Abstract

Structural change in the cellular prion protein, PrPC to a ProteinaseK‐resistant β‐sheet‐rich insoluble form PrPSC and its accumulation have been considered to be central to the pathogenesis of the prion diseases (TSE). In a recent paper, Deleault et al have shown that specific endogenous RNA molecules can induce in vitro structural conversion of endogenous PrPC to PrPSC.1 Small highly structured synthetic RNAs can also induce this conversion process.2 However, recent in vivo results show that PrPSC is not directly involved in the prion pathogenesis.3 It is possible, however, that nucleic‐acid‐induced PrPSC associated with the inducer nucleic acid could be the components of the infectious agent. BioEssays 26:469–473, 2004. © 2004 Wiley Periodicals, Inc.