2021
DOI: 10.3390/cells10081865
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The Link between VAPB Loss of Function and Amyotrophic Lateral Sclerosis

Abstract: The VAP proteins are integral adaptor proteins of the endoplasmic reticulum (ER) membrane that recruit a myriad of interacting partners to the ER surface. Through these interactions, the VAPs mediate a large number of processes, notably the generation of membrane contact sites between the ER and essentially all other cellular membranes. In 2004, it was discovered that a mutation (p.P56S) in the VAPB paralogue causes a rare form of dominantly inherited familial amyotrophic lateral sclerosis (ALS8). The mutant p… Show more

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Cited by 28 publications
(28 citation statements)
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References 212 publications
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“…We proposed that the overexpression of the parkin protein, especially through its ubiquitin ligase activity, favors neuroprotection after uncontrolled dysregulation of mitochondrial Ca 2+ levels. MAM collapse is a common pathogenesis mechanism in ALS linked to SIGMAR1, SOD1, VAPB, TARDBP, and FUS [78,79]. When analyzing ER mitochondria calcium cycle dynamics (ERMCC) in murine model swith hSOD1-G93A (overexpressing mutant) MNs-as a model for ALS-with sub-sector resolution, using fluorescent calcium imaging, and comparing vulnerable MNs and non-neurons from hSOD1-G93A mice with their non-transgenic littermates, decelerated clearance of cytosolic calcium was associated with hSOD1-G93A.…”
Section: The Subcellular Communication Between Organelles Especially Mitochondrial-associated-membrane (Mams) Modulates Ion Currents and mentioning
confidence: 99%
“…We proposed that the overexpression of the parkin protein, especially through its ubiquitin ligase activity, favors neuroprotection after uncontrolled dysregulation of mitochondrial Ca 2+ levels. MAM collapse is a common pathogenesis mechanism in ALS linked to SIGMAR1, SOD1, VAPB, TARDBP, and FUS [78,79]. When analyzing ER mitochondria calcium cycle dynamics (ERMCC) in murine model swith hSOD1-G93A (overexpressing mutant) MNs-as a model for ALS-with sub-sector resolution, using fluorescent calcium imaging, and comparing vulnerable MNs and non-neurons from hSOD1-G93A mice with their non-transgenic littermates, decelerated clearance of cytosolic calcium was associated with hSOD1-G93A.…”
Section: The Subcellular Communication Between Organelles Especially Mitochondrial-associated-membrane (Mams) Modulates Ion Currents and mentioning
confidence: 99%
“…They also participate in the unfolded protein response machine, an ER activity that suppresses accumulation of misfolded proteins to maintain cell viability and function [188]. VAPB has been connected to various neurodegenerative diseases, including ALS [189,190]. Indeed, several mutations of the VAPB gene have been observed in patients with ALS, such as P56S, T46I, del160, D130E, A145V, S160∆, and V234I [58,[191][192][193].…”
Section: Rodents Carrying Vesicle-associated Membrane Protein (Vamp)-associated Protein B Mutationsmentioning
confidence: 99%
“…Hereditary Spastic Paraplegias Spastin [279] ER tubule regulation [17], ER-endosome MCS [177] Endosomal fission fails at MCS [177] Protrudin [280] ER membrane curvature and tubule fission [281], ER-endosome MCS [204], ER MCS-dependent endosome maturation [125] ER morphology and function dysregulated [225,281] Seipin [282] ER-lipid droplet MCS [283] Axon regeneration impaired [284] Atlastin-1 [285] ER membrane fusion [5] ER morphology dysregulated [17] REEP1 [286] ER membrane curvature [2], ER-mitochondria MCS [106] ER-mitochondria interactions disrupted [106] REEP2 [287] ER membrane curvature regulation [2] ER morphology disrupted [288] KIF5A [195] ER dynamics via kinesin-1 [195] Impaired axonal transport [195] Amyotrophic Lateral Sclerosis VAPB [289] MCS between ER and many organelles (reviewed [290,291]) ER morphology dysregulated [292][293][294][295], ER-mitochondria MCS [296,297],interactions between VAPB and oxysterol binding protein (OSBP) perturbed [298] Reticulon 4 [299] ER membrane curvature [2] Chaperone protein disulfide isomerase (PDI) distribution altered [299] Sigma-1 Receptor [300]<...>…”
Section: Disease Protein Implicated Protein Role In Healthy Er Function Affected In Diseasementioning
confidence: 99%
“…Mutations in KIF5A could conceivably affect this pathway. The disruption of ER–endosomal interactions also affects endosomal sorting and leads to lysosomal defects ( Section 2.2 .6 and 3.1.2), and this is frequently linked to diseases such as HSP and ALS ( Table 1 ), where it can be caused by mutations in spastin, strumpelin, REEP1 [ 177 ], and VAPB, as described elsewhere in this special issue [ 291 ].…”
Section: Morphology Dynamics and Diseasementioning
confidence: 99%
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