Overexpression of the
            <i>Hspa13</i>
            (
            <i>Stch</i>
            ) gene reduces prion disease incubation time in mice

Grizenkova, Julia; Akhtar, Shaheen; Hummerich, Holger; Tomlinson, Andrew; Asante, Emmanuel A.; Wenborn, Adam; Fizet, Jérémie; Poulter, Mark; Wiseman, Frances K.; Fisher, Elizabeth; Tybulewicz, Victor L. J.; Brandner, Sebastian; Collinge, John; Lloyd, Sarah E.

doi:10.1073/pnas.1208917109

Cited by 22 publications

(31 citation statements)

References 46 publications

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“…The only phenotype associated with these mice is female sterility in homozygote knockouts [27]. We inoculated mice intracerebrally with two different mouse-adapted scrapie prion strains, Chandler/RML and ME7, and a mouse adapted BSE prion strain, MRC2 (BSE passaged in Prnp a mice) [28], [34]. In Sod1 −/− mice a significant decrease in incubation time was seen for all three prion strains as compared to Sod1 +/+ controls (Figure 2 and Table S2).…”

Section: Resultsmentioning

confidence: 99%

“…The Chandler/RML (I9900), ME7 (I9459) and MRC2 (I9468) prion strains were sourced and prepared as previously described [22], [28]. Mice were anaesthetized with isofluorane/O 2 and inoculated intra-cerebrally into the right parietal lobe with 30 µl of inocula as previously described [15].…”

Section: Methodsmentioning

confidence: 99%

“…For detection of Sod1, samples were prepared as above but without proteinase K digestion and detected with a rabbit polyclonal antibody (0.5 ug/ml) (Abcam). Anti-β-actin mouse monoclonal antibody (0.05 ug/ml) (Sigma) was used as an internal control as previously described [28].…”

Section: Methodsmentioning

confidence: 99%

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Sod1 Deficiency Reduces Incubation Time in Mouse Models of Prion Disease

et al. 2013

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Prion infections, causing neurodegenerative conditions such as Creutzfeldt-Jakob disease and kuru in humans, scrapie in sheep and BSE in cattle are characterised by prolonged and variable incubation periods that are faithfully reproduced in mouse models. Incubation time is partly determined by genetic factors including polymorphisms in the prion protein gene. Quantitative trait loci studies in mice and human genome-wide association studies have confirmed that multiple genes are involved. Candidate gene approaches have also been used and identified App, Il1-r1 and Sod1 as affecting incubation times. In this study we looked for an association between App, Il1-r1 and Sod1 representative SNPs and prion disease incubation time in the Northport heterogeneous stock of mice inoculated with the Chandler/RML prion strain. No association was seen with App, however, significant associations were seen with Il1-r1 (P = 0.02) and Sod1 (P<0.0001) suggesting that polymorphisms at these loci contribute to the natural variation observed in incubation time. Furthermore, following challenge with Chandler/RML, ME7 and MRC2 prion strains, Sod1 deficient mice showed highly significant reductions in incubation time of 20, 13 and 24%, respectively. No differences were detected in Sod1 expression or activity. Our data confirm the protective role of endogenous Sod1 in prion disease.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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Sod1 Deficiency Reduces Incubation Time in Mouse Models of Prion Disease

et al. 2013

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“…In mice the absence of CRYAB in combination with another sHSP, HSPB2, exacerbates the behavioral changes in an Alzheimer model (Ojha et al 2011 ). In contrast the overexpression of a HSP70 class chaperone, Hspa13, accelerated prion-mediated disease in mice (Grizenkova et al 2012 ). These studies support the argument that αB-crystallin, like HSP90, has capacitor-like activity with respect to genetic traits Proteostasis and Cell Cycle Control The overexpression of αB-crystallin can reverse the morbidity in mice caused by GFAP (Hagemann et al 2009 ) and in cellular models this is likely due to increased proteasomal activity .…”

Section: Fig 172 αB-crystallin At the Crossroads Of Life And Its Romentioning

confidence: 96%

The Dynamic Duo of Small Heat Proteins and IFs Maintain Cell Homeostasis, Resist Cellular Stress and Enable Evolution in Cells and Tissues

Perng

Quinlan

2015

Heat Shock Proteins

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As with many proteins, their initial christening with a name corrals our thinking on their functions and roles. IFs were not named as heat shock proteins, but along with heat shock proteins, they continue to be expressed in response to heat shock. In this review we outline the case for exposing the identity of the "dynamic duo" as small heat shock proteins (sHSPs) and their IF (IF) partners in their battle to assuage stress. Together they maintain the homeostasis of and integrate key cellular processes within cells that allow potential evolutionary opportunity to be seized (Quinlan RA, Ellis RJ, Philos Trans R Soc Lond B Biol Sci 368:20130091, 2013). Both sHSPs and IFs form dynamic polymeric structures -nano-particles and intermediate (nano) fi laments respectively. Both have a wide range of interaction (client) proteins. IFs provide a convenient matrix to host small heat shock proteins and potentiate their role as chaperones, whilst IF function is sHSP-dependent. Together, it is their emerging capacity as integrators of both cell homeostasis and the stress response within and between tissues, however, which is the most exciting. This is because the dynamic duo co-operate on the two central chaperone activities -assisting protein assemblies and dealing with the consequences of protein damage. We propose that the sHSP-IF partnership is key to understanding the stress response, not least because it emphasizes the role of these protein chaperones in assisting the building, regulation and turnover of the IF protein assemblies as well as in diseases caused by their malfunction.

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“…We have taken the alternative approach of looking for differential expression between inbred lines of mice with different incubation times. We used uninfected mice and to enrich for relevant genes we looked for a correlation between expression level and incubation time across five lines of mice [35]. Five potential candidates were identified including Hspa13 ( Stch ), a member of the Hsp70 family of ATPase heat shock proteins.…”

Section: Mrna Expressionmentioning

confidence: 99%

Genetics of prion diseases

Lloyd¹,

Mead²,

Collinge³

2013

Current Opinion in Genetics & Development

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Prion diseases are transmissible, fatal neurodegenerative diseases that include scrapie and bovine spongiform encephalopathy (BSE) in animals and Creutzfeldt–Jakob disease (CJD) in human. The prion protein gene (PRNP) is the major genetic determinant of susceptibility, however, several studies now suggest that other genes are also important. Two recent genome wide association studies in human have identified four new loci of interest: ZBTB38-RASA2 in UK CJD cases and MTMR7 and NPAS2 in variant CJD. Complementary studies in mouse have used complex crosses to identify new modifiers such as Cpne8 and provided supporting evidence for previously implicated genes (Rarb and Stmn2). Expression profiling has identified new candidates, including Hspa13, which reduces incubation time in a transgenic model.

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Overexpression of the Hspa13 ( Stch ) gene reduces prion disease incubation time in mice

Cited by 22 publications

References 46 publications

Sod1 Deficiency Reduces Incubation Time in Mouse Models of Prion Disease

Sod1 Deficiency Reduces Incubation Time in Mouse Models of Prion Disease

The Dynamic Duo of Small Heat Proteins and IFs Maintain Cell Homeostasis, Resist Cellular Stress and Enable Evolution in Cells and Tissues

Genetics of prion diseases

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