Literature DB >> 17953525

Induction of murine AA amyloidosis by various homogeneous amyloid fibrils and amyloid-like synthetic peptides.

Y Liu1, D Cui, Y Hoshii, H Kawano, Y Une, T Gondo, T Ishihara.   

Abstract

We investigated amyloid-enhancing factor (AEF) activity of amyloid fibrils extracted from amyloid-laden livers of mice, cow, cheetah, cat and swan. All amyloid fibrils were confirmed to be amyloid protein A (AA) by an immunohistochemical analysis. We found that these fibrils accelerated the deposition of amyloid in an experimental mouse model of AA amyloidosis. Furthermore, the degree of deposition was dependent on the concentration of fibrils. When we compared the minimal concentration of amyloid fibrils needed to induce deposition, we found that these fibrils showed different efficiencies. Murine amyloid fibril induced amyloid deposition more efficiently than cow, cat, cheetah or swan amyloid fibrils. These data suggest that amyloid deposition is preferentially induced by amyloid fibrils with the same primary sequence as the endogenous amyloid protein. We then analysed the AEF activity of synthetic peptides, synthesized corresponding to amino acids 1-15 of mouse SAA (mSAA), 2-15 of cow SAA (bSAA), 1-15 of cat SAA (cSAA), which was the same as cheetah, and the common amino acids 33-45 of these four SAA (aSAA). We found that mSAA, bSAA and cSAA formed amyloid-like fibrils in morphology and showed similar AEF properties to those of native amyloid fibrils. Although aSAA also formed highly ordered amyloid-like fibrils, it showed weaker AEF activity than the other synthetic fibrils. Our results indicate that amyloidosis is transmissible between species under certain conditions; however, the efficiency of amyloid deposition is species-specific and appears to be related to the primary amino acid sequence, especially the N-terminal segment of the amyloid protein.

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Year:  2007        PMID: 17953525     DOI: 10.1111/j.1365-3083.2007.02005.x

Source DB:  PubMed          Journal:  Scand J Immunol        ISSN: 0300-9475            Impact factor:   3.487


  8 in total

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Review 2.  Noncerebral Amyloidoses: Aspects on Seeding, Cross-Seeding, and Transmission.

Authors:  Gunilla T Westermark; Marcus Fändrich; Katarzyna Lundmark; Per Westermark
Journal:  Cold Spring Harb Perspect Med       Date:  2018-01-02       Impact factor: 6.915

3.  Systemic Amyloid A Amyloidosis in Island Foxes (Urocyon littoralis): Severity and Risk Factors.

Authors:  P M Gaffney; C Witte; D L Clifford; D M Imai; T D O'Brien; M Trejo; F Liberta; K Annamalai; M Fändrich; E Masliah; L Munson; C J Sigurdson
Journal:  Vet Pathol       Date:  2015-09-29       Impact factor: 2.221

4.  Species-barrier on the cross-species oral transmission of bovine AA amyloidosis in mice.

Authors:  Susumu Iwaide; Naoki Ujike; Kyoko Kobayashi; Yukiko Sassa; Tomoaki Murakami
Journal:  J Vet Med Sci       Date:  2021-04-28       Impact factor: 1.267

5.  Experimental transmission of systemic AA amyloidosis in autoimmune disease and type 2 diabetes mellitus model mice.

Authors:  Mayuko Maeda; Tomoaki Murakami; Naeem Muhammad; Yasuo Inoshima; Naotaka Ishiguro
Journal:  Exp Anim       Date:  2016-06-16

Review 6.  No effects without causes: the Iron Dysregulation and Dormant Microbes hypothesis for chronic, inflammatory diseases.

Authors:  Douglas B Kell; Etheresia Pretorius
Journal:  Biol Rev Camb Philos Soc       Date:  2018-03-25

7.  Oxazolone-induced gastrointestinal disorders enhance the oral transmission of AA amyloidosis in mice.

Authors:  Hiroto Kobayashi; Susumu Iwaide; Naoki Ujike; Tomoaki Murakami
Journal:  J Vet Med Sci       Date:  2021-04-20       Impact factor: 1.267

8.  Variation of amino acid sequences of serum amyloid a (SAA) and immunohistochemical analysis of amyloid a (AA) in Japanese domestic cats.

Authors:  Meina Tei; Kazuyuki Uchida; James K Chambers; Ken-Ichi Watanabe; Takashi Tamamoto; Koichi Ohno; Hiroyuki Nakayama
Journal:  J Vet Med Sci       Date:  2017-12-04       Impact factor: 1.267

  8 in total

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