Local and substrate-specific S-palmitoylation determines subcellular localization of Gαo

Solis, Gonzalo P.; Valnohová, Jana; Álvarez, Cecilia; Katanaev, Vladimir L.

doi:10.1101/2020.08.25.266692

Cited by 7 publications

(8 citation statements)

References 87 publications

(253 reference statements)

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“…The G203R, R209C, and E246K mutants show a similar dual localization (fig. S1, A to D), indicative of the normal posttranslational modifications of the mutants ( 20 ). Quantification of fluorescence intensities at the two compartments confirmed the near-equal distribution of wild-type Gα o and the three pathologic mutants (fig.…”

Section: Resultsmentioning

confidence: 99%

Restoration of the GTPase activity and cellular interactions of Gα _o mutants by Zn ²⁺ in GNAO1 encephalopathy models

et al. 2022

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De novo point mutations in GNAO1 , gene encoding the major neuronal G protein Gα o , have recently emerged in patients with pediatric encephalopathy having motor, developmental, and epileptic dysfunctions. Half of clinical cases affect codons Gly 203 , Arg 209 , or Glu 246 ; we show that these mutations accelerate GTP uptake and inactivate GTP hydrolysis through displacement Gln 205 critical for GTP hydrolysis, resulting in constitutive GTP binding by Gα o . However, the mutants fail to adopt the activated conformation and display aberrant interactions with signaling partners. Through high-throughput screening of approved drugs, we identify zinc pyrithione and Zn 2+ as agents restoring active conformation, GTPase activity, and cellular interactions of the encephalopathy mutants, with negligible effects on wild-type Gα o . We describe a Drosophila model of GNAO1 encephalopathy where dietary zinc restores the motor function and longevity of the mutant flies. Zinc supplements are approved for diverse human neurological conditions. Our work provides insights into the molecular etiology of GNAO1 encephalopathy and defines a potential therapy for the patients.

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Section: Resultsmentioning

confidence: 99%

Restoration of the GTPase activity and cellular interactions of Gα _o mutants by Zn ²⁺ in GNAO1 encephalopathy models

et al. 2022

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“…The subcellular localization of three other Gαo pathological point mutants (Gly203Arg, Ile279Asn, and Asp174Gly) has been previously analyzed and found not to affect the plasma membrane localization [14], in contrast to what we see for the Gln52 mutants (Figure 4). It is worth noting that the retained Golgi localization of the Gln52 mutants is indicative of the proper lipid modifications of the Gln52 Gαo mutants [43].…”

Section: Discussionmentioning

confidence: 96%

Pediatric Encephalopathy: Clinical, Biochemical and Cellular Insights into the Role of Gln52 of GNAO1 and GNAI1 for the Dominant Disease

Solis

Кожанова

Koval

et al. 2021

Cells

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Heterotrimeric G proteins are immediate transducers of G protein-coupled receptors—the biggest receptor family in metazoans—and play innumerate functions in health and disease. A set of de novo point mutations in GNAO1 and GNAI1, the genes encoding the α-subunits (Gαo and Gαi1, respectively) of the heterotrimeric G proteins, have been described to cause pediatric encephalopathies represented by epileptic seizures, movement disorders, developmental delay, intellectual disability, and signs of neurodegeneration. Among such mutations, the Gln52Pro substitutions have been previously identified in GNAO1 and GNAI1. Here, we describe the case of an infant with another mutation in the same site, Gln52Arg. The patient manifested epileptic and movement disorders and a developmental delay, at the onset of 1.5 weeks after birth. We have analyzed biochemical and cellular properties of the three types of dominant pathogenic mutants in the Gln52 position described so far: Gαo[Gln52Pro], Gαi1[Gln52Pro], and the novel Gαo[Gln52Arg]. At the biochemical level, the three mutant proteins are deficient in binding and hydrolyzing GTP, which is the fundamental function of the healthy G proteins. At the cellular level, the mutants are defective in the interaction with partner proteins recognizing either the GDP-loaded or the GTP-loaded forms of Gαo. Further, of the two intracellular sites of Gαo localization, plasma membrane and Golgi, the former is strongly reduced for the mutant proteins. We conclude that the point mutations at Gln52 inactivate the Gαo and Gαi1 proteins leading to aberrant intracellular localization and partner protein interactions. These features likely lie at the core of the molecular etiology of pediatric encephalopathies associated with the codon 52 mutations in GNAO1/GNAI1.

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“…When examining gene expression using the DropViz hippocampal single-cell RNAseq database, we found that 10 of the 30 palmitoylating/ de-palmitoylating enzymes and accessory proteins were predominantly enriched in neurons and also highly co-expressed with neuron-enriched differentially palmitoylated proteins from our screen. ZDHHC enzymes in this subset are thought to localize to a variety of subcellular domains, including the Golgi (ZDHHC3, ZDHHC13, ZDHHC17, ZDHHC21, ZDHHC23) and postsynapse (ZDHHC2, ZDHHC5, ZDHHC8) (Malgapo & Linder, 2021; Solis, Valnohova, Alvarez, & Katanaev, 2020). We found that a substantial proportion of the differentially palmitoylated substrates identified in our screen localize at the pre- and/or postsynapse, making ZDHHC2, ZDHHC5 and ZDHHC8 well positioned to mediate postsynaptic increases in substrate palmitoylation in response to plasticity-inducing stimuli.…”

Section: Discussionmentioning

confidence: 99%

Synaptic Activity-Dependent Changes in the Hippocampal Palmitoylome

Nasseri

Matin

Tosefsky

et al. 2021

Preprint

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Dynamic protein S-palmitoylation is critical for neuronal function, development, and synaptic plasticity. Activity-dependent changes in palmitoylation have been observed for several neuronal substrates, however a full characterization of the activity-regulated palmitoylome is lacking. Here, we use an unbiased approach to identify differentially palmitoylated proteins in the mouse hippocampus following context-dependent fear conditioning. Of the 121 differentially palmitoylated proteins identified 63 were synaptic proteins, while others were associated with metabolic functions, cytoskeletal organization, and signal transduction. The vast majority of synaptic proteins exhibited increased palmitoylation following fear conditioning, whereas proteins that exhibited decreased palmitoylation were predominantly associated with metabolic processes. We show a link between dynamic palmitoylation and synapse plasticity by demonstrating that the palmitoylation of one of our identified proteins, PRG-1/LPPR4, is essential for activity-induced insertion of AMPA receptors into the postsynaptic membrane. Together, this study identifies networks of synaptic proteins whose dynamic palmitoylation may play a central role in learning and memory.SUMMARYThis study identifies networks of proteins that undergo dynamic post-translational palmitoylation in response to fear conditioning and demonstrates that palmitoylation of one of these proteins is essential for synapse plasticity. Together, this illustrates the importance of palmitoylation in learning/memory and synapse plasticity.

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Local and substrate-specific S-palmitoylation determines subcellular localization of Gαo

Cited by 7 publications

References 87 publications

Restoration of the GTPase activity and cellular interactions of Gα _o mutants by Zn ²⁺ in GNAO1 encephalopathy models

Restoration of the GTPase activity and cellular interactions of Gα _o mutants by Zn ²⁺ in GNAO1 encephalopathy models

Pediatric Encephalopathy: Clinical, Biochemical and Cellular Insights into the Role of Gln52 of GNAO1 and GNAI1 for the Dominant Disease

Synaptic Activity-Dependent Changes in the Hippocampal Palmitoylome

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Local and substrate-specific S-palmitoylation determines subcellular localization of Gαo

Cited by 7 publications

References 87 publications

Restoration of the GTPase activity and cellular interactions of Gα o mutants by Zn 2+ in GNAO1 encephalopathy models

Restoration of the GTPase activity and cellular interactions of Gα o mutants by Zn 2+ in GNAO1 encephalopathy models

Pediatric Encephalopathy: Clinical, Biochemical and Cellular Insights into the Role of Gln52 of GNAO1 and GNAI1 for the Dominant Disease

Synaptic Activity-Dependent Changes in the Hippocampal Palmitoylome

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Restoration of the GTPase activity and cellular interactions of Gα _o mutants by Zn ²⁺ in GNAO1 encephalopathy models

Restoration of the GTPase activity and cellular interactions of Gα _o mutants by Zn ²⁺ in GNAO1 encephalopathy models