Your search keyword '"Race, Brent"' showing total 11 results

1. Sodium hypochlorite inactivation of human CJD prions.

Author

Groveman, Bradley R., Race, Brent, Hughson, Andrew G., and Haigh, Cathryn L.

Subjects

*CREUTZFELDT-Jakob disease, *PRION diseases, *GUINEA pigs, *PRIONS, *GENETIC mutation, *TRANSGENIC mice

Abstract

Prion diseases are transmissible, fatal neurologic diseases of mammals caused by the accumulation of mis-folded, disease associated prion protein (PrPd). Creutzfeldt-Jakob Disease (CJD) is the most common human prion disease and can occur by sporadic onset (sCJD) (~85% of CJD cases), genetic mutations in the prion protein gene (10–15%) or iatrogenic transmission (rare). PrPd is difficult to inactivate and many methods to reduce prion infectivity are dangerous, caustic, expensive, or impractical. Identifying viable and safe methods for decontamination of CJD exposed materials is critically important for medical facilities and research institutions. Previous research has shown that concentrated sodium hypochlorite (bleach) was effective at inactivation of CJD prions derived from brains of mice or guinea pigs. Unfortunately, human prions adapted to rodents may mis-fold differently than in humans, and the rodent adapted prions may not have the same resistance or susceptibility to inactivation present in bona fide CJD prions. To confirm that bleach was efficacious against human sourced CJD prions, we exposed different subtypes of sCJD-infected human brain homogenates to different concentrations of bleach for increasing exposure times. Initial and residual prion seeding activity following inactivation were measured using Real-Time Quaking Induced Conversion. In addition, we tested how passage of human sCJD into either transgenic mice that expressed human prion protein, or transmission of CJD to human cerebral organoids (CO), two common laboratory practices, may affect CJD prions' susceptibility to bleach inactivation. Our results show that bleach is effective against human sourced sCJD prions, and both treatment time and concentration of bleach were important factors for CJD inactivation. CJD derived from human brains, transgenic mouse brains or CO were all susceptible to inactivation with as low as a 10 percent bleach solution with a 30-minute exposure time or a 50 percent bleach solution with as little as a 1-minute exposure time. [ABSTRACT FROM AUTHOR]

Published

2024

2. The PINK1/Parkin pathway of mitophagy exerts a protective effect during prion disease

Author

Ward, Anne, primary, Jessop, Forrest, additional, Faris, Robert, additional, Hollister, Jason, additional, Shoup, Daniel, additional, Race, Brent, additional, Bosio, Catharine M., additional, and Priola, Suzette A., additional

Published

2024

3. CD11c is not required by microglia to convey neuroprotection after prion infection

Author

Carroll, James A., primary, Striebel, James F., additional, Baune, Chase, additional, Chesebro, Bruce, additional, and Race, Brent, additional

Published

2023

4. Efficacy of Wex-cide 128 disinfectant against multiple prion strains

Author

Baune, Chase, primary, Groveman, Bradley R., additional, Hughson, Andrew G., additional, Thomas, Tina, additional, Twardoski, Barry, additional, Priola, Suzette, additional, Chesebro, Bruce, additional, and Race, Brent, additional

Published

2023

5. Microglia have limited influence on early prion pathogenesis, clearance, or replication

Author

Race, Brent, primary, Williams, Katie, additional, Baune, Chase, additional, Striebel, James F., additional, Long, Dan, additional, Thomas, Tina, additional, Lubke, Lori, additional, Chesebro, Bruce, additional, and Carroll, James A., additional

Published

2022

6. Reduced SOD2 expression does not influence prion disease course or pathology in mice

Author

Foliaki, Simote T., primary, Race, Brent, additional, Williams, Katie, additional, Baune, Chase, additional, Groveman, Bradley R., additional, and Haigh, Cathryn L., additional

Published

2021

7. Inactivation of chronic wasting disease prions using sodium hypochlorite

Author

Williams, Katie, primary, Hughson, Andrew G., additional, Chesebro, Bruce, additional, and Race, Brent, additional

Published

2019

8. Altered distribution, aggregation, and protease resistance of cellular prion protein following intracranial inoculation

Author

Ward, Anne, primary, Hollister, Jason R., additional, Choi, Young Pyo, additional, Race, Brent, additional, Williams, Katie, additional, Shoup, Daniel W., additional, Moore, Roger A., additional, and Priola, Suzette A., additional

Published

2019

9. Toll-like receptor 2 confers partial neuroprotection during prion disease

Author

Carroll, James A., primary, Race, Brent, additional, Williams, Katie, additional, and Chesebro, Bruce, additional

Published

2018

10. Prion Seeding Activities of Mouse Scrapie Strains with Divergent PrPSc Protease Sensitivities and Amyloid Plaque Content Using RT-QuIC and eQuIC

Author

Vascellari, Sarah, primary, Orrù, Christina D., additional, Hughson, Andrew G., additional, King, Declan, additional, Barron, Rona, additional, Wilham, Jason M., additional, Baron, Gerald S., additional, Race, Brent, additional, Pani, Alessandra, additional, and Caughey, Byron, additional

Published

2012

11. Prion Seeding Activities of Mouse Scrapie Strains with Divergent PrPSc Protease Sensitivities and Amyloid Plaque Content Using RT-QuIC and eQuIC.

Author

Vascellari, Sarah, Orrù, Christina D., Hughson, Andrew G., King, Declan, Barron, Rona, Wilham, Jason M., Baron, Gerald S., Race, Brent, Pani, Alessandra, and Caughey, Byron

Subjects

AUTISM spectrum disorders, HUMAN endogenous retroviruses, GENETICS, MESSENGER RNA, PATIENTS, DEVELOPMENTAL disabilities

Abstract

Different transmissible spongiform encephalopathy (TSE)-associated forms of prion protein (e.g. PrPSc) can vary markedly in ultrastructure and biochemical characteristics, but each is propagated in the host. PrPSc propagation involves conversion from its normal isoform, PrPC, by a seeded or templated polymerization mechanism. Such a mechanism is also the basis of the RT-QuIC and eQuIC prion assays which use recombinant PrP (rPrPSen) as a substrate. These ultrasensitive detection assays have been developed for TSE prions of several host species and sample tissues, but not for murine models which are central to TSE pathogenesis research. Here we have adapted RT-QuIC and eQuIC to various murine prions and evaluated how seeding activity depends on glycophosphatidylinositol (GPI) anchoring and the abundance of amyloid plaques and protease-resistant PrPSc (PrPRes). Scrapie brain dilutions up to 10¯8 and 10¯13 were detected by RT-QuIC and eQuIC, respectively. Comparisons of scrapie-affected wild-type mice and transgenic mice expressing GPI anchorless PrP showed that, although similar concentrations of seeding activity accumulated in brain, the heavily amyloid-laden anchorless mouse tissue seeded more rapid reactions. Next we compared seeding activities in the brains of mice with similar infectivity titers, but widely divergent PrPRes levels. For this purpose we compared the 263K and 139A scrapie strains in transgenic mice expressing P101L PrPC. Although the brains of 263K-affected mice had little immunoblot-detectable PrPRes, RT-QuIC indicated that seeding activity was comparable to that associated with a high-PrPRes strain, 139A. Thus, in this comparison, RT-QuIC seeding activity correlated more closely with infectivity than with PrPRes levels. We also found that eQuIC, which incorporates a PrPSc immunoprecipitation step, detected seeding activity in plasma from wild-type and anchorless PrP transgenic mice inoculated with 22L, 79A and/or RML scrapie strains. Overall, we conclude that these new mouse-adapted prion seeding assays detect diverse types of PrPSc. [ABSTRACT FROM AUTHOR]

Published

2012