Sorting receptor Rer1 controls surface expression of muscle acetylcholine receptors by ER retention of unassembled α-subunits

Valkova, Christina; Albrizio, Marina; Röder, Ira V.; Schwake, Michael; Betto, Romeo; Rudolf, Rüdiger; Kaether, Christoph

doi:10.1073/pnas.1001624108

Cited by 42 publications

(61 citation statements)

References 23 publications

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“…Stepwise deletion of the complementation construct up to almost C3 (iD⌬62-TM4 to iD⌬67-TM4) resulted in a slight decrease in overall membrane expression. This decrease was coexistent with lower membrane expression of ␣1-trc, again corroborating the concomitant transport of receptor domains from the ER toward the plasma membrane (14,28). Interestingly, the amount of cell surface protein observed for iD⌬67-TM4 was indistinguishable from the other complementation constructs.…”

Section: Discussionsupporting

confidence: 48%

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The Importance of TM3-4 Loop Subdomains for Functional Reconstitution of Glycine Receptors by Independent Domains

Unterer

Becker

Villmann

2012

Journal of Biological Chemistry

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Background: Truncated non-functional GlyRs are reconstituted in channel function by co-expression with a C-terminal domain. Results: TM3-4 loop residues are expressed independently of TM4 and the truncated GlyR. Conclusion: TM4 and the C terminus are not sufficient to rescue GlyR function; rather, residues of the TM3-4 loop are required. Significance: TM3-4 loop residues trigger directly or indirectly conformational changes necessary for GlyR functionality.

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Section: Discussionsupporting

confidence: 48%

“…Functionality of the truncated non-functional GlyR␣1 variant from the mouse mutant oscillator was restored in vitro in HEK293 cells and primary spinal cord neurons by coexpression with an independent complementation domain (28). The restoration of GlyR functionality in the two-domain approach exhibited 50% of wild type activity.…”

Section: Discussionmentioning

confidence: 90%

The Importance of TM3-4 Loop Subdomains for Functional Reconstitution of Glycine Receptors by Independent Domains

Unterer

Becker

Villmann

2012

Journal of Biological Chemistry

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“…Evidence for lysosomal degradation of CHRN comes from studies using iodinated protein flux 45,46 and from the effects of lysosomal inhibitors on CHRN levels in C2C12 muscle cells. 18,47 Given the recent discussions about the physiological roles of TRIM63 in muscle atrophy and the findings of its possible function in the turnover of the CHRN, we focused on this process in more detail.…”

Section: Discussionmentioning

confidence: 99%

Role of autophagy, SQSTM1, SH3GLB1, and TRIM63 in the turnover of nicotinic acetylcholine receptors

et al. 2013

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“…Recently, Rer1, a Golgi-ER retrieval receptor, was demonstrated to control the expression of vertebrate muscle AChRs by ensuring the retention of unassembled subunits in the ER (47). To test the possibility that EMC-6 might also be involved in the control of the ER exit of receptor subunits, we analyzed the UNC-29 glycosylation profile in unc-63(0) and emc-6(kr150) (Fig.…”

Section: Emc-6 Stabilizes L-achr Subunits Before or During Receptormentioning

confidence: 99%

Biosynthesis of ionotropic acetylcholine receptors requires the evolutionarily conserved ER membrane complex

Richard

Boulin

Robert

et al. 2013

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

105

146

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The number of nicotinic acetylcholine receptors (AChRs) present in the plasma membrane of muscle and neuronal cells is limited by the assembly of individual subunits into mature pentameric receptors. This process is usually inefficient, and a large number of the synthesized subunits are degraded by endoplasmic reticulum (ER)-associated degradation. To identify cellular factors required for the synthesis of AChRs, we performed a genetic screen in the nematode Caenorhabditis elegans for mutants with decreased sensitivity to the cholinergic agonist levamisole. We isolated a partial loss-of-function allele of ER membrane protein complex-6 (emc-6), a previously uncharacterized gene in C. elegans. emc-6 encodes an evolutionarily conserved 111-aa protein with two predicted transmembrane domains. EMC-6 is ubiquitously expressed and localizes to the ER. Partial inhibition of EMC-6 caused decreased expression of heteromeric levamisole-sensitive AChRs by destabilizing unassembled subunits in the ER. Inhibition of emc-6 also reduced the expression of homomeric nicotine-sensitive AChRs and GABA A receptors in C. elegans muscle cells. emc-6 is orthologous to the yeast and human EMC6 genes that code for a component of the recently identified ER membrane complex (EMC). Our data suggest this complex is required for protein folding and is connected to ER-associated degradation. We demonstrated that inactivation of additional EMC members in C. elegans also impaired AChR synthesis and induced the unfolded protein response. These results suggest that the EMC is a component of the ER folding machinery. AChRs might provide a valuable proxy to decipher the function of the EMC further.

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Sorting receptor Rer1 controls surface expression of muscle acetylcholine receptors by ER retention of unassembled α-subunits

Cited by 42 publications

References 23 publications

The Importance of TM3-4 Loop Subdomains for Functional Reconstitution of Glycine Receptors by Independent Domains

The Importance of TM3-4 Loop Subdomains for Functional Reconstitution of Glycine Receptors by Independent Domains

Role of autophagy, SQSTM1, SH3GLB1, and TRIM63 in the turnover of nicotinic acetylcholine receptors

Biosynthesis of ionotropic acetylcholine receptors requires the evolutionarily conserved ER membrane complex

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