The necessity for the presence of B cells does not imply that the

The necessity for the presence of B cells does not imply that they are sufficient for neuroinvasion. However, all attempts to identify additional necessary compartments have yielded less unambiguous results. A further candidate that is most likely required for neuroinvasion is certainly the FDC. FDCs have long been identified as the main site of accumulation of PrPSc in lymphoid organs.59 However, experiments aimed at exploring the role of FDCs in peripheral prion pathogenesis Inhibitors,research,lifescience,medical have been less conclusive. So far, all the published material unanimously indicates that accumulation of prions of intraperitoneally

(IP) inoculated mice can only occur in spleens that have properly formed germinal centers and immunohistochemically identifiable FDCs: it has proven impossible to recover prions from spleens of IP inoculated mice deficient in tumor necrosis factor (TNF) receptor-1 (TNFR1)67 (M. A. Klein et al, Inhibitors,research,lifescience,medical unpublished data) or TNF-α,66 none of which contain identifiable FDCs in their spleens. In the case of the FDC-deficient lymphotoxin β (LTβ) knockout mice,68 splenic infectivity was unfortunately not determined. Moreover, administration of soluble lymphotoxin β receptor

(LTβR) very efficiently prevents the buildup of a splenic prion burden in wild-type mice,69 a fact that was later confirmed to also be valid Inhibitors,research,lifescience,medical for the ME7 prion strain for scrapie,70 despite its many alleged differences from the RML strain. On the other hand, neuroinvasion – the development of brain disease after peripheral challenge – was completely unaffected in TNFR167 and LTβ68 knockout mice, and could not even be fully Inhibitors,research,lifescience,medical repressed by the LTβR-Fc treatment.69,70 Inhibitors,research,lifescience,medical Therefore, while the lack of LTβ signaling to FDCs is likely to account for some of the

protection from peripheral prion inoculation observed in B-cell-deficient mice, all of the latter results point to an additional role of B cells in prion neuroinvasion, Anacetrapib which is clearly independent of PrP expression71 and must be distinct from LTβ/TNF signaling to FDCs. Because sympathetic nerve fibers do not appear to penetrate the germinal centers of lymphoid organs (M. Glatzel and A. Aguzzi, unpublished observation), lymphocytes may conceivably play a role in the migration of prions from FDCs to peripheral nerves. Prions and blood Because prions can be detected in lymphoreticular tissues of nvCJD patients, is there a risk of iatrogenic transmission via exposure to blood or tissues derived from preclinical nvCJD cases, and possibly from contaminated surgical instruments? Very thorough epidemiological surveys over two decades have not implicated blood transfusions or administration of blood products as risk factors for prion diseases.

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