Dominant-Negative Inhibition of Prion Formation Diminished by Deletion Mutagenesis of the Prion Protein

doi:10.1128/JVI.74.9.4351-4360.2000

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Journal of Virology, May 2000, p. 4351-4360, Vol. 74, No. 9
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Dominant-Negative Inhibition of Prion Formation Diminished by Deletion Mutagenesis of the Prion Protein

Laurence Zulianello,¹^,² Kiyotoshi Kaneko,¹^,² Michael Scott,¹^,² Susanne Erpel,¹^,² Dong Han,¹^,² Fred E. Cohen,¹^,³^,⁴^,⁵ and Stanley B. Prusiner¹^,²^,³^,^*

Institute for Neurodegenerative Diseases¹ and Departments of Neurology,² Biochemistry and Biophysics,³ Medicine,⁴ and Cellular and Molecular Pharmacology,⁵ University of California, San Francisco, California 94143

Received 8 October 1999/Accepted 6 January 2000

Polymorphic basic residues near the C terminus of the prion protein (PrP) in humans and sheep appear to protect against priondisease. In heterozygotes, inhibition of prion formation appearsto be dominant negative and has been simulated in cultured cellspersistently infected with scrapie prions. The results of nuclearmagnetic resonance and mutagenesis studies indicate that specificsubstitutions at the C-terminal residues 167, 171, 214, and 218of PrP^C act as dominant-negative, inhibitors of PrP^Sc formation (K. Kaneko et al., Proc. Natl. Acad. Sci. USA 94:10069-10074,1997). Trafficking of substituted PrP^C to caveaola-like domains or rafts by the glycolipid anchor wasrequired for the dominant-negative phenotype; interestingly, aminoacid replacements at multiple sites were less effective than single-residuesubstitutions. To elucidate which domains of PrP^C are responsible for dominant-negative inhibition of PrP^Sc formation, we analyzed whether N-terminally truncated PrP(Q218K)molecules exhibited dominant-negative effects in the conversionof full-length PrP^C to PrP^Sc. We found that the C-terminal domain of PrP is not sufficientto impede the conversion of the full-length PrP^C molecule and that N-terminally truncated molecules (with residues23 to 88 and 23 to 120 deleted) have reduced dominant-negativeactivity. Whether the N-terminal region of PrP acts by stabilizingthe C-terminal domain of the molecule or by modulating the bindingof PrP^C to an auxiliary molecule that participates in PrP^Sc formation remains to beestablished.

^* Corresponding author. Mailing address: Institute for Neurodegenerative Diseases, Box 0518, University of California, San Francisco,CA 94143-0518. Phone: (415) 476-4482. Fax: (415) 476-8386. E-mail:abbott{at}itsa.ucsf.edu.

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