Prions at the crossroads: the need to identify the active TSE agent

Abstract

Structural change in the cellular prion protein, PrP^C to a ProteinaseK‐resistant β‐sheet‐rich insoluble form PrP^SC 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 PrP^C to PrP^SC.1 Small highly structured synthetic RNAs can also induce this conversion process.2 However, recent in vivo results show that PrP^SC is not directly involved in the prion pathogenesis.3 It is possible, however, that nucleic‐acid‐induced PrP^SC associated with the inducer nucleic acid could be the components of the infectious agent. BioEssays 26:469–473, 2004.