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Journal of Virology, December 2000, p. 11928-11934, Vol. 74, No. 24
Institute for Neurodegenerative
Diseases1 and Departments of
Neurology,2 Cellular and Molecular
Pharmacology,6
Medicine,3
Pathology,5 and Biochemistry and
Biophysics,4 University of California at San
Francisco, San Francisco, California 94143
Received 14 July 2000/Accepted 22 September 2000
An abridged PrP molecule of 106 amino acids designated PrP106 can
form infectious miniprions in transgenic (Tg) mice (29). Addition of six-histidine (His6) affinity tags to selective
sites within PrP106 resulted unexpectedly in new PrP proteins that
spontaneously adopted protease-resistant conformations when expressed
in neuroblastoma cells and Tg mice. Acquisition of protease resistance
depended on the length, charge, and placement of the affinity tag.
Introduction of the disease-linked mutation E200K into the sequence of
PrP106(140/6His) increased the recovery of protease-resistant PrP
fivefold, whereas introduction of the mutations C213A and
0022-538X/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.
Affinity-Tagged Miniprion Derivatives Spontaneously
Adopt Protease-Resistant Conformations

214-220
did not affect the recovery of protease-resistant PrP. Treatment of
cultured cells expressing affinity-tagged PrP106 mutants with
polypropyleneimine dendrimer rendered these proteins sensitive to
protease digestion in a manner similar to wild-type PrPSc.
We conclude that certain affinity-tagged PrP106 proteins spontaneously fold into conformations partially resembling, yet distinct from, wild-type PrPSc. These proteins might be useful tools in
the identification of new disease-causing mutations as well as for
screening compounds for therapeutic efficacy.
*
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: ind{at}itsa.ucsf.edu.
Present address: Tohoku University School of Medicine, 2-1 Seiryou-Machi, Aoba-ku, Sendai, 980 Japan.
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