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Literature DB >> 1438300

Predicted alpha-helical regions of the prion protein when synthesized as peptides form amyloid.

M Gasset¹, M A Baldwin, D H Lloyd, J M Gabriel, D M Holtzman, F Cohen, R Fletterick, S B Prusiner.

Abstract

By comparing the amino acid sequences of 11 mammalian and 1 avian prion proteins (PrP), structural analyses predicted four alpha-helical regions. Peptides corresponding to these regions of Syrian hamster PrP were synthesized, and, contrary to predictions, three of the four spontaneously formed amyloids as shown by electron microscopy and Congo red staining. By IR spectroscopy, these amyloid peptides exhibited secondary structures composed largely of beta-sheets. The first of the predicted helices is the 14-amino acid peptide corresponding to residues 109-122; this peptide and the overlapping 15-residue sequence 113-127 both form amyloid. The most highly amyloidogenic peptide is AGAAAAGA, which corresponds to Syrian hamster PrP residues 113-120 and is conserved across all species for which the PrP sequence has been determined. Two other predicted alpha-helices corresponding to residues 178-191 and 202-218 form amyloids and exhibit considerable beta-sheet structure when synthesized as peptides. These findings suggest the possibility that the conversion of the cellular isoform of PrP to the scrapie isoform of PrP involves the transition of one or more putative PrP alpha-helices into beta-sheets and that prion diseases are disorders of protein conformation.

Entities: Chemical Species

Mesh：

Substances：
Peptides
Prions

Year: 1992 PMID： 1438300 PMCID： PMC50458 DOI： 10.1073/pnas.89.22.10940

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

43 in total

1. N-terminal truncation of the scrapie-associated form of PrP by lysosomal protease(s): implications regarding the site of conversion of PrP to the protease-resistant state.

Authors: B Caughey; G J Raymond; D Ernst; R E Race
Journal: J Virol Date: 1991-12 Impact factor: 5.103

2. Amyloid-like properties of a synthetic peptide corresponding to the carboxy terminus of beta-amyloid protein precursor.

Authors: C B Caputo; P E Fraser; I E Sobel; D A Kirschner
Journal: Arch Biochem Biophys Date: 1992-01 Impact factor: 4.013

3. Structure of a protein superfiber: spider dragline silk.

Authors: M Xu; R V Lewis
Journal: Proc Natl Acad Sci U S A Date: 1990-09 Impact factor: 11.205

4. Pro----leu change at position 102 of prion protein is the most common but not the sole mutation related to Gerstmann-Sträussler syndrome.

Authors: K Doh-ura; J Tateishi; H Sasaki; T Kitamoto; Y Sakaki
Journal: Biochem Biophys Res Commun Date: 1989-09-15 Impact factor: 3.575

5. The precursor of Alzheimer's disease amyloid A4 protein resembles a cell-surface receptor.

Authors: J Kang; H G Lemaire; A Unterbeck; J M Salbaum; C L Masters; K H Grzeschik; G Multhaup; K Beyreuther; B Müller-Hill
Journal: Nature Date: 1987 Feb 19-25 Impact factor: 49.962

6. Molecular characteristics of prion rods purified from scrapie-infected hamster brains.

Authors: M P McKinley; M B Braunfeld; C G Bellinger; S B Prusiner
Journal: J Infect Dis Date: 1986-07 Impact factor: 5.226

7. Secondary structure analysis of the scrapie-associated protein PrP 27-30 in water by infrared spectroscopy.

Authors: B W Caughey; A Dong; K S Bhat; D Ernst; S F Hayes; W S Caughey
Journal: Biochemistry Date: 1991-08-06 Impact factor: 3.162

8. Identification of glycoinositol phospholipid linked and truncated forms of the scrapie prion protein.

Authors: N Stahl; M A Baldwin; A L Burlingame; S B Prusiner
Journal: Biochemistry Date: 1990-09-25 Impact factor: 3.162

9. Adenovirus E4-dependent activation of the early E2 promoter is insufficient to promote the early-to-late-phase transition.

Authors: C Hemström; A Virtanen; E Bridge; G Ketner; U Pettersson
Journal: J Virol Date: 1991-03 Impact factor: 5.103

10. Scrapie and cellular prion proteins differ in their kinetics of synthesis and topology in cultured cells.

Authors: D R Borchelt; M Scott; A Taraboulos; N Stahl; S B Prusiner
Journal: J Cell Biol Date: 1990-03 Impact factor: 10.539

82 in total

1. Molecular modelling indicates that the pathological conformations of prion proteins might be beta-helical.

Authors: D T Downing; N D Lazo
Journal: Biochem J Date: 1999-10-15 Impact factor: 3.857

2. Immobilized prion protein undergoes spontaneous rearrangement to a conformation having features in common with the infectious form.

Authors: E Leclerc; D Peretz; H Ball; H Sakurai; G Legname; A Serban; S B Prusiner; D R Burton; R A Williamson
Journal: EMBO J Date: 2001-04-02 Impact factor: 11.598

Predicted alpha-helical regions of the prion protein when synthesized as peptides form amyloid.

1. N-terminal truncation of the scrapie-associated form of PrP by lysosomal protease(s): implications regarding the site of conversion of PrP to the protease-resistant state.

2. Amyloid-like properties of a synthetic peptide corresponding to the carboxy terminus of beta-amyloid protein precursor.

3. Structure of a protein superfiber: spider dragline silk.

4. Pro----leu change at position 102 of prion protein is the most common but not the sole mutation related to Gerstmann-Sträussler syndrome.

5. The precursor of Alzheimer's disease amyloid A4 protein resembles a cell-surface receptor.

6. Molecular characteristics of prion rods purified from scrapie-infected hamster brains.

7. Secondary structure analysis of the scrapie-associated protein PrP 27-30 in water by infrared spectroscopy.

8. Identification of glycoinositol phospholipid linked and truncated forms of the scrapie prion protein.

9. Adenovirus E4-dependent activation of the early E2 promoter is insufficient to promote the early-to-late-phase transition.

10. Scrapie and cellular prion proteins differ in their kinetics of synthesis and topology in cultured cells.

1. Molecular modelling indicates that the pathological conformations of prion proteins might be beta-helical.

2. Immobilized prion protein undergoes spontaneous rearrangement to a conformation having features in common with the infectious form.

3. Affinity-tagged miniprion derivatives spontaneously adopt protease-resistant conformations.

4. Protein engineering as a strategy to avoid formation of amyloid fibrils.

5. Competing intrachain interactions regulate the formation of beta-sheet fibrils in bovine PrP peptides.

6. Strain-specified relative conformational stability of the scrapie prion protein.

7. Molecular dynamics simulations of alanine rich beta-sheet oligomers: Insight into amyloid formation.

8. The stability and dynamics of the human calcitonin amyloid peptide DFNKF.

9. Structural polymorphism in amyloids: new insights from studies with Y145Stop prion protein fibrils.

10. Prion protein (PrP) synthetic peptides induce cellular PrP to acquire properties of the scrapie isoform.