Literature DB >> 22854213

Fibril formation and toxicity of the non-amyloidogenic rat amylin peptide.

Nathaniel G N Milton1, J Robin Harris.   

Abstract

Full-length native rat amylin 1-37 has previously been widely shown to be unable to form fibrils and to lack the toxicity of the human amylin form leading to its use as a non-amyloidogenic control peptide. A recent study has suggested that rat amylin 1-37 forms amyloidogenic β-sheet structures in the presence of the human amylin form and suggested that this property could promote toxicity. Using TEM analysis we show here fibril formation by synthetic rat amylin 1-37 and 8-37 peptides when the lyophilized HPLC purified peptides are initially dissolved in 20 mM Tris-HCl. Dissolution of synthetic rat amylin 1-37 and 8-37 peptides in H(2)O or phosphate buffered saline failed to produce fibrils. Addition of 20 mM Tris-HCl to synthetic rat amylin 1-37 and 8-37 peptides initially dissolved in H(2)O also failed to induce fibril formation. The rat amylin fibrils have a uniform structure and bind Congo red suggesting that they are amyloid fibrils. The rat amylin fibrils also bind catalase, which could be inhibited by Amyloid-β 31-35 and a catalase amyloid-β binding domain-like peptide (R9). The rat amylin 1-37 and 8-37 fibrils are toxic in both human pancreatic islet and neuronal cell culture systems. The toxicity of rat amylin fibrils can be inhibited by an amylin receptor antagonist (AC187) and a caspase inhibitor (zVAD-fmk) in a similar manner to previous observations for human amylin toxicity. Chemically induced rat amylin fibril formation of uniform structured fibrils provides a potentially novel anti-amyloid drug discovery tool.
Copyright © 2012 Elsevier Ltd. All rights reserved.

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Year:  2012        PMID: 22854213     DOI: 10.1016/j.micron.2012.07.001

Source DB:  PubMed          Journal:  Micron        ISSN: 0968-4328            Impact factor:   2.251


  14 in total

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3.  Benzothiazole aniline tetra(ethylene glycol) and 3-amino-1,2,4-triazole inhibit neuroprotection against amyloid peptides by catalase overexpression in vitro.

Authors:  Amrutha Chilumuri; Mark Odell; Nathaniel G N Milton
Journal:  ACS Chem Neurosci       Date:  2013-09-09       Impact factor: 4.418

4.  Preparation and characterization of PEGylated amylin.

Authors:  Luiz Henrique Guerreiro; Mariana F A N Guterres; Bruno Melo-Ferreira; Luiza C S Erthal; Marcela da Silva Rosa; Daniela Lourenço; Priscilla Tinoco; Luís Maurício T R Lima
Journal:  AAPS PharmSciTech       Date:  2013-07-02       Impact factor: 3.246

5.  Time-resolved studies define the nature of toxic IAPP intermediates, providing insight for anti-amyloidosis therapeutics.

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Journal:  Elife       Date:  2016-05-23       Impact factor: 8.140

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Authors:  Amrutha Chilumuri; Maria Ashioti; Amanda N Nercessian; Nathaniel G N Milton
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8.  Monoconjugation of Human Amylin with Methylpolyethyleneglycol.

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Review 9.  On the Environmental Factors Affecting the Structural and Cytotoxic Properties of IAPP Peptides.

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10.  Lessons from two prevalent amyloidoses-what amylin and Aβ have in common.

Authors:  Jürgen Götz; Yun-An Lim; Anne Eckert
Journal:  Front Aging Neurosci       Date:  2013-08-08       Impact factor: 5.750

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