Ankyrin-G regulates forebrain connectivity and network synchronization via interaction with GABARAP

Nelson, Andrew D.; Caballero‐Florán, Rene Nahum; Díaz, Jean Carlos Rodríguez; Hull, Jacob M.; Yuan, Yukun; Li, J.; Chen, K.; Walder, Kathryn K.; Lopez-Santiago, Luis F.; Bennett, Vann; McInnis, Melvin G.; Isom, Lori L.; Wang, Chao; Zhang, M.; Jones, Kevin S.; Jenkins, Paul M.

doi:10.1038/s41380-018-0308-x

Cited by 42 publications

(52 citation statements)

References 65 publications

(89 reference statements)

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“…For example, α-helically extended LIR in ankyrins AnkB shows an affinity to GABARAPs in sub-nanomolar ranges (K D values 0.21–0.29 nM) [ 100 ]. The physiological importance of the GABARAP:AnkG interaction is underscored by the study in which a LIR-deficient form of AnkG (W1989R), which fails to bind to GABARAP, leads to a massive reduction in forebrain GABAergic synapses associated with hyperexcitability of pyramidal cell and disruptions in the synchronization of neuronal networks [ 111 ]. Interestingly, LC3 proteins display a lower affinity for this LIR (K D 3.2–10.5 nM), highlighting the functional specialization within the LC3/GABARAP family.…”

Section: Interactions Between Atg8/lc3/gabarap Proteins and Their mentioning

confidence: 99%

Atg8-Family Proteins—Structural Features and Molecular Interactions in Autophagy and Beyond

Wesch

Kirkin

Rogov

2020

Cells

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Autophagy is a common name for a number of catabolic processes, which keep the cellular homeostasis by removing damaged and dysfunctional intracellular components. Impairment or misbalance of autophagy can lead to various diseases, such as neurodegeneration, infection diseases, and cancer. A central axis of autophagy is formed along the interactions of autophagy modifiers (Atg8-family proteins) with a variety of their cellular counter partners. Besides autophagy, Atg8-proteins participate in many other pathways, among which membrane trafficking and neuronal signaling are the most known. Despite the fact that autophagy modifiers are well-studied, as the small globular proteins show similarity to ubiquitin on a structural level, the mechanism of their interactions are still not completely understood. A thorough analysis and classification of all known mechanisms of Atg8-protein interactions could shed light on their functioning and connect the pathways involving Atg8-proteins. In this review, we present our views of the key features of the Atg8-proteins and describe the basic principles of their recognition and binding by interaction partners. We discuss affinity and selectivity of their interactions as well as provide perspectives for discovery of new Atg8-interacting proteins and therapeutic approaches to tackle major human diseases.

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Section: Interactions Between Atg8/lc3/gabarap Proteins and Their mentioning

confidence: 99%

Atg8-Family Proteins—Structural Features and Molecular Interactions in Autophagy and Beyond

Wesch

Kirkin

Rogov

2020

Cells

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“…Similarly, 480 kDa ankyrin‐G interacts with GABARAP, a MAP member of the ubiquitin‐like LC3 family at extrasynaptic somatodendritic plasma membranes of pyramidal neurons (Tseng et al, ). 480 kDa ankyrin‐G binds GABARAP through a tryptophan residue (W1989) within a LC3‐interacting (LIR) motif in the inserted region (Alemu et al, ; Nelson et al, ; Tseng et al, ). 480 kDa ankyrin‐G localization at extrasynaptic GABAergic microdomains is promoted by protein–protein interactions via the inserted region and by its direct insertion into the plasma membrane through C70‐dependent palmitoylation, which are both required for stabilizing GABA A receptor synapses (Tseng et al, ).…”

Section: Functional Roles Of the Spectrin And Ankyrin Assemblies In Nmentioning

confidence: 99%

“…480 kDa ankyrin-G binds GABARAP through a tryptophan residue (W1989) within a LC3-interacting (LIR) motif in the inserted region (Alemu et al, 2012;Nelson et al, 2018;Tseng et al, 2015). 480 kDa ankyrin-G localization at extrasynaptic GABAergic microdomains is promoted by protein-protein interactions via the inserted region and by its direct insertion into the plasma membrane through C70-dependent palmitoylation, which are both required for stabilizing GABA A receptor synapses .…”

Section: Microtubules and Microtubule-associated Proteinsmentioning

confidence: 99%

Cargo hold and delivery: Ankyrins, spectrins, and their functional patterning of neurons

Lorenzo

2020

Cytoskeleton

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The highly polarized, typically very long, and nonmitotic nature of neurons present them with unique challenges in the maintenance of their homeostasis. This architectural complexity serves a rich and tightly controlled set of functions that enables their fast communication with neighboring cells and endows them with exquisite plasticity. The submembrane neuronal cytoskeleton occupies a pivotal position in orchestrating the structural patterning that determines local and long‐range subcellular specialization, membrane dynamics, and a wide range of signaling events. At its center is the partnership between ankyrins and spectrins, which self‐assemble with both remarkable long‐range regularity and micro‐ and nanoscale specificity to precisely position and stabilize cell adhesion molecules, membrane transporters, ion channels, and other cytoskeletal proteins. To accomplish these generally conserved, but often functionally divergent and spatially diverse, roles these partners use a combinatorial program of a couple of dozens interacting family members, whose code is not fully unraveled. In a departure from their scaffolding roles, ankyrins and spectrins also enable the delivery of material to the plasma membrane by facilitating intracellular transport. Thus, it is unsurprising that deficits in ankyrins and spectrins underlie several neurodevelopmental, neurodegenerative, and psychiatric disorders. Here, I summarize key aspects of the biology of spectrins and ankyrins in the mammalian neuron and provide a snapshot of the latest advances in decoding their roles in the nervous system.

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“…The neurospecific domain interacts with multiple protein partners at the AIS, including GABARAP (35, 36), Nude1/NudeL1 (37), and microtubule end-binding (EB) proteins (23). Humans bearing a R1989W mutation of gAnkG that reduces the affinity for GABARAP by over a 1,000-fold have bipolar symptoms, while mice bearing the same mutation exhibit reduction in GABAergic synapses and hyperexcitability (38).…”

mentioning

confidence: 99%

Neurodevelopmental mutation of giant ankyrin-G disrupts a core mechanism for axon initial segment assembly

Yang

Walder-Christensen

Lalani

et al. 2019

Proc. Natl. Acad. Sci. U.S.A.

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Giant ankyrin-G (gAnkG) coordinates assembly of axon initial segments (AISs), which are sites of action potential generation located in proximal axons of most vertebrate neurons. Here, we identify a mechanism required for normal neural development in humans that ensures ordered recruitment of gAnkG and β4-spectrin to the AIS. We identified 3 human neurodevelopmental missense mutations located in the neurospecific domain of gAnkG that prevent recruitment of β4-spectrin, resulting in a lower density and more elongated pattern for gAnkG and its partners than in the mature AIS. We found that these mutations inhibit transition of gAnkG from a closed configuration with close apposition of N- and C-terminal domains to an extended state that is required for binding and recruitment of β4-spectrin, and normally occurs early in development of the AIS. We further found that the neurospecific domain is highly phosphorylated in mouse brain, and that phosphorylation at 2 sites (S1982 and S2619) is required for the conformational change and for recruitment of β4-spectrin. Together, these findings resolve a discrete intermediate stage in formation of the AIS that is regulated through phosphorylation of the neurospecific domain of gAnkG.

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Ankyrin-G regulates forebrain connectivity and network synchronization via interaction with GABARAP

Cited by 42 publications

References 65 publications

Atg8-Family Proteins—Structural Features and Molecular Interactions in Autophagy and Beyond

Atg8-Family Proteins—Structural Features and Molecular Interactions in Autophagy and Beyond

Cargo hold and delivery: Ankyrins, spectrins, and their functional patterning of neurons

Neurodevelopmental mutation of giant ankyrin-G disrupts a core mechanism for axon initial segment assembly

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