Dynamic bi-directional phosphorylation events associated with the reciprocal regulation of synapses during homeostatic up- and down-scaling

Desch, Kristina; Langer, Julian D.; Schuman, Erin M.

doi:10.1101/2021.03.26.437166

Cited by 9 publications

(12 citation statements)

References 78 publications

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“…One of the most intriguing finding in our study is that the autophagy-mediated PKA signaling primarily regulates the phosphorylation state of cytoskeletal scaffolding proteins confined to the postsynaptic density of excitatory synapses, whereas its contribution to the regulation of presynaptic and/or mitochondrial proteins is minor. Intriguingly, the majority of candidates identified in our global phosphoproteomics analysis (including LRRC7, DLGAP4, DLGAP2, SHANK3, STXBP5, SYNGAP1, EPB4.1L1) have been recently described to be essential for PKA-dependent synaptic downscaling of glutamatergic neurons ( 62 ). Homeostatic synaptic scaling defines a negative regulation of postsynaptic strength due to increased or decreased neuronal activity and is crucial to prevent runaway excitation and maintain circuit stability in the neocortex.…”

Section: Discussionmentioning

confidence: 98%

Autophagy regulates neuronal excitability by controlling cAMP/Protein Kinase A signaling

Overhoff

Tellkamp

Heß

et al. 2022

Preprint

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Autophagy provides nutrients during starvation and eliminates detrimental cellular components. However, accumulating evidence indicates that autophagy is not merely a housekeeping process. Here, we show that the protein AuTophaGy 5 (ATG5) functions in neurons to regulate the cAMP-dependent protein kinase A (PKA)-mediated phosphorylation of a synapse-confined proteome. This function of ATG5 is independent of bulk turnover of synaptic proteins and requires the targeting of PKA inhibitory R1 subunits to autophagosomes. Neuronal loss of ATG5 causes synaptic accumulation of PKA R1, which sequesters the PKA catalytic subunit and diminishes the cAMP/PKA-dependent phosphorylation of postsynaptic cytoskeletal proteins mediating AMPAR trafficking. Glutamatergic neurons-confined ATG5 deletion augments AMPAR-dependent excitatory neurotransmission and causes the appearance of spontaneous recurrent seizures in mice. Our findings identify a novel role of autophagy in regulating PKA signaling at glutamatergic synapses and suggest the PKA as a target for restoration of synaptic function in neurodegenerative conditions with autophagy dysfunction.

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Section: Discussionmentioning

confidence: 98%

Autophagy regulates neuronal excitability by controlling cAMP/Protein Kinase A signaling

Overhoff

Tellkamp

Heß

et al. 2022

Preprint

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“…Notably, many of these substrates change in phosphorylation upon induction of homeostatic downscaling (fig. S7) ( 75 ), a form of synaptic plasticity believed to occur during sleep to weaken excitatory synapses ( 8 , 73 ). Furthermore, predictive and experimental validation of microglial TNFα-targeted kinases allowed identification of PKCs and MAPKs (fig.…”

Section: Discussionmentioning

confidence: 99%

Microglial TNFα orchestrates brain phosphorylation during the sleep period and controls homeostatic sleep

Pinto

Cottin

Dingli

et al. 2022

Preprint

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The time we spend asleep is adjusted to previous time spent awake, and therefore believed to be under tight homeostatic control. Here, we establish microglia as a new cellular component of the sleep homeostat circuit. By using quantitative phosphoproteomics we demonstrate that microglia-derived TNFα controls thousands of phosphorylation sites during the sleep period. Substrates of microglial TNFα comprise sleep-promoting kinases and numerous synaptic proteins, including a subset whose phosphorylation status codes sleep need and determines sleep duration. As a result, lack of microglial TNFα attenuates the build-up of sleep need, as measured by slow wave activity, and prevents immediate compensation for loss of sleep. Together, we propose that microglia control sleep homeostasis by releasing TNFα that acts at the neuronal circuitry through dynamic control of phosphorylation. attenuates the build-up of sleep need, as measured by slow wave activity, and prevents immediate compensation for loss of sleep. Together, we propose that microglia control sleep homeostasis by releasing TNFα that acts at the neuronal circuitry through dynamic control of phosphorylation.

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“…For example, phosphorylation of tau regulates its solubility, which in turn is linked to its aggregation and formation of the neurofibrillary tangles found in Alzheimer's disease [93]. PTMs are also essential for the modulation of activity-dependent processes related to learning and memory [94,95]. Despite an increasing understanding of UPS regulation, many open questions remain, especially in the context of neurons, and little is known about local PTMs of ribosomes or UPS components, which likely play an important role in targeted protein synthesis and degradation.…”

Section: How Do Ptms Influence Protein Degradation?mentioning

confidence: 99%

Proteostatic regulation in neuronal compartments

Giandomenico

Álvarez-Castelao

Schuman

2022

Trends in Neurosciences

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Neurons continuously adapt to external cues and challenges, including stimulation, plasticity-inducing signals and aging. These adaptations are critical for neuronal physiology and extended survival. Proteostasis is the process by which cells adjust their protein content to achieve the specific protein repertoire necessary for cellular function. Due to their complex morphology and polarized nature, neurons possess unique proteostatic requirements. Proteostatic control in axons and dendrites must be implemented through regulation of protein synthesis and degradation in a decentralized fashion, but at the same time, it requires integration, at least in part, in the soma. Here, we discuss current understanding of neuronal proteostasis, as well as open questions and future directions requiring further exploration. The challenge of regulating a distant proteomeMost catalyzed chemical reactions inside cells depend on protein levels, and fine-tuning protein concentrations is key to ensure proper cellular function. Because throughout the cellular lifespan proteins accumulate damage, become dysfunctional and need to be replaced continually, protein synthesis and protein turnover are central to cellular physiology and function. The dynamic regulation of a balanced and functional proteome (i.e., proteostasis) concerns all proteins whose levels need to be adjusted in space and time in response to intracellular and extracellular cues. Thus, the specific parameters of cellular proteostasis vary across cell types and states. However, cellular proteostasis invariably relies on the precise control of protein synthesis, folding and conformational maintenance, post-translational modifications (PTMs), degradation, and secretion [1]. Precise control of these parameters is already challenging in cells that have little or no polarity, but becomes a particularly impressive feat for highly polarized cells, such as neurons.Neurons stand out from all other cell types in their unique morphology and high degree of compartmentalization; characteristics that are central to neuronal computation. Often, extrinsic signals are spatially localized so that only a confined portion of the neuron receives a certain signal, with the neuronal portion being, for instance, a cluster of dendrites (influenced by a neuromodulator), a single dendritic branch, a synaptic neighborhood, or even an individual synapse. How these local signals are transmitted to the somata remains largely unknown. Work over the last two decades has shown that neurons have the capacity to tune their proteome locally through regulation of local protein synthesis, degradation, and PTMs to regulate multiple aspects of dendritic and axonal biology [2]. Nevertheless, to date, we still lack a comprehensive understanding of how different cellular degradation pathways interact with the protein synthesis machinery to shape and maintain the local proteome.In this review, we discuss current understanding of neuronal local proteostatic regulation, and key knowledge gaps in the field. We also com...

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Dynamic bi-directional phosphorylation events associated with the reciprocal regulation of synapses during homeostatic up- and down-scaling

Cited by 9 publications

References 78 publications

Autophagy regulates neuronal excitability by controlling cAMP/Protein Kinase A signaling

Autophagy regulates neuronal excitability by controlling cAMP/Protein Kinase A signaling

Microglial TNFα orchestrates brain phosphorylation during the sleep period and controls homeostatic sleep

Proteostatic regulation in neuronal compartments

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