Neuronal Chloride Regulation via KCC2 Is Modulated through a GABA<sub>B</sub>Receptor Protein Complex

Wright, Rebecca A.; Newey, Sarah E.; Ilie, Andrei; Wefelmeyer, Winnie; Raimondo, Joseph V.; Ginham, Rachel; Mcllhinney, R.A. Jeffrey; Akerman, Colin J.

doi:10.1523/jneurosci.2164-16.2017

Cited by 49 publications

(53 citation statements)

References 80 publications

(160 reference statements)

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“…The 800 kDa complex also contained a prominent subnetwork of proteins associated with synaptic signaling and organization (GABBR1, GABBR2, GRM2, and GRM3). Importantly, the GABAB receptor has previously been demonstrated to interact with KCC2 directly (35), which further substantiates our findings. For approximately half of the proteins in both the 600 and 800 kDa complexes, there were no known interactors other than KCC2.…”

Section: Analyzing the Composition Of Stable Protein Complexes Of Kcc2supporting

confidence: 90%

“…This could be either due the transient or low affinity nature of these interactions, or that these interactors are less abundant in complex with KCC2 than the interactors presented here, as unbiased methodologies provide information on associated proteins in rank order of abundance. LC-MS/MS further confirmed the veracity of our purification strategy as these high molecular weight species contained GABABRs, which has been previously shown to be associated with KCC2 (35). Interestingly we identified gephyrin associated with KCC2 in the 800 kDa band along with CYFIP1/2, NCKAP1 and CNTN1 and other proteins that are enriched at inhibitory synapses (51,52).…”

Section: Discussionsupporting

confidence: 80%

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The K-Cl co-transporter 2 is a point of convergence for multiple autism spectrum disorder and epilepsy risk gene products

Smalley

Kontou

Choi

et al. 2020

Preprint

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KCC2 plays a critical role in determining the efficacy of synaptic inhibition and deficits in its activity lead to epilepsy and neurodevelopmental delay. Here we use unbiased proteomic analyses to demonstrate that KCC2 forms stable protein complexes in the neuronal plasma membrane with 96 autism and/or epilepsy risk gene (ASD/Epi) products including ANKB, ANKG, CNTN1, ITPR1, NCKAP1, SCN2A, SHANK3, SPTAN1, and SPTBN1. Many of these proteins are also targets of Fragile-X mental retardation protein (FMRP), the inactivation of which is the leading monogenic cause of autism. Accordingly, the expression of a subset of these KCC2-binding partners was decreased in Fmr1 knockout mice. Fmr1 knockout compromised KCC2 phosphorylation, a key regulatory mechanism for transporter activity and the postnatal development of GABAergic inhibition. Thus, KCC2 is a point of convergence for multiple ASD/Epi risk genes and therapies targeting this transporter may have broad utility in alleviating these heterogeneous disorders and their associated epilepsies.

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Section: Analyzing the Composition Of Stable Protein Complexes Of Kcc2supporting

confidence: 90%

Section: Discussionsupporting

confidence: 80%

The K-Cl co-transporter 2 is a point of convergence for multiple autism spectrum disorder and epilepsy risk gene products

Smalley

Kontou

Choi

et al. 2020

Preprint

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“…We then investigated the mechanisms underlying Task-3 down-regulation upon KCC2 silencing. KCC2 has been shown to interact with a variety of proteins, including transmembrane proteins such as GluK2 44 , Neto2 45 and GABA B receptors 46 that regulate KCC2 membrane expression or the intracellular guanylyl exchange factor β PIX which is regulated through direct interaction with KCC2 35,36 . We therefore asked whether KCC2 might also interact with Task-3 channels and thereby influence their membrane expression and/or function.…”

Section: Resultsmentioning

confidence: 99%

“…KCC2 interacts with a variety of transmembrane as well as intracellular partners, including postsynaptic receptors 44,45,46 , actin-related proteins 34,35,36 and others involved in protein trafficking and recycling 37 . Although these interactions are most often considered with regard to KCC2 expression or function, they also influence the function of KCC2 partners.…”

Section: Discussionmentioning

confidence: 99%

KCC2 regulates neuronal excitability and hippocampal activity via interaction with Task-3 channels

Goutierre

Awabdh

François

et al. 2018

Preprint

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The K + /Cl − co-transporter KCC2 (SLC12A5) regulates neuronal transmembrane chloride gradients and thereby controls GABA signaling in the brain. KCC2 downregulation is observed in several neurological and psychiatric disorders including epilepsy, neuropathic pain and autism spectrum disorders. Paradoxical, excitatory GABA signaling is usually assumed to contribute to abnormal network activity underlying the pathology. We tested this hypothesis and explored the functional impact of chronic KCC2 downregulation in the rat dentate gyrus. Although the reversal potential of GABAA receptor currents was depolarized in KCC2 knockdown neurons, this shift was fully compensated by depolarization of their resting membrane potential. This effect was due to downregulation of Task-3 leak potassium channels that we show require KCC2 for membrane trafficking. Increased neuronal excitability upon KCC2 suppression altered dentate gyrus rhythmogenesis that could be normalized by chemogenetic hyperpolarization. Our data reveal KCC2 downregulation engages complex synaptic and cellular alterations beyond GABA signaling that concur to perturb network activity, thus offering novel targets for therapeutic intervention.

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“…Rat organotypic hippocampal slice cultures were prepared using a method similar to that described (40,41) and that KCC2 is the major active Cltransporter in these neurons as EGABA is affected by KCC2-blocking drugs, but not by NKCC1-blocking drugs (42).…”

Section: Methodsmentioning

confidence: 99%

Chloride dynamics alter the input-output properties of neurons

Currin

Trevelyan

Akerman

et al. 2019

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Fast synaptic inhibition is a critical determinant of neuronal output, with subcellular targeting of synaptic inhibition able to exert different transformations of the neuronal input-output function. At the receptor level, synaptic inhibition is primarily mediated by chloride-permeable Type A GABA receptors. Consequently, dynamics in the neuronal chloride concentration can alter the functional properties of inhibitory synapses. How differences in the spatial targeting of inhibitory synapses interact with intracellular chloride dynamics to modulate the input-output function of neurons is not well understood. To address this, we developed computational models of multi-compartment neurons that incorporate experimentally parametrised mechanisms to account for neuronal chloride influx, diffusion, and extrusion. We found that synaptic input (either excitatory, inhibitory, or both) can lead to subcellular variations in chloride concentration, despite a uniform distribution of chloride extrusion mechanisms. Accounting for chloride changes resulted in substantial alterations in the neuronal inputoutput function. This was particularly the case for peripherally targeted dendritic inhibition where dynamic chloride compromised the ability of inhibition to offset neuronal input-output curves. Our simulations revealed that progressive changes in chloride concentration mean that the neuronal input-output function is not static but varies significantly as a function of the duration of synaptic drive. Finally, we found that the observed effects of dynamic chloride on neuronal output were entirely mediated by changes in the dendritic reversal potential for GABA. Our findings provide a framework for understanding the computational effects of chloride dynamics on dendritically targeted synaptic inhibition. Author SummaryThe fundamental unit of computation in the brain is the neuron, whose output reflects information within the brain. A determining factor in the transfer and processing of information in the brain is the modulation of activity by inhibitory synaptic inputs. Fast synaptic inhibition is mediated by the neurotransmitter GABA binding to GABAA receptors, which are permeable to chloride ions. How changes in chloride ion concentration affect neuronal output is an important consideration for information flow in the brain that is currently not being thoroughly investigated. In this research, we used multi-compartmental models of neurons to link the deleterious effects that accumulation of chloride ions can have on inhibitory signalling with changes in neuronal ouput. Together, our results highlight the importance of accounting for changes in chloride concentration in theoretical and computer-based models that seek to explore the computational properties of inhibition.

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Neuronal Chloride Regulation via KCC2 Is Modulated through a GABA_BReceptor Protein Complex

Cited by 49 publications

References 80 publications

The K-Cl co-transporter 2 is a point of convergence for multiple autism spectrum disorder and epilepsy risk gene products

The K-Cl co-transporter 2 is a point of convergence for multiple autism spectrum disorder and epilepsy risk gene products

KCC2 regulates neuronal excitability and hippocampal activity via interaction with Task-3 channels

Chloride dynamics alter the input-output properties of neurons

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Neuronal Chloride Regulation via KCC2 Is Modulated through a GABABReceptor Protein Complex

Cited by 49 publications

References 80 publications

The K-Cl co-transporter 2 is a point of convergence for multiple autism spectrum disorder and epilepsy risk gene products

The K-Cl co-transporter 2 is a point of convergence for multiple autism spectrum disorder and epilepsy risk gene products

KCC2 regulates neuronal excitability and hippocampal activity via interaction with Task-3 channels

Chloride dynamics alter the input-output properties of neurons

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Neuronal Chloride Regulation via KCC2 Is Modulated through a GABA_BReceptor Protein Complex