2014
DOI: 10.1111/tra.12237
|View full text |Cite
|
Sign up to set email alerts
|

Molecular Insights into Rab7‐Mediated Endosomal Recruitment of Core Retromer: Deciphering the Role of Vps26 and Vps35

Abstract: Retromer, a peripheral membrane protein complex, plays an instrumental role in host of cellular processes by its ability to recycle receptors from endosomes to the trans-Golgi network. It consists of two distinct sub-complexes, a membrane recognizing, sorting nexins (SNX) complex and a cargo recognition, vacuolar protein sorting (Vps) complex. Small

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
1
1
1
1

Citation Types

2
59
1

Year Published

2015
2015
2022
2022

Publication Types

Select...
5
2
1

Relationship

0
8

Authors

Journals

citations
Cited by 70 publications
(62 citation statements)
references
References 63 publications
(119 reference statements)
2
59
1
Order By: Relevance
“…Our data show that although the core complex remains unaffected by the P316S, the R524W mutation partially disrupts this formation and also negatively impacts the association with regulatory molecules needed for cargo sorting. Previously, Vps35-Rab7a-SNX3 interaction studies demonstrated that binding of Rab7a and SNX3 is within the first 300 amino acids of Vps35 and immediately adjacent to the Vps26-Vps35 interface (41). Despite this, we showed that R524W, but not the P316S mutation within Vps35, severely impacts the retromerRab7a interaction and Vps35 R524W-retromer membrane association, coupled with reduced interactions with the WASH complex subunit FAM21, the RabGAP TBC1D5, and PDZ motif cargo adaptor SNX27.…”
Section: Vps35 R524w Mutation Impairs the Function Of Retromercontrasting
confidence: 48%
“…Our data show that although the core complex remains unaffected by the P316S, the R524W mutation partially disrupts this formation and also negatively impacts the association with regulatory molecules needed for cargo sorting. Previously, Vps35-Rab7a-SNX3 interaction studies demonstrated that binding of Rab7a and SNX3 is within the first 300 amino acids of Vps35 and immediately adjacent to the Vps26-Vps35 interface (41). Despite this, we showed that R524W, but not the P316S mutation within Vps35, severely impacts the retromerRab7a interaction and Vps35 R524W-retromer membrane association, coupled with reduced interactions with the WASH complex subunit FAM21, the RabGAP TBC1D5, and PDZ motif cargo adaptor SNX27.…”
Section: Vps35 R524w Mutation Impairs the Function Of Retromercontrasting
confidence: 48%
“…Rab7 is known to recruit the retromer on endosomal membrane, and it is required for the transfer of cargo from the late endosomes to the lysosome (Priya et al, 2015;Pryor and Luzio, 2009). A conserved function of WASH in retromer-dependent endocytic recycling of the luminal protein Serpentine has already been found during Drosophila trachea development (Dong et al, 2013).…”
Section: Research Articlementioning
confidence: 99%
“…Our data shows that although the core complex remains unaffected by the P316S and R524W mutations, the association with regulatory molecules is significantly altered in the presence of Vps35 R524W mutation. Previously, Vps35-Rab7a-SNX3 interaction interface studies demonstrated that binding of Rab7a and SNX3 is within the first 300 amino acids of Vps35 and immediately adjacent to the Vps26-Vps35 interface [101]. Despite this, we showed that R524W but not the P316S mutation within Vps35 severely impacts the retromer-Rab7a interaction and Vps35 R524W-retromer membrane association, coupled with reduced interactions with the WASH complex subunit FAM21, the RabGAP TBC1D5 and PDZ motif cargo adaptor SNX27.…”
Section: Discussionmentioning
confidence: 46%
“…Consistent with this study, this thesis shows that use of R55 increased the total Vps35 protein level and limited the formation of α-synuclein inclusions, even following the stable loss of retromer using a shRNA system (See section Though the underlying mechanism as to why Vps35 R524W does not interact with most of the known interacting partners was not described in this thesis, the loss of Vps35 R524W-retromer's membrane association may be explained by the previous in vitro study which characterized a conformational shift within the complex at the initial stages of the trimer formation [277]. Given that the formation of the retromer trimer is a prerequisite for its interaction with both Rab7A and the endosomal membrane [101,276], one explanation for the observations reported here could be influenced by the capacity of the Vps35 R524W-retromer to undergo this conformational change, rather than impacting on the binding Additionally, whether the trafficking defect observed following the expression of Vps35 D620N could be rescued following incubation with R55 is currently unknown.…”
Section: Pharmacological Modulators Of Retromermentioning
confidence: 95%
See 1 more Smart Citation