Literature DB >> 23857314

Vitamin D 2 interacts with Human PrP(c) (90-231) and breaks PrP(c) oligomerization in vitro.

Midori Suenaga1, Yusuke Hiramoto, Yoichi Matsunaga.   

Abstract

PrP(sc), the pathogenic isoform of PrP(c), can convert PrP(c) into PrP(sc) through direct interactions. PrP(c) oligomerization is a required processing step before PrP(sc) formation, and soluble oligomers appear to be the toxic species in amyloid-related disorders. In the current study, direct interactions between vitamin D 2 and human recombinant PrP(c) (90-231) were observed by Biacore assay, and 3F4 antibody, specific for amino acid fragment 109-112 of PrP(c), inhibited this interaction. An ELISA study using3F4 antibody showed that PrP(c) (101-130), corresponding sequence to human PrP, was affected by vitamin D 2, supporting the results of Biacore studies and suggesting that the PrP(c) sequence around the 3F4 epitope was responsible for the interaction with vitamin D 2. Furthermore, the effects of vitamin D 2 on disruption of PrP(c) (90-231) oligomerization were elucidated by dot blot analysis and differential protease k susceptibilities. While many chemical compounds have been proposed as potential therapeutic agents for the treatment of scrapie, most of these are toxic. However, given the safety and blood brain barrier permeability of vitamin D 2, we propose that vitamin D 2 may be a suitable agent to target PrP(c) in the brain and therefore is a potential therapeutic candidate for prion disease.

Entities:  

Keywords:  PrPc; PrPsc; oligomerization; prion disease; vitamin D2

Mesh:

Substances:

Year:  2013        PMID: 23857314      PMCID: PMC3904317          DOI: 10.4161/pri.25739

Source DB:  PubMed          Journal:  Prion        ISSN: 1933-6896            Impact factor:   3.931


  45 in total

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Review 2.  BIACORE: an affinity biosensor system for characterization of biomolecular interactions.

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6.  25-Hydroxylase activity in subcellular fractions from human liver. Evidence for different rates of mitochondrial hydroxylation of vitamin D2 and D3.

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7.  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

8.  Unique 24-hydroxylated metabolites represent a significant pathway of metabolism of vitamin D2 in humans: 24-hydroxyvitamin D2 and 1,24-dihydroxyvitamin D2 detectable in human serum.

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9.  Identification and characterization of a spontaneously aggregating amyloid-forming variant of human PrP((90-231)) through phage-display screening of variants randomized between residues 101 and 112.

Authors:  Archana Verma; Swati Sharma; Nirmal Kumar Ganguly; Siddharta Majumdar; Purnananda Guptasarma; Manni Luthra-Guptasarma
Journal:  Int J Biochem Cell Biol       Date:  2007-10-13       Impact factor: 5.085

10.  Contribution of two conserved glycine residues to fibrillogenesis of the 106-126 prion protein fragment. Evidence that a soluble variant of the 106-126 peptide is neurotoxic.

Authors:  Tullio Florio; Domenico Paludi; Valentina Villa; Daniela Rossi Principe; Alessandro Corsaro; Enrico Millo; Gianluca Damonte; Cristina D'Arrigo; Claudio Russo; Gennaro Schettini; Antonio Aceto
Journal:  J Neurochem       Date:  2003-04       Impact factor: 5.372

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  1 in total

1.  Vitamin D protects dopaminergic neurons against neuroinflammation and oxidative stress in hemiparkinsonian rats.

Authors:  Ludmila A R Lima; Maria Janice P Lopes; Roberta O Costa; Francisco Arnaldo V Lima; Kelly Rose T Neves; Iana B F Calou; Geanne M Andrade; Glauce S B Viana
Journal:  J Neuroinflammation       Date:  2018-08-31       Impact factor: 8.322

  1 in total

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