Conservation of a Glycine-rich Region in the Prion Protein Is Required for Uptake of Prion Infectivity

Harrison, Christopher F.; Lawson, Victoria; Coleman, Bradley M.; Kim, Yong‐Sun; Masters, Colin L.; Cappai, Roberto; Barnham, Kevin J.; Hill, Andrew F.

doi:10.1074/jbc.m109.093310

Cited by 40 publications

(55 citation statements)

References 67 publications

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“…This region (residues 268 to 315) is particularly glycine rich (Fig. 8a), with multiple putative GXXXG motifs; these motifs are believed to mediate hydrophobic helical protein-protein interactions and have also been found in other proteins involved in neurodegenerative disorders (13,40). We should also note that while sorbitol can be an oxidative stressor (Fig.…”

Section: Discussionmentioning

confidence: 93%

TDP-43 Is Directed to Stress Granules by Sorbitol, a Novel Physiological Osmotic and Oxidative Stressor

Dewey

Cenik

Sephton

et al. 2011

Molecular and Cellular Biology

299

306

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TDP-43, or TAR DNA-binding protein 43, is a pathological marker of a spectrum of neurodegenerative disorders, including amyotrophic lateral sclerosis and frontotemporal lobar degeneration with ubiquitinpositive inclusions. TDP-43 is an RNA/DNA-binding protein implicated in transcriptional and posttranscriptional regulation. Recent work also suggests that TDP-43 associates with cytoplasmic stress granules, which are transient structures that form in response to stress. In this study, we establish sorbitol as a novel physiological stressor that directs TDP-43 to stress granules in Hek293T cells and primary cultured glia. We quantify the association of TDP-43 with stress granules over time and show that stress granule association and size are dependent on the glycine-rich region of TDP-43, which harbors the majority of pathogenic mutations. Moreover, we establish that cells harboring wild-type and mutant TDP-43 have distinct stress responses: mutant TDP-43 forms significantly larger stress granules, and is incorporated into stress granules earlier, than wild-type TDP-43; in striking contrast, wild-type TDP-43 forms more stress granules over time, but the granule size remains relatively unchanged. We propose that mutant TDP-43 alters stress granule dynamics, which may contribute to the progression of TDP-43 proteinopathies.TAR DNA-binding protein 43 (TDP-43) is a highly conserved, ubiquitously expressed RNA-binding protein of the heterogeneous nuclear ribonucleoprotein (hnRNP) family (11,47,73). TDP-43 and other hnRNPs are multifunctional proteins that regulate gene expression in both the nucleus and the cytoplasm (47, 75). In the nucleus, TDP-43 binds singlestranded DNA and RNA (10,11,19,20,49,62) and can function as both a transcriptional repressor (1, 2, 62) and a splicing modulator (15,17,20,55). Specifically, TDP-43 regulates pre-mRNA splicing by binding mRNA with (UG) 6-12 sequences (19) and by recruiting other hnRNP proteins into repressive splicing complexes (10,18,55). However, as a nucleocytoplasmic shuttling protein (12), TDP-43 also has distinct cytoplasmic functions, including mRNA stabilization (74).Recent studies indicate that TDP-43 localizes to stress granules (SGs) in response to heat shock, oxidative stress, and chemical inducers of stress (23,33). SGs are dynamic cytoplasmic structures that are believed to act as sorting stations for mRNAs (5). SG composition and morphology differ according to stress and cell type (5, 39), but some core components are conserved. These core components include the RNA-binding protein TIAR (TIA-1 cytotoxic granule-associated RNA-binding protein-like 1) and the stalled translation initiation complex components eIF3 and eIF4G (44,45). In contrast, the incorporation of the RNA-binding proteins HuR and hnRNP A1 into SGs differs with the cell type and stress (5, 39). The physiological stressors that cause TDP-43 aggregates and SGs to form-and the cells in which this occurs-remain unresolved. Moreover, very little is known about the function of cytoplasmic TDP-43, a press...

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Section: Discussionmentioning

confidence: 93%

TDP-43 Is Directed to Stress Granules by Sorbitol, a Novel Physiological Osmotic and Oxidative Stressor

Dewey

Cenik

Sephton

et al. 2011

Molecular and Cellular Biology

299

306

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“…Confocal Microscopy-Cells were prepared for confocal microscopy as described previously with modifications (30). Cells were seeded into 8-well Slide chamber slides (iBidi GmbH, Martinsried, Germany) and allowed to attach overnight.…”

Section: Maintenance and Infection Of Cultured Cell Lines With Prionsmentioning

confidence: 99%

Stimulating the Release of Exosomes Increases the Intercellular Transfer of Prions

Guo

Bellingham

Hill

2016

Journal of Biological Chemistry

Self Cite

130

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“…In screening assays utilizing MoPrP-derived peptide libraries grafted into immunoglobulin G molecules, the peptides corresponding to residues 23 to 33, 97 to 109, and 135 to 157 of MoPrP strongly bound to PrP Sc (29,30,48 (35), and 218 to 232 (18) of MoPrP or the amino acid substitution at residue 138 (37) interfered with the propagation of PrP Sc . However, the incubation of prion-infected cells (RK13 cells) with the 1C5 antibody against residues 118 to 129 of MoPrP (7) for a week was ineffective at reducing the accumulation of PrP Sc in the cells (16). We consider that the dominant and highaffinity binding interface for PrP…”

Section: Discussionmentioning

confidence: 94%

Mouse Prion Protein (PrP) Segment 100 to 104 Regulates Conversion of PrP ^C to PrP ^Sc in Prion-Infected Neuroblastoma Cells

Hara

Okemoto-Nakamura

Shinkai-Ouchi

et al. 2012

J Virol

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Conservation of a Glycine-rich Region in the Prion Protein Is Required for Uptake of Prion Infectivity

Cited by 40 publications

References 67 publications

TDP-43 Is Directed to Stress Granules by Sorbitol, a Novel Physiological Osmotic and Oxidative Stressor

TDP-43 Is Directed to Stress Granules by Sorbitol, a Novel Physiological Osmotic and Oxidative Stressor

Stimulating the Release of Exosomes Increases the Intercellular Transfer of Prions

Mouse Prion Protein (PrP) Segment 100 to 104 Regulates Conversion of PrP ^C to PrP ^Sc in Prion-Infected Neuroblastoma Cells

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Conservation of a Glycine-rich Region in the Prion Protein Is Required for Uptake of Prion Infectivity

Cited by 40 publications

References 67 publications

TDP-43 Is Directed to Stress Granules by Sorbitol, a Novel Physiological Osmotic and Oxidative Stressor

TDP-43 Is Directed to Stress Granules by Sorbitol, a Novel Physiological Osmotic and Oxidative Stressor

Stimulating the Release of Exosomes Increases the Intercellular Transfer of Prions

Mouse Prion Protein (PrP) Segment 100 to 104 Regulates Conversion of PrP C to PrP Sc in Prion-Infected Neuroblastoma Cells

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Mouse Prion Protein (PrP) Segment 100 to 104 Regulates Conversion of PrP ^C to PrP ^Sc in Prion-Infected Neuroblastoma Cells