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Literature DB >> 9445012

Overexpression of nonconvertible PrPc delta114-121 in scrapie-infected mouse neuroblastoma cells leads to trans-dominant inhibition of wild-type PrP(Sc) accumulation.

Abstract

One hallmark of prion diseases is the accumulation of the abnormal isoform PrP(Sc) of a normal cellular glycoprotein, PrPc, which is characterized by a high content of beta-sheet structures and by its partial resistance to proteinase K. It was hypothesized that the PrP region comprising amino acid residues 109 to 122 [PrP(109-122)], which spontaneously forms amyloid when it is synthesized as a peptide but which does not display significant secondary structure in the context of the full-length PrPc molecule, should play a role in promoting the conversion into PrP(Sc). By using persistently scrapie-infected mouse neuroblastoma (Sc+-MNB) cells as a model system for prion replication, we set out to design dominant-negative mutants of PrPc that are capable of blocking the conversion of endogenous, wild-type PrPc into PrP(Sc). We constructed a deletion mutant (PrPc delta114-121) lacking eight codons that span most of the highly amyloidogenic part, AGAAAAGA, of PrP(109-122). Transient transfections of mammalian expression vectors encoding either wild-type PrPc or PrPc delta114-121 into uninfected mouse neuroblastoma cells (Neuro2a) led to overexpression of the respective PrPc versions, which proved to be correctly localized on the extracellular face of the plasma membrane. Transfection of Sc+-MNB cells revealed that PrPc delta114-121 was not a substrate for conversion into a proteinase K-resistant isoform. Furthermore, its presence led to a significant reduction in the steady-state levels of PrP(Sc) derived from endogenous PrPc. Thus, we showed that the presence of amino acids 114 to 121 of mouse PrPc plays an important role in the conversion process of PrPc into PrP(Sc) and that a deletion mutant lacking these codons indeed behaves as a dominant-negative mutant with respect to PrP(Sc) accumulation. This mechanism could form a basis for a new gene therapy and/or a prevention concept for prion diseases.

Entities: Disease Gene Species

Mesh：

Substances：

Year: 1998 PMID： 9445012 PMCID： PMC124590

Source DB: PubMed Journal: J Virol ISSN： 0022-538X Impact factor: 5.103

48 in total

Review 1. The prion folding problem.

Authors: P M Harrison; P Bamborough; V Daggett; S B Prusiner; F E Cohen
Journal: Curr Opin Struct Biol Date: 1997-02 Impact factor: 6.809

2. Partial unfolding and refolding of scrapie-associated prion protein: evidence for a critical 16-kDa C-terminal domain.

Authors: D A Kocisko; P T Lansbury; B Caughey
Journal: Biochemistry Date: 1996-10-15 Impact factor: 3.162

3. Cleavage of structural proteins during the assembly of the head of bacteriophage T4.

Authors: U K Laemmli
Journal: Nature Date: 1970-08-15 Impact factor: 49.962

4. Mice devoid of PrP are resistant to scrapie.

Authors: H Büeler; A Aguzzi; A Sailer; R A Greiner; P Autenried; M Aguet; C Weissmann
Journal: Cell Date: 1993-07-02 Impact factor: 41.582

5. Synthesis and trafficking of prion proteins in cultured cells.

Authors: A Taraboulos; A J Raeber; D R Borchelt; D Serban; S B Prusiner
Journal: Mol Biol Cell Date: 1992-08 Impact factor: 4.138

6. Neurotoxicity of a prion protein fragment.

Authors: G Forloni; N Angeretti; R Chiesa; E Monzani; M Salmona; O Bugiani; F Tagliavini
Journal: Nature Date: 1993-04-08 Impact factor: 49.962

7. Molecular cloning and complete sequence of prion protein cDNA from mouse brain infected with the scrapie agent.

Authors: C Locht; B Chesebro; R Race; J M Keith
Journal: Proc Natl Acad Sci U S A Date: 1986-09 Impact factor: 11.205

8. Normal host prion protein necessary for scrapie-induced neurotoxicity.

Authors: S Brandner; S Isenmann; A Raeber; M Fischer; A Sailer; Y Kobayashi; S Marino; C Weissmann; A Aguzzi
Journal: Nature Date: 1996-01-25 Impact factor: 49.962

9. Prion protein (PrP) with amino-proximal deletions restoring susceptibility of PrP knockout mice to scrapie.

Authors: M Fischer; T Rülicke; A Raeber; A Sailer; M Moser; B Oesch; S Brandner; A Aguzzi; C Weissmann
Journal: EMBO J Date: 1996-03-15 Impact factor: 11.598

10. A single hamster PrP amino acid blocks conversion to protease-resistant PrP in scrapie-infected mouse neuroblastoma cells.

Authors: S A Priola; B Chesebro
Journal: J Virol Date: 1995-12 Impact factor: 5.103

40 in total

1. Specific binding of normal prion protein to the scrapie form via a localized domain initiates its conversion to the protease-resistant state.

Authors: M Horiuchi; B Caughey
Journal: EMBO J Date: 1999-06-15 Impact factor: 11.598

2. Nucleation-dependent conformational conversion of the Y145Stop variant of human prion protein: structural clues for prion propagation.

Authors: Bishwajit Kundu; Nilesh R Maiti; Eric M Jones; Krystyna A Surewicz; David L Vanik; Witold K Surewicz
Journal: Proc Natl Acad Sci U S A Date: 2003-09-30 Impact factor: 11.205

10. The region approximately between amino acids 81 and 137 of proteinase K-resistant PrPSc is critical for the infectivity of the Chandler prion strain.

Authors: Ryo Shindoh; Chan-Lan Kim; Chang-Hyun Song; Rie Hasebe; Motohiro Horiuchi
Journal: J Virol Date: 2009-01-28 Impact factor: 5.103

Overexpression of nonconvertible PrPc delta114-121 in scrapie-infected mouse neuroblastoma cells leads to trans-dominant inhibition of wild-type PrP(Sc) accumulation.

Review 1. The prion folding problem.

2. Partial unfolding and refolding of scrapie-associated prion protein: evidence for a critical 16-kDa C-terminal domain.

3. Cleavage of structural proteins during the assembly of the head of bacteriophage T4.

4. Mice devoid of PrP are resistant to scrapie.

5. Synthesis and trafficking of prion proteins in cultured cells.

6. Neurotoxicity of a prion protein fragment.

7. Molecular cloning and complete sequence of prion protein cDNA from mouse brain infected with the scrapie agent.

8. Normal host prion protein necessary for scrapie-induced neurotoxicity.

9. Prion protein (PrP) with amino-proximal deletions restoring susceptibility of PrP knockout mice to scrapie.

10. A single hamster PrP amino acid blocks conversion to protease-resistant PrP in scrapie-infected mouse neuroblastoma cells.

1. Specific binding of normal prion protein to the scrapie form via a localized domain initiates its conversion to the protease-resistant state.

2. Nucleation-dependent conformational conversion of the Y145Stop variant of human prion protein: structural clues for prion propagation.

3. Optimal molecular structures of prion AGAAAAGA amyloid fibrils formatted by simulated annealing.

4. Enhanced stability of human prion proteins with two disulfide bridges.

5. Lethal recessive myelin toxicity of prion protein lacking its central domain.

6. Cofactor molecules induce structural transformation during infectious prion formation.

7. Design of metastable β-sheet oligomers from natively unstructured peptide.

8. Stress-protective signalling of prion protein is corrupted by scrapie prions.

Review 9. Probing the role of structural features of mouse PrP in yeast by expression as Sup35-PrP fusions.

10. The region approximately between amino acids 81 and 137 of proteinase K-resistant PrPSc is critical for the infectivity of the Chandler prion strain.