

confidence: 99%

The Synaptic Extracellular Matrix: Long-Lived, Stable, and Still Remarkably Dynamic

Dankovich

Rizzoli

2022

Front. Synaptic Neurosci.

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In the adult brain, synapses are tightly enwrapped by lattices of the extracellular matrix that consist of extremely long-lived molecules. These lattices are deemed to stabilize synapses, restrict the reorganization of their transmission machinery, and prevent them from undergoing structural or morphological changes. At the same time, they are expected to retain some degree of flexibility to permit occasional events of synaptic plasticity. The recent understanding that structural changes to synapses are significantly more frequent than previously assumed (occurring even on a timescale of minutes) has called for a mechanism that allows continual and energy-efficient remodeling of the extracellular matrix (ECM) at synapses. Here, we review recent evidence for such a process based on the constitutive recycling of synaptic ECM molecules. We discuss the key characteristics of this mechanism, focusing on its roles in mediating synaptic transmission and plasticity, and speculate on additional potential functions in neuronal signaling.

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Dystroglycan Mediates Clustering of Essential GABAergic Components in Cerebellar Purkinje Cells

Cited by 26 publications

References 65 publications

Gephyrin-Lacking PV Synapses on Neocortical Pyramidal Neurons

Gephyrin-Lacking PV Synapses on Neocortical Pyramidal Neurons

Calsyntenin-3, an atypical cadherin, suppresses inhibitory basket- and stellate-cell synapses but boosts excitatory parallel-fiber synapses in cerebellum

The Synaptic Extracellular Matrix: Long-Lived, Stable, and Still Remarkably Dynamic

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