Specificity, Size, and Frequency of Spaces That Characterize the Mechanism of Bulk Transepithelial Transport of Prions in the Nasal Cavities of Hamsters and Mice

Kincaid, Anthony E.; Ayers, Jacob I.; Bartz, Jason C.

doi:10.1128/jvi.01103-16

Cited by 11 publications

(11 citation statements)

References 54 publications

(68 reference statements)

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“…In all infected animals, DY TME-infected brain homogenate was also detected in the lumen of lymphatic vessels located in the lamina propria of all 3 animals ( Fig 2 , panel B). A similar pattern of brain homogenate distribution was observed in both (n = 2) of the mock-infected hamsters, which is consistent with previous results [ 47 ].…”

Section: Resultssupporting

confidence: 92%

PrPSc formation and clearance as determinants of prion tropism

et al. 2017

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Prion strains are characterized by strain-specific differences in neuropathology but can also differ in incubation period, clinical disease, host-range and tissue tropism. The hyper (HY) and drowsy (DY) strains of hamster-adapted transmissible mink encephalopathy (TME) differ in tissue tropism and susceptibility to infection by extraneural routes of infection. Notably, DY TME is not detected in the secondary lymphoreticular system (LRS) tissues of infected hosts regardless of the route of inoculation. We found that similar to the lymphotropic strain HY TME, DY TME crosses mucosal epithelia, enters draining lymphatic vessels in underlying laminae propriae, and is transported to LRS tissues. Since DY TME causes disease once it enters the peripheral nervous system, the restriction in DY TME pathogenesis is due to its inability to establish infection in LRS tissues, not a failure of transport. To determine if LRS tissues can support DY TME formation, we performed protein misfolding cyclic amplification using DY PrPSc as the seed and spleen homogenate as the source of PrPC. We found that the spleen environment can support DY PrPSc formation, although at lower rates compared to lymphotropic strains, suggesting that the failure of DY TME to establish infection in the spleen is not due to the absence of a strain-specific conversion cofactor. Finally, we provide evidence that DY PrPSc is more susceptible to degradation when compared to PrPSc from other lymphotrophic strains. We hypothesize that the relative rates of PrPSc formation and clearance can influence prion tropism.

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Section: Resultssupporting

confidence: 92%

PrPSc formation and clearance as determinants of prion tropism

et al. 2017

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“…In addition to potential cofactors that could influence CWD infectivity, such as particle binding [ 47 ] and compromised mucosal integrity [ 48 , 53 ], there is PRNP genotype, in which polymorphisms at codon 96 of the white-tailed deer are known to affect the temporal dynamics of CWD infections [ 23 , 41 , 45 ]. In the present studies, most cohorts of 96GG deer became CWD-positive before 96GS animals in the same exposure group [cohorts 1, 2, 4, 6].…”

Section: Discussionmentioning

confidence: 99%

Very low oral exposure to prions of brain or saliva origin can transmit chronic wasting disease

et al. 2020

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The minimum infectious dose required to induce CWD infection in cervids remains unknown, as does whether peripherally shed prions and/or multiple low dose exposures are important factors in CWD transmission. With the goal of better understand CWD infection in nature, we studied oral exposures of deer to very low doses of CWD prions and also examined whether the frequency of exposure or prion source may influence infection and pathogenesis. We orally inoculated white-tailed deer with either single or multiple divided doses of prions of brain or saliva origin and monitored infection by serial longitudinal tissue biopsies spanning over two years. We report that oral exposure to as little as 300 nanograms (ng) of CWD-positive brain or to saliva containing seeding activity equivalent to 300 ng of CWD-positive brain, were sufficient to transmit CWD disease. This was true whether the inoculum was administered as a single bolus or divided as three weekly 100 ng exposures. However, when the 300 ng total dose was apportioned as 10, 30 ng doses delivered over 12 weeks, no infection occurred. While low-dose exposures to prions of brain or saliva origin prolonged the time from inoculation to first detection of infection, once infection was established, we observed no differences in disease pathogenesis. These studies suggest that the CWD minimum infectious dose approximates 100 to 300 ng CWD-positive brain (or saliva equivalent), and that CWD infection appears to conform more with a threshold than a cumulative dose dynamic.

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“…Thus, it cannot be excluded that soil-bound prions might also be inhaled and infect the host as the animal forages for food. Although M cells are present in the epithelia covering the nasal-associated lymphoid tissue ( 60 ), studies in hamsters indicate that this prion uptake across the nasal epithelium occurs independently of M cells ( 61 ). Whether prion uptake across the mucosal surfaces in the upper gastrointestinal and upper respiratory tracts of natural host species is also PrP C independent remains to be determined.…”

Section: Discussionmentioning

confidence: 99%

Oral Prion Neuroinvasion Occurs Independently of PrP ^C Expression in the Gut Epithelium

Marshall

Bradford

Clarke

et al. 2018

J Virol

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The accumulation of orally acquired prions within Peyer's patches in the small intestine is essential for the efficient spread of disease to the brain. Little is known of how the prions initially establish infection within Peyer's patches. Some gastrointestinal pathogens utilize molecules, such as the cellular prion protein PrPC, expressed on gut epithelial cells to enter Peyer's patches. Acute mucosal inflammation can enhance PrPC expression in the intestine, implying the potential to enhance oral prion disease susceptibility. We used transgenic mice to determine whether the uptake of prions into Peyer's patches was dependent upon PrPC expression in the gut epithelium. We show that orally acquired prions can establish infection in Peyer's patches independently of PrPC expression in gut epithelial cells. Our data suggest that the magnitude of PrPC expression in the epithelium lining the small intestine is unlikely to be an important factor which influences oral prion disease susceptibility.

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Specificity, Size, and Frequency of Spaces That Characterize the Mechanism of Bulk Transepithelial Transport of Prions in the Nasal Cavities of Hamsters and Mice

Cited by 11 publications

References 54 publications

PrPSc formation and clearance as determinants of prion tropism

PrPSc formation and clearance as determinants of prion tropism

Very low oral exposure to prions of brain or saliva origin can transmit chronic wasting disease

Oral Prion Neuroinvasion Occurs Independently of PrP ^C Expression in the Gut Epithelium

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Specificity, Size, and Frequency of Spaces That Characterize the Mechanism of Bulk Transepithelial Transport of Prions in the Nasal Cavities of Hamsters and Mice

Cited by 11 publications

References 54 publications

PrPSc formation and clearance as determinants of prion tropism

PrPSc formation and clearance as determinants of prion tropism

Very low oral exposure to prions of brain or saliva origin can transmit chronic wasting disease

Oral Prion Neuroinvasion Occurs Independently of PrP C Expression in the Gut Epithelium

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Oral Prion Neuroinvasion Occurs Independently of PrP ^C Expression in the Gut Epithelium