Literature DB >> 11080207

The role of prion peptide structure and aggregation in toxicity and membrane binding.

D L Rymer1, T A Good.   

Abstract

Prion diseases are neurodegenerative disorders associated with a conformational change in the normal cellular isoform of the prion protein, PrP(C), to an abnormal scrapie isoform, PrP(SC). Unlike the alpha-helical PrP(C), the protease-resistant core of PrP(SC) is predominantly beta-sheet and possesses a tendency to polymerize into amyloid fibrils. We performed experiments with two synthetic human prion peptides, PrP(106-126) and PrP(127-147), to determine how peptide structure affects neurotoxicity and protein-membrane interactions. Peptide solutions possessing beta-sheet and amyloid structures were neurotoxic to PC12 cells in vitro and bound with measurable affinities to cholesterol-rich phospholipid membranes at ambient conditions, but peptide solutions lacking stable beta-sheet structures and amyloid content were nontoxic and possessed less than one tenth of the binding affinities of the amyloid-containing peptides. Regardless of structure, the peptide binding affinities to cholesterol-depleted membranes were greatly reduced. These results suggest that the beta-sheet and amyloid structures of the prion peptides give rise to their toxicity and membrane binding affinities and that membrane binding affinity, especially in cholesterol-rich environments, may be related to toxicity. Our results may have significance in understanding the role of the fibrillogenic cerebral deposits associated with some of the prion diseases in neurodegeneration and may have implications for other amyloidoses.

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Year:  2000        PMID: 11080207     DOI: 10.1046/j.1471-4159.2000.0752536.x

Source DB:  PubMed          Journal:  J Neurochem        ISSN: 0022-3042            Impact factor:   5.372


  19 in total

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Review 3.  The Molecular Physiopathogenesis of Islet Amyloidosis.

Authors:  Diti Chatterjee Bhowmick; Sanghamitra Singh; Saurabh Trikha; Aleksandar M Jeremic
Journal:  Handb Exp Pharmacol       Date:  2018

Review 4.  Prion protein interactions with nucleic acid: possible models for prion disease and prion function.

Authors:  Abraham Grossman; Brian Zeiler; Victor Sapirstein
Journal:  Neurochem Res       Date:  2003-06       Impact factor: 3.996

5.  In vivo and in vitro neurotoxicity of the human prion protein (PrP) fragment P118-135 independently of PrP expression.

Authors:  Joëlle Chabry; Christiane Ratsimanohatra; Isabelle Sponne; Pierre-Paul Elena; Jean-Pierre Vincent; Thierry Pillot
Journal:  J Neurosci       Date:  2003-01-15       Impact factor: 6.167

Review 6.  Molecular advances in understanding inherited prion diseases.

Authors:  David R Brown
Journal:  Mol Neurobiol       Date:  2002-06       Impact factor: 5.590

Review 7.  Prospects for the pharmacotherapy of amyotrophic lateral sclerosis : old strategies and new paradigms for the third millennium.

Authors:  Barry W Festoff; Zhiming Suo; Bruce A Citron
Journal:  CNS Drugs       Date:  2003       Impact factor: 5.749

8.  The toxicity of the PrP106-126 prion peptide on cultured photoreceptors correlates with the prion protein distribution in the mammalian and human retina.

Authors:  Jie Gong; Abdeljelil Jellali; Valérie Forster; Jérôme Mutterer; Elisabeth Dubus; Wilko D Altrock; José A Sahel; Alvaro Rendon; Serge Picaud
Journal:  Am J Pathol       Date:  2007-04       Impact factor: 4.307

9.  Membrane-mediated amyloid formation of PrP 106-126: A kinetic study.

Authors:  Yen Sun; Wei-Chin Hung; Ming-Tao Lee; Huey W Huang
Journal:  Biochim Biophys Acta       Date:  2015-07-26

10.  Prion protein-detergent micelle interactions studied by NMR in solution.

Authors:  Simone Hornemann; Christine von Schroetter; Fred F Damberger; Kurt Wüthrich
Journal:  J Biol Chem       Date:  2009-06-22       Impact factor: 5.157

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