Compelling transgenetic evidence for transmission of bovine spongiform encephalopathy prions to humans

Michael R. Scott(University of California, San Francisco), Robert Will(University of California, San Francisco), James W. Ironside(University of California, San Francisco), Hoang-Oanh B. Nguyen(University of California, San Francisco), Patrick Tremblay(University of California, San Francisco), Stephen J. DeArmond(University of California, San Francisco), Stanley B. Prusiner(University of California, San Francisco)
Proceedings of the National Academy of Sciences
December 21, 1999
Cited by 596Open Access

Abstract

There is growing concern that bovine spongiform encephalopathy (BSE) may have passed from cattle to humans. We report here that transgenic (Tg) mice expressing bovine (Bo) prion protein (PrP) serially propagate BSE prions and that there is no species barrier for transmission from cattle to Tg(BoPrP) mice. These same mice were also highly susceptible to a new variant of Creutzfeldt-Jakob disease (nvCJD) and natural sheep scrapie. The incubation times (approximately 250 days), neuropathology, and disease-causing PrP isoforms in Tg(BoPrP)Prnp(0/0) mice inoculated with nvCJD and BSE brain extracts were indistinguishable and differed dramatically from those seen in these mice injected with natural scrapie prions. Our findings provide the most compelling evidence to date that prions from cattle with BSE have infected humans and caused fatal neurodegeneration.


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