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ABSTRACT Prions, the causative agents of Creutzfeldt-Jacob Disease (CJD) in humans and bovine spongiform encephalopathy (BSE) and scrapie in animals, are principally composed of PrPSc, a
conformational isomer of cellular prion protein (PrPC). The propensity of PrPC to adopt alternative folds suggests that there may be an unusually high proportion of alternative conformations
in dynamic equilibrium with the native state. However, the rates of hydrogen/deuterium exchange demonstrate that the conformation of human PrPC is not abnormally plastic. The stable core of
PrPC has extensive contributions from all three α-helices and shows protection factors equal to the equilibrium constant for the major unfolding transition. A residual, hyper-stable region
is retained upon unfolding, and exchange analysis identifies this as a small nucleus of ~10 residues around the disulfide bond. These results show that the most likely route for the
conversion of PrPC to PrPSc is through a highly unfolded state that retains, at most, only this small nucleus of structure, rather than through a highly organized folding intermediate.
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PRION PROTEIN Article Open access 04 November 2021 REFERENCES * Collinge, J. _ Hum. Mol. Genet._ 6, 1699–1705 (1997). Article CAS Google Scholar * Zhang, H. et al. _ Biochemistry_ 36,
3543–3553 (1997). * Kelly, J.W. _ Curr. Opin. Struct. Biol._ 6, 11–17 (1996). Article CAS Google Scholar * Bai, Y., Sosnick, T.R., Mayne, L. & Englander, S.W. _Science_ 269, 192–197
(1995). Article CAS Google Scholar * Booth, D.R. _ et al_. _Nature_ 385, 787–793 (1997). Article CAS Google Scholar * Riek, R. et al. _Nature_ 382, 180–182 (1996). Article CAS Google
Scholar * Billeter, M. _ et al._ _Proc. Natl. Acad. Sci. USA_ 94, 7281 –7285 (1997). Article CAS Google Scholar * James, T.L. _ et al_. _Proc. Natl. Acad. Sci. USA_ 94, 10086 –10091
(1997). Article CAS Google Scholar * Freund, S.M., Wong, K.B. & Fersht, A.R. _Proc. Natl. Acad. Sci. USA_ 93, 10600–10603 (1996). Article CAS Google Scholar * Neira, J.L. _ et al._
_Fold. Des._ 1, 189– 208 (1996). Article CAS Google Scholar * Hosszu, L.L.P. _ et al_. _Nature Struct. Biol._ 4, 801– 804 (1997). Article CAS Google Scholar * Wang, Y. & Shortle,
D. _Fold. Des._ 2, 93–100 (1997). Article CAS Google Scholar * Blake, C. & Serpell, L. _Structure._ 4, 989–998 (1996). Article CAS Google Scholar * Sunde, M. et al. _J. Mol. Biol._
273, 729– 739 (1997). Article CAS Google Scholar * Fink, A.L. _ Fold. Des._ 3, R9–23 ( 1998). Article CAS Google Scholar * Murray, A.J., Lewis, S.J., Barclay, A.N. & Brady, R.L. _
Proc. Natl. Acad. Sci. USA._ 92, 7337– 7341 (1995). Article CAS Google Scholar * Hayes, M.V., Sessions, R.B., Brady, R.L. & Clarke, A.R. _ J. Mol. Biol._ 285, 1855–1865 (1999).
Article Google Scholar * Safar, J., Roller, P.P., Gajdusek, D.C. & Gibbs, C.J. Jr. _ Biochemistry_ 33, 8375–8383 (1994). Article CAS Google Scholar * Hornemann, S. &
Glockshuber, R. _Proc. Natl. Acad. Sci. USA_ 95, 6010–6014 (1998). Article CAS Google Scholar * Bax, A. & Ikura, M. _J. Biomol. NMR_ 1, 99–104 (1991). Article CAS Google Scholar *
Wittekind, M. & Mueller, L. _J. Magnet. Res. Series B_ 101, 201–205 (1993). Article CAS Google Scholar * Muhandiram, D.R. & Kay, L.E. _J. Magnet. Res. Series B_ 103, 203–216 (
1994). Article CAS Google Scholar * Kay, L.E., Xu, G.Y. & Yamazaki, T. _J. Magnet. Res. Series A_ 109, 129–133 (1994). Article CAS Google Scholar * Wishart, D.S. & Sykes, B.D.
_J. Biomol. NMR_ 4, 171–180 (1994). Article CAS Google Scholar * Bai, Y., Milne, J.S., Mayne, L. & Englander, S.W. _Proteins_ 17, 75–86 (1993). Article CAS Google Scholar * Parker,
M.J., Spencer, J. & Clarke, A.R. _J. Mol. Biol._ 253, 771– 786 (1995). Article CAS Google Scholar * Wishart, D.S., Sykes, B.D. & Richards, F.M. _J. Mol. Biol._ 222, 311– 333
(1991). Article CAS Google Scholar * Donne, D.G. _ et al_. _Proc. Natl. Acad. Sci. USA_ 94, 13452 –13457 (1997). Article CAS Google Scholar * Billeter, M. _ et al._ _Proc. Natl. Acad.
Sci. USA_ 94, 7281 –7285 (1997). Article CAS Google Scholar * Ferrin, T.E., Huang, C.C., Jarvis, L.E. & Langridge, R. _ J. Mol. Graphics_ 6, 13(1988). Article CAS Google Scholar *
Ferrin, T.E., Couch, G.S., Huang, C.C., Pettersen, E.F. & Langridge, R. _J. Mol. Graphics_ 9, 27– 32 (1991). Article CAS Google Scholar Download references ACKNOWLEDGEMENTS This work
was funded by the Wellcome Trust and the Medical Research Council. A.R.C. and J.P.W. are Lister Institute Research Fellows. The Krebs Institute is a BBSRC-funded center. AUTHOR INFORMATION
Author notes * Laszlo L. P. Hosszu, Nicola J. Baxter, Graham S. Jackson, Jonathan P. Waltho and C. Jeremy Craven: These authors contributed equally to this work. AUTHORS AND AFFILIATIONS *
Department of Neurogenetics, Prion Disease Group, Imperial College School of Medicine at St. Mary's, London, W2 1NY, UK Laszlo L. P. Hosszu, Nicola J. Baxter, Graham S. Jackson, Aisling
Power & Anthony R. Clarke * Department of Biochemistry, School of Medical Sciences, University of Bristol, Bristol, BS8 1TD, UK Laszlo L. P. Hosszu, Anthony R. Clarke & John
Collinge * Krebs Institute for Biomolecular Research, Dept. of Molecular Biology and Biotechnology, University of Sheffield, Sheffield, S10 2TN, UK Jonathan P. Waltho & C. Jeremy Craven
Authors * Laszlo L. P. Hosszu View author publications You can also search for this author inPubMed Google Scholar * Nicola J. Baxter View author publications You can also search for this
author inPubMed Google Scholar * Graham S. Jackson View author publications You can also search for this author inPubMed Google Scholar * Aisling Power View author publications You can also
search for this author inPubMed Google Scholar * Anthony R. Clarke View author publications You can also search for this author inPubMed Google Scholar * Jonathan P. Waltho View author
publications You can also search for this author inPubMed Google Scholar * C. Jeremy Craven View author publications You can also search for this author inPubMed Google Scholar * John
Collinge View author publications You can also search for this author inPubMed Google Scholar CORRESPONDING AUTHOR Correspondence to Anthony R. Clarke. RIGHTS AND PERMISSIONS Reprints and
permissions ABOUT THIS ARTICLE CITE THIS ARTICLE Hosszu, L., Baxter, N., Jackson, G. _et al._ Structural mobility of the human prion protein probed by backbone hydrogen exchange. _Nat Struct
Mol Biol_ 6, 740–743 (1999). https://doi.org/10.1038/11507 Download citation * Received: 22 January 1999 * Accepted: 16 April 1999 * Issue Date: August 1999 * DOI:
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