RIC-3 expression and splicing regulate nAChR functional expression

Ben-David, Yael; Mizrachi, Tehila; Kagan, Sarah; Krisher, Tamar; Cohen, Emiliano; Brenner, Talma; Treinin, Millet

doi:10.1186/s13041-016-0231-5

Cited by 23 publications

(34 citation statements)

References 33 publications

(41 reference statements)

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“…This together with the known role of RIC-3 in α7 nAChR maturation suggests that RIC3 variants may affect MS via their effects on α7 nAChR maturation in immune cells. Importantly, we demonstrated that ric3 expression in immune cells is dynamically regulated following immune activation 31 . Moreover, recent unpublished results show that ric3 expression is transiently reduced in splenocytes and is gradually reduced in spinal cords during EAE progression (Yael BenDavid, unpublished).…”

Section: Ric-3 and Diseases Of The Central Nervous Systemmentioning

confidence: 95%

“…. Recently we showed that these opposite effects on nAChR expression can be achieved using different RIC-3-toreceptor ratios, and that sensitivity of nAChR maturation to this ratio depends on the identity of the nAChR and on the specific RIC-3 isoform (different isoforms are produced by alternative splicing, see below) 31 . Second, RIC-3 was shown to affect different aspects of nAChR maturation depending on identity of the receptor's subunits.…”

Section: Maturation Of Nachrs and The Ric-3 Proteinmentioning

confidence: 99%

“…First, RIC-3 was shown to have either positive or negative effects on co-expressed receptors depending on the RIC-3-to-receptor ratio 31 . Thus mechanisms regulating RIC-3 expression or stability are likely to regulate cholinergic signaling via nAChRs.…”

Section: Mechanisms Regulating Ric-3 Expression and Activity And Theimentioning

confidence: 99%

“…One conserved alternatively spliced RIC-3 isoform, lacking the conserved C-terminal coiled-coil domain, is defective for either the positive or negative effects of RIC-3 in a nAChR subtype dependent manner 31 .…”

Section: Mechanisms Regulating Ric-3 Expression and Activity And Theimentioning

confidence: 99%

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RIC-3, a potential target for regulating cholinergic signaling and inflammation

Treinin¹

2017

J Immunological Sci

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The nic�� acetylcholine receptor (nAChR) gene family encodes for subunits of acetylcholine gated ion channels. These receptors are expressed widely and have many �� including an�� tory e� ects mediated by the α7 nAChR, as part of the cholinergic an�� tory pathway, in immune cells, microglia and astrocytes. Matura�� of α7 nAChRs into �� ligand-gated ion channels in the plasma membrane is a complex process likely to require the RIC-3 protein. This endoplasmic re�� resident chaperone a� ects matura�� of �� nAChRs, but its inter�� with these receptors and its e� ects on their matura�� er for �� erent nAChRs. Moreover, these inter�� and e� ects are regulated by �� mechanisms. Gene�� analysis has implicated RIC-3 in the neuroin��tory disease �� Sclerosis (MS), and in the neurodegenera� e Parkinson's disease (PD). Neuroin�� contributes to the progression of neurodegenera� e diseases including PD. This informa�� combines to suggest that RIC-3 may contribute to progression of both MS and PD via its e� ects on the α7 nAChR and the cholinergic an� in��tory pathway. Furthermore, we suggest that mechanisms regula�� RIC-3 expr�� y have a role in controlling in�� The nicotinic acetylcholine receptor familyThe nicotinic acetylcholine receptors (nAChRs) are a large and diverse family of acetylcholine-gated ion channels. In mammals this family is composed of nine alpha subunits and seven non-alpha subunits. These subunits assemble to form mostly heteromeric (α7 and α9 nAChR subunits can form homomeric receptors), cation-selective channels having diverse properties and expression patterns. In skeletal-muscles and in the autonomic nervous system nAChRs mediate excitatory synaptic transmission. However, in the central nervous system (CNS) nAChRs do not usually mediate synaptic transmission and instead play modulatory roles, including a role in regulating neurotransmitter release, reviewed by Dani and Bertrand 1. In addition to being expressed in muscles and neurons, nAChRs are also found in multiple types of non-excitable cells where they affect migration, differentiation, proliferation, and signal transduction 2 .CNS-expressed nAChRs have been implicated in memory, cognition, addiction, and several neurodegenerative diseases. Evidence for these functions comes from the addictive effects of tobacco-derived nicotine and from epidemiological studies linking tobacco smoking to neurodegenerative diseases such as schizophrenia and Parkinson's disease (reviewed by Dani and

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Section: Ric-3 and Diseases Of The Central Nervous Systemmentioning

confidence: 95%

Section: Maturation Of Nachrs and The Ric-3 Proteinmentioning

confidence: 99%

Section: Mechanisms Regulating Ric-3 Expression and Activity And Theimentioning

confidence: 99%

Section: Mechanisms Regulating Ric-3 Expression and Activity And Theimentioning

confidence: 99%

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RIC-3, a potential target for regulating cholinergic signaling and inflammation

Treinin¹

2017

J Immunological Sci

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“…This regulation of RIC-3 expression and splicing is likely to have functional implications as electrophysiology results, summarized above, show either positive or negative effects of RIC- 3 on nAChR expression, depending on RIC-3 expression level, specific RIC-3 isoform, and specific nAChR [5]. …”

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confidence: 99%

Regulation of RIC-3 and of nAChR expression

Ben-David¹,

Treinin²

2016

Oncotarget

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Two residues determine nicotinic acetylcholine receptor requirement for RIC‐3

Noonan

Beech

2023

Protein Science

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Nicotinic acetylcholine receptors (N‐AChRs) mediate fast synaptic signalling and are members of the pentameric ligand‐gated ion channel (pLGIC) family. They rely on a network of accessory proteins in vivo for correct formation and transport to the cell surface. RIC‐3 is an endoplasmic reticulum protein that physically interacts with nascent pLGIC subunits and promotes their oligomerization. It is not known why some N‐AChRs require RIC‐3 in heterologous expression systems, while others do not. Previously we reported that the ACR‐16 N‐AChR from the parasitic nematode Dracunculus medinensis does not require RIC‐3 in Xenopus laevis oocytes. This is unusual because all other nematode ACR‐16, like the closely related Ascaris suum ACR‐16, require RIC‐3. Their high sequence similarity limits the number of amino acids that may be responsible, and the goal of this study was to identify them. A series of chimeras and point mutations between A. suum and D. medinensis ACR‐16, followed by functional characterization with electrophysiology, identified two residues that account for a majority of the receptor requirement for RIC‐3. ACR‐16 with R/K159 in the cys‐loop and I504 in the C‐terminal tail did not require RIC‐3 for functional expression. Mutating either of these to R/K159E or I504T, residues found in other nematode ACR‐16, conferred a RIC‐3 requirement. Our results agree with previous studies showing that these regions interact and are involved in receptor synthesis. Although it is currently unclear what precise mechanism they regulate, these residues may be critical during specific subunit folding and/or assembly cascades that RIC‐3 may promote.This article is protected by copyright. All rights reserved.

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RIC-3 expression and splicing regulate nAChR functional expression

Cited by 23 publications

References 33 publications

RIC-3, a potential target for regulating cholinergic signaling and inflammation

RIC-3, a potential target for regulating cholinergic signaling and inflammation

Regulation of RIC-3 and of nAChR expression

Two residues determine nicotinic acetylcholine receptor requirement for RIC‐3

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