α2δ-3 Is Required for Rapid Transsynaptic Homeostatic Signaling

Wang, Tingting; Jones, Ryan; Whippen, Jenna; Davis, Graeme W.

doi:10.1016/j.celrep.2016.08.030

Cited by 55 publications

(64 citation statements)

References 46 publications

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“…In blue, two components residing in the synaptic extracellular matrix have been implicated in PHP. The α2δ3 auxiliary subunit of the presynaptic calcium channel is necessary for PHP 36 . The matrix-derived signaling protein Endostatin, a cleavage product of the collagen homologue Multiplexin, is also necessary for PHP 37 .…”

Section: Extended Datamentioning

confidence: 99%

Retrograde semaphorin–plexin signalling drives homeostatic synaptic plasticity

Orr

Fetter

Davis

2017

Nature

100

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Homeostatic signaling systems ensure stable, yet flexible neural activity and animal behavior1–4. Defining the underlying molecular mechanisms of neuronal homeostatic signaling will be essential in order to establish clear connections to the causes and progression of neurological disease. Presynaptic homeostatic plasticity (PHP) is a conserved form of neuronal homeostatic signaling, observed in organisms ranging from Drosophila to human1,5. Here, we demonstrate that Semaphorin2b (Sema2b) is target-derived signal that acts upon presynaptic PlexinB (PlexB) receptors to mediate the retrograde, homeostatic control of presynaptic neurotransmitter release at the Drosophila neuromuscular junction. Sema2b-PlexB signaling regulates the expression of PHP via the cytoplasmic protein Mical and the oxoreductase-dependent control of presynaptic actin6,7. During neural development, Semaphorin-Plexin signaling instructs axon guidance and neuronal morphogenesis8–10. Yet, Semaphorins and Plexins are also expressed in the adult brain11–16. Here we demonstrate that Semaphorin-Plexin signaling controls presynaptic neurotransmitter release. We propose that Sema2b-PlexB signaling is an essential platform for the stabilization of synaptic transmission throughout life.

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Section: Extended Datamentioning

confidence: 99%

Retrograde semaphorin–plexin signalling drives homeostatic synaptic plasticity

Orr

Fetter

Davis

2017

Nature

100

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“…Notably, in Drosophila motoneurons both dα 2 δ 1 and dα 2 δ 3 are co-expressed, but localize to different subneuronal compartments. dα 2 δ 3 but not dα 2 δ 1 localizes at axon terminals and is required for presynaptic function (Wang et al, 2016; this study) and embryonic synapse development (Kurshan et al, 2009). Moreover, we find that dα 2 δ 3 and dα 2 δ 1 affect different aspects of motoneuron calcium channel function (see below) .…”

Section: Discussionmentioning

confidence: 60%

“…During embryonic development loss of dα 2 δ 3 (stj) function impairs early steps of synapse formation before calcium channels arrive at the presynaptic terminal, as well as the subsequent recruitment of Ca v 2-like channels to the active zone (Kurshan et al, 2009). Moreover, at mature larval neuromuscular junctions, dα 2 δ 3 is required for rapid induction and continuous expression of pre-synaptic homeostatic potentiation (Wang et al, 2016). Our data demonstrate that dα 2 δ 3 is not only required for Ca v 2 channel function at the pre-synaptic terminal, but also for normal flight motoneuron somatodendritic and axonal calcium currents, both of which are mediated by the Drosophila Ca v 2 channel homolog cacophony .…”

Section: Discussionmentioning

confidence: 99%

Different α₂δ Accessory Subunits Regulate Distinctly Different Aspects of Calcium Channel Function in the Same Drosophila Neurons

Heinrich

Ryglewski

2019

Preprint

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Voltage gated calcium channels (VGCCs) regulate neuronal excitability and translate activity into calcium dependent intracellular signaling. The pore forming α 1 subunit of high voltage activated (HVA) VGCCs operates not in isolation but associates with α 2 δ accessory subunits. α 2 δ subunits can affect calcium channel biophysical properties, surfacing, localization and transport, but their in vivo functions are incompletely understood. In vertebrates, it is largely unknown whether different combinations of the four α 2 δ and the 7 α 1 subunits mediate different or partially redundant functions or whether different α 1 /α 2 δ combinations regulate different aspects of VGCC function. This study capitalizes on the relatively simpler situation in the Drosophila genetic model that contains only two genes for HVA calcium channels, one Ca v 1 homolog and one Ca v 2 homolog, both with well-described functions in different compartments of identified motoneurons. We find that both dα 2 δ 1 and dα 2 δ 3 (stj) are broadly but differently expressed in the nervous system. Both are expressed in motoneurons, but with differential subcellular localization. Functional analysis reveals that dα 2 δ 3 is required for normal Ca v 1 and Ca v 2 current amplitudes and for correct Ca v 2 channel function in all neuronal compartments, axon terminal, axon, and somatodendritic domain. By contrast, dα 2 δ 1 does not affect Ca v 1 or Ca v 2 current amplitudes or presynaptic function, but it is required for correct Ca v 2 channel allocation to the axonal versus the dendritic domain. Therefore, different α 2 δ subunits are required in the same neurons to precisely regulate distinctly different functions of HVA calcium channels, which is in accord with specific α 2 δ mutations causing different brain diseases. Significance StatementCalcium influx through the pore forming α 1 -subunit of voltage gated calcium channels serves essential neuronal functions, such as synaptic vesicle release, control of action potential shape and frequencies, synaptic input computations, and transcriptional control. Localization and function of α 1 -calcium channel subunits depend on interactions with α 2 δ accessory subunits. Here we present in vivo analysis of Drosophila motoneurons revealing that different α 2 δ subunits independently regulate distinctly different aspects of calcium channel function in the same neuron, such as current amplitude and dendritic versus axonal channel localization. Our findings start unraveling how different α 1 /α 2 δ combinations regulate functional calcium channel diversity in different sub-neuronal compartments, and may provide an entry point toward understanding how mutations of different α 2 δ genes underlie brain diseases.

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“…Besides Brp, several presynaptic components have been implicated in the control of PHP (reviewed in (Frank, 2014)). They include (1) Cacophony, the α1 subunit of CaV2-type calcium channels and its auxiliary protein α2-3, which control the presynaptic Ca 2+ influx Wang et al, 2016), (Letts et al) the signaling molecules upstream Cac, Eph, Ephexin and Cdc42 (Frank et al, 2009), and (3) the BMP pathway components, Wit and Mad, required for the retrograde BMP signaling (Goold and Davis, 2007). In addition, expression of PHP requires molecules that regulate vesicle release and the RRP size, such as RIM , Rab3-GAP (Muller et al, 2011), Dysbindin (Dickman and Davis, 2009), SNAP25 and Snapin (Dickman et al, 2012).…”

Section: Discussionmentioning

confidence: 99%

Neto-α controls synapse organization and homeostasis at the Drosophila neuromuscular junction

Han

Vicidomini

Ramos

et al. 2019

Preprint

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Glutamate receptor auxiliary proteins control receptor distribution and function, ultimately controlling synapse assembly, maturation and plasticity. At the Drosophila neuromuscular junction (NMJ), a synapse with both pre-and post-synaptic kainate-type glutamate receptors (KARs), we show that the auxiliary protein Neto evolved functionally distinct isoforms to modulate synapse development and homeostasis. Using genetics, cell biology and electrophysiology we demonstrate that Neto-α functions on both sides of the NMJ. In muscle, Neto-α limits the size of the postsynaptic receptors field. In motor neurons, Neto-α controls neurotransmitter release in a KAR-dependent manner. Furthermore, Neto-α is both required and sufficient for the presynaptic increase in neurotransmitter release in response to reduced postsynaptic sensitivity. This KARindependent function of Neto-α is involved in activity-induced cytomatrix remodeling. We propose that Drosophila ensured NMJ functionality by acquiring two Neto isoforms with differential expression patterns and activities.

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α2δ-3 Is Required for Rapid Transsynaptic Homeostatic Signaling

Cited by 55 publications

References 46 publications

Retrograde semaphorin–plexin signalling drives homeostatic synaptic plasticity

Retrograde semaphorin–plexin signalling drives homeostatic synaptic plasticity

Different α₂δ Accessory Subunits Regulate Distinctly Different Aspects of Calcium Channel Function in the Same Drosophila Neurons

Neto-α controls synapse organization and homeostasis at the Drosophila neuromuscular junction

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α2δ-3 Is Required for Rapid Transsynaptic Homeostatic Signaling

Cited by 55 publications

References 46 publications

Retrograde semaphorin–plexin signalling drives homeostatic synaptic plasticity

Retrograde semaphorin–plexin signalling drives homeostatic synaptic plasticity

Different α2δ Accessory Subunits Regulate Distinctly Different Aspects of Calcium Channel Function in the Same Drosophila Neurons

Neto-α controls synapse organization and homeostasis at the Drosophila neuromuscular junction

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Different α₂δ Accessory Subunits Regulate Distinctly Different Aspects of Calcium Channel Function in the Same Drosophila Neurons