2014
DOI: 10.1016/j.cub.2014.07.004
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Retromer Binding to FAM21 and the WASH Complex Is Perturbed by the Parkinson Disease-Linked VPS35(D620N) Mutation

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Cited by 44 publications
(49 citation statements)
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“…Similar trafficking defects on CI-M6PR have been reported in cell-based models expressing PD-causing retromer variant Vps35 D620N. This variant is assembled into the retromer complex correctly, however, the presence of Vps35 D620N alters the intracellular distribution of CI-M6PR and leads to an elevation of procathepsin D in various cell types including fibroblast cells isolated from PD patients carrying Vps35 D620N variant [76,85,86]. Recent work reported an additional variant, Vps35 R524W, is also associated with the sorting defects of CI-M6PR.…”
Section: Impaired Endolysosomal-mediated Protein Degradationsupporting
confidence: 67%
“…Similar trafficking defects on CI-M6PR have been reported in cell-based models expressing PD-causing retromer variant Vps35 D620N. This variant is assembled into the retromer complex correctly, however, the presence of Vps35 D620N alters the intracellular distribution of CI-M6PR and leads to an elevation of procathepsin D in various cell types including fibroblast cells isolated from PD patients carrying Vps35 D620N variant [76,85,86]. Recent work reported an additional variant, Vps35 R524W, is also associated with the sorting defects of CI-M6PR.…”
Section: Impaired Endolysosomal-mediated Protein Degradationsupporting
confidence: 67%
“…29 A rare missense mutation of VPS35, p.Asp620Asn (D620N), has been found to cause Parkinson disease and results in impaired association of the retromer cargo-selective subcomplex with the WASH complex. 30,31 The L625P mutation is located in the VPS35 C-terminal domain involved in VPS29 binding, similar to the D620N missense mutation. When HeLa cells were transiently transfected with a GFP-tagged VPS35 L625P mutant, the mutation reduced the amount of VPS29 that co-immunoprecipitates with the tagged VPS35 (Figure 2), although the effect was not as pronounced as that of the H675R mutation, a mutation initially characterized in Saccharomyces Cerevisiae that totally abolishes the binding to VPS29.…”
Section: Resultsmentioning
confidence: 98%
“…In these cases, depletion of retromer contributes to neurodegeneration through impaired endolysosomal trafficking of certain enzymes responsible for the generation or clearance of aggregation-prone proteins; BACE1, a protease responsible for β-amyloid production in Alzheimer's disease and cathepsin D, the main lysosomal enzyme for α-synuclein degradation in Parkinson's disease, respectively (62,63). Additionally, the D620 mutant, Parkinson's disease-linked form of Vps35 is the subject of intensive research, however data from various groups are contradictory regarding the loss-or gain-of-function nature of this allele and its exact effects on intracellular trafficking (64,65). It is evident though that this mutant allele does not represent a null mutation, but it has serious effects on neurotransmitter receptor trafficking in vitro and causes neurodegeneration and loss of locomotor activity in vivo (66)(67)(68).…”
Section: Figure 8: Function Of Retromer In Normal Cells (A) and The Ementioning
confidence: 99%