Nebula/DSCR1 Upregulation Delays Neurodegeneration and Protects against APP-Induced Axonal Transport Defects by Restoring Calcineurin and GSK-3β Signaling

Shaw, Jillian L.; Chang, Karen

doi:10.1371/journal.pgen.1003792

Cited by 31 publications

(47 citation statements)

References 97 publications

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“…AD-associated presenilin 1 mutations and hyperphosphorylated tau have also been shown to induce axonal transport defects through activation of GSK3b [25,96,98]. Correcting fast axonal transport defects by reducing GSK3b activity was found to be beneficial in a Drosophila model of AD [99,100]. Deregulation of Cdk5 is also linked to defects in the slow axonal transport of neurofilaments in AD [77].…”

Section: Amyotrophic Lateral Sclerosis (Als)mentioning

confidence: 99%

Regulation of Axonal Transport by Protein Kinases

Gibbs

Greensmith

Schiavo

2015

Trends in Biochemical Sciences

107

102

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The intracellular transport of organelles, proteins, lipids, and RNA along the axon is essential for neuronal function and survival. This process, called axonal transport, is mediated by two classes of ATP-dependent motors, kinesins, and cytoplasmic dynein, which carry their cargoes along microtubule tracks. Protein kinases regulate axonal transport through direct phosphorylation of motors, adapter proteins, and cargoes, and indirectly through modification of the microtubule network. The misregulation of axonal transport by protein kinases has been implicated in the pathogenesis of several nervous system disorders. Here, we review the role of protein kinases acting directly on axonal transport and discuss how their deregulation affects neuronal function, paving the way for the exploitation of these enzymes as novel drug targets.

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Section: Amyotrophic Lateral Sclerosis (Als)mentioning

confidence: 99%

Regulation of Axonal Transport by Protein Kinases

Gibbs

Greensmith

Schiavo

2015

Trends in Biochemical Sciences

107

102

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“…Therapeutic interventions can be aimed at the specific phosphotransferase activities relevant to AT deficits. Hence, some studies on AD are beginning to focus on investigating proteasome activities; for example, a few recent studies have examined the way proteasomeassociated protein Nedd8 ultimate buster (NUB1)-induced GSK3β degradation [98,99].…”

Section: Development Of Effective Therapies Targeting Atmentioning

confidence: 99%

Axonal Transport Defects in Alzheimer’s Disease

Wang

Tan

2014

Mol Neurobiol

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A large body of evidences indicates that axonal transport (AT) defects play an important role in the pathogenesis of Alzheimer' disease (AD). AT, a critical cellular process for the maintenance and function of a neuron, requires components of the cytoskeletons as "tracks", motor proteins and ATP as "driving force", adaptor proteins to ensure the specific connection of the transported cargoes and motor proteins as well as active regulation. In AD pathology, AD-linked pathologic factors respectively perturb the four basic components of AT through different signaling pathways to cause AT defects. Mitochondrial transport, which is different from other transport cargoes, is also impaired via special pathways in AD. In this paper, we review the inhibitory effects of those factors on AT and their possible pathways, indicating these factors act in overlapping, synergistic, and circulating ways. Given the contributions of AT defects to AD, recent therapeutic studies focus on microtubule-stabilizing (MT-stabilizing) agents and alteration in phosphotransferase activities, and we propose more therapeutic strategies targeting AT defects.

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“…Increases in Et STP may also be related to drug efflux from the cell, which decreases effective intracellular drug concentrations. Indeed, a study by Shaw and Chang () showed that PP2B is involved in axonal transport. The results of these studies and the present study demonstrated that upregulation of Et STP may be related to drug resistance.…”

Section: Discussionmentioning

confidence: 99%

Molecular characterization of serine/threonine protein phosphatase of Eimeria tenella

Zhao

Zhu

et al. 2020

J Eukaryotic Microbiology

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Avian coccidiosis is a widespread and economically significant poultry disease caused by several Eimeria species, including Eimeria tenella. Previously, E. tenella serine/threonine protein phosphatase (EtSTP) was found to be differentially expressed in drug‐sensitive (DS) and drug‐resistant strains using RNA‐seq. In the present study, we found that transcription and translation levels of EtSTP were higher in diclazuril‐resistant (DZR) strains and maduramicin‐resistant (MRR) strains than in DS strains using quantitative real‐time PCR (qPCR) and Western blotting. Enzyme activity results indicated that the catalytic activity of EtSTP was higher in the two drug‐resistant strains than in DS strains. Western blot and qPCR analysis also showed that expression levels of EtSTP were higher in unsporulated oocysts (UO) and second‐generation merozoites (SM). Indirect immunofluorescence localization showed that EtSTP was located in most areas of the parasite with the exception of refractile bodies, and fluorescence intensity was enhanced during development. In vitro inhibition experiments showed that the ability of sporozoites (SZ) to invade cells was significantly decreased after treatment with anti‐rEtSTP antibody. These results indicated that EtSTP acted mainly during the developmental and reproductive stages of the parasite and may be related to the resistance of coccidia to external drug pressure.

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Nebula/DSCR1 Upregulation Delays Neurodegeneration and Protects against APP-Induced Axonal Transport Defects by Restoring Calcineurin and GSK-3β Signaling

Cited by 31 publications

References 97 publications

Regulation of Axonal Transport by Protein Kinases

Regulation of Axonal Transport by Protein Kinases

Axonal Transport Defects in Alzheimer’s Disease

Molecular characterization of serine/threonine protein phosphatase of Eimeria tenella

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