Exploring the Propensities of Helices in PrPC to Form beta  Sheet Using NMR Structures and Sequence Alignments

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Exploring the Propensities of Helices in PrP^C to Form $beta$ Sheet Using NMR Structures and Sequence Alignments

R. I. Dima and D. Thirumalai

Institute for Physical Science and Technology, and Department of Chemistry and Biochemistry, University of Maryland, College Park, Maryland 20742 USA

Neurodegenerative diseases induced by transmissible spongiform encephalopathies are associated with prions. The most spectacularevent in the formation of the infectious scrapie form, referredto as PrP^Sc, is the conformational change from the predominantly $alpha$ -helicalconformation of PrP^C to the PrP^Sc state that is rich in $beta$ -sheet content. Using sequence alignmentsand structural analysis of the available nuclear magnetic resonancestructures of PrP^C, we explore the propensities of helices in PrP^C to be in a $beta$ -strand conformation. Comparison of a number of structuralcharacteristics (such as solvent accessible area, distributionof ( $Phi$ , $Psi$ ) angles, mismatches in hydrogen bonds, nature of residuesin local and nonlocal contacts, distribution of regular densitiesof amino acids, clustering of hydrophobic and hydrophilic residuesin helices) between PrP^C structures and a databank of "normal" proteins shows that themost unusual features are found in helix 2 (H2) (residues 172-194)followed by helix 1 (H1) (residues 144-153). In particular, theC-terminal residues in H2 are frustrated in their helical state.The databank of normal proteins consists of 58 helical proteins,36 $alpha$ + $beta$ proteins, and 31 $beta$ -sheet proteins. Our conclusions arealso substantiated by gapless threading calculations that showthat the normalized Z-scores of prion proteins are similar tothose of other $alpha$ + $beta$ proteins with low helical content. Applicationof the recently introduced notion of discordance, namely, incompatibilityof the predicted and observed secondary structures, also pointsto the frustration of H2 not only in the wild type but also inmutants of human PrP^C. This suggests that the instability of PrP^C proteins may play a role in their being susceptible to the profoundconformational change. Our analysis shows that, in addition tothe previously proposed role for the segment (90-120) and possiblyH1, the C-terminus of H2 and possibly N-terminus may play a rolein the $alpha$ $right-arrow$ $beta$ transition. An implication of our results is that theease of polymerization depends on the unfolding rate of the monomer.Sequence alignments show that helices in avian prion proteins(chicken, duck, crane) are better accommodated in a helical state,which might explain the absence of PrP^Sc formation over finite time scales in these species. From thisanalysis, we predict that correlated mutations that reduce thefrustration in the second half of helix 2 in mammalian prion proteinscould inhibit the formation of PrP^Sc.

Biophys J, September 2002, p. 1268-1280, Vol. 83, No. 3
© 2002 by the Biophysical Society 0006-3495/02/09/1268/13 $2.00

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Exploring the Propensities of Helices in PrPC to Form Sheet Using NMR Structures and Sequence Alignments

Exploring the Propensities of Helices in PrP^C to Form $beta$ Sheet Using NMR Structures and Sequence Alignments