GABARAPs dysfunction by autophagy deficiency in adolescent brain impairs GABA _A receptor trafficking and social behavior

Abstract: Dysfunctional mTOR signaling is associated with the pathogenesis of neurodevelopmental and neuropsychiatric disorders. However, it is unclear what molecular mechanisms and pathogenic mediators are involved and whether mTOR-regulated autophagy continues to be crucial beyond neurodevelopment. Here, we selectively deleted Atg7 in forebrain GABAergic interneurons in adolescent mice and unexpectedly found that these mice showed a set of behavioral deficits similar to Atg7 deletion in forebrain excitatory neurons. B… Show more

“…The present data indicate a novel physiological role for autophagy in regulating GABAergic signaling, providing a potential mechanism for the reduced inhibitory inputs observed in neurodevelopmental and neurological disorders such as epilepsy and autism [26]. These findings have bridged the gap between mTOR, autophagy, and GABAergic signaling, which started to emerge in 2009 when the role of autophagy in GABA A receptor trafficking was first demonstrated [51].…”

“…This occurs, for instance, through degradation and turnover of both pre-and post-synaptic substrates, including synaptic vesicles, scaffold proteins, and neurotransmitter receptors [23][24][25]. In keeping with this, failure of mTOR-dependent autophagy was recently shown to promote aberrant synaptic clustering of GABA A receptors and subsequent imbalance of excitation-inhibition in the brain, which might be key for epileptogenesis [26]. Alterations in mTOR-dependent autophagy are also implicated in abnormal dopamine system activity, which is implicated in epileptogenesis as well [27].…”

“…In a similar fashion, autophagy suppression due to TSC2-related mTOR hyperactivation disrupts the trafficking of GABA A receptors via the sequestration of γ-aminobutyric acid receptor-associated proteins (GABARAPs) by p62-positive aggregates [26]. Such an effect is reproduced by autophagy deficiency following either ATG7 or ULK2 deletion in forebrain inhibitory or excitatory neurons [26,49].…”

“…In a similar fashion, autophagy suppression due to TSC2-related mTOR hyperactivation disrupts the trafficking of GABA A receptors via the sequestration of γ-aminobutyric acid receptor-associated proteins (GABARAPs) by p62-positive aggregates [26]. Such an effect is reproduced by autophagy deficiency following either ATG7 or ULK2 deletion in forebrain inhibitory or excitatory neurons [26,49]. In fact, beyond LC3, proteins belonging to the GABARAP family have been shown to be involved in the trafficking of GABA A receptors to the neuronal plasma membrane, and they also have numerous binding partners that are involved in synapse formation, maintenance, and plasticity [23,50].…”

mTOR-Related Cell-Clearing Systems in Epileptic Seizures, an Update

“…The present data indicate a novel physiological role for autophagy in regulating GABAergic signaling, providing a potential mechanism for the reduced inhibitory inputs observed in neurodevelopmental and neurological disorders such as epilepsy and autism [26]. These findings have bridged the gap between mTOR, autophagy, and GABAergic signaling, which started to emerge in 2009 when the role of autophagy in GABA A receptor trafficking was first demonstrated [51].…”

“…This occurs, for instance, through degradation and turnover of both pre-and post-synaptic substrates, including synaptic vesicles, scaffold proteins, and neurotransmitter receptors [23][24][25]. In keeping with this, failure of mTOR-dependent autophagy was recently shown to promote aberrant synaptic clustering of GABA A receptors and subsequent imbalance of excitation-inhibition in the brain, which might be key for epileptogenesis [26]. Alterations in mTOR-dependent autophagy are also implicated in abnormal dopamine system activity, which is implicated in epileptogenesis as well [27].…”

“…In a similar fashion, autophagy suppression due to TSC2-related mTOR hyperactivation disrupts the trafficking of GABA A receptors via the sequestration of γ-aminobutyric acid receptor-associated proteins (GABARAPs) by p62-positive aggregates [26]. Such an effect is reproduced by autophagy deficiency following either ATG7 or ULK2 deletion in forebrain inhibitory or excitatory neurons [26,49].…”

“…In a similar fashion, autophagy suppression due to TSC2-related mTOR hyperactivation disrupts the trafficking of GABA A receptors via the sequestration of γ-aminobutyric acid receptor-associated proteins (GABARAPs) by p62-positive aggregates [26]. Such an effect is reproduced by autophagy deficiency following either ATG7 or ULK2 deletion in forebrain inhibitory or excitatory neurons [26,49]. In fact, beyond LC3, proteins belonging to the GABARAP family have been shown to be involved in the trafficking of GABA A receptors to the neuronal plasma membrane, and they also have numerous binding partners that are involved in synapse formation, maintenance, and plasticity [23,50].…”

mTOR-Related Cell-Clearing Systems in Epileptic Seizures, an Update

“…As recently reviewed, dysfunctional autophagy at both pre-and post-synaptic sites leads to aging and neurodegeneration (Nikoletopoulou et al, 2015;Vijayan and Verstreken, 2017;Azarnia Tehran et al, 2018;Liang and Sigrist, 2018). Degradation of postsynaptic neurotransmitter receptors involves trafficking in autophagosomal structures (Rowland, 2006;Shehata et al, 2012Shehata et al, , 2018Hui et al, 2019). At dopaminergic presynaptic sites, autophagy shapes synapse ultrastructure and modulates neurotransmitter release, while at glutamatergic synapses mTOR-regulated autophagy promotes spine pruning during development (Hernandez et al, 2012;Tang et al, 2014).…”

Emerging Role of the Autophagy/Lysosomal Degradative Pathway in Neurodevelopmental Disorders With Epilepsy

Involvement of Autophagic Machinery in Neuropathogenesis: Targeting and Relevant Methods of Detection