http://www.cnr.it/ontology/cnr/individuo/prodotto/ID56153

Potential pathogenic role of beta-amyloid(1-42)-aluminum complex in Alzheimer's disease (Articolo in rivista)

Type

Articolo in rivista (Classe)
Prodotto della ricerca (Classe)

Label

Potential pathogenic role of beta-amyloid(1-42)-aluminum complex in Alzheimer's disease (Articolo in rivista) (literal)

Anno

2008-01-01T00:00:00+01:00 (literal)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#doi

10.1016/j.biocel.2007.10.014 (literal)

Alternative label

Drago D; Bettella M; Bolognin S; Cendron L; Scancar J; Milacic R; Ricchelli F; Casini A; Messori L; Tognon G; Zatta P (2008)
Potential pathogenic role of beta-amyloid(1-42)-aluminum complex in Alzheimer's disease
in International journal of biochemistry & cell biology
(literal)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#autori

Drago D; Bettella M; Bolognin S; Cendron L; Scancar J; Milacic R; Ricchelli F; Casini A; Messori L; Tognon G; Zatta P (literal)

Pagina inizio

731 (literal)

Pagina fine

746 (literal)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#numeroVolume

40 (literal)

Rivista

International journal of biochemistry & cell biology (Rivista)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#numeroFascicolo

4 (literal)

Note

ISI Web of Science (WOS) (literal)

Http://www.cnr.it/ontology/cnr/pubblicazioni.owl#affiliazioni

Drago D, Bettella M, Bolognin S, Cendron L, Università di Padova; Scancar J, Milacic R, Jozef Stefan Institute, Ljubljana, Slovenia; Casini A, Messori L, Università di Firenze; Ricchelli F, Tognon G, Zatta P, CNR (literal)

Titolo

Potential pathogenic role of beta-amyloid(1-42)-aluminum complex in Alzheimer's disease (literal)

Abstract

The etiopathogenesis of Alzheimer's disease is far from being clearly understood. However, the involvement of metal ions as a potential key factor towards conformational modifications and aggregation of amyloid is widely recognized. The aim of the present study is to shed some light on the relationship between metal ions, amyloid conformation/aggregation, and their potential relationship with the conformational aspects of AD.We compare the effects of ?-amyloid1-42 and its various metal complexes (b-amyloid-Al, b-amyloid-Zn, b-amyloid-Cu, b-amyloid-Fe) in human neuroblastoma cells in terms of cell viability, membrane structure properties, and cell morphology. No significant toxic effects were observed in neuroblastoma cells after 24 h treatment both with b-amyloid and b-amyloid-metals (b-amyloid-Zn, b-amyloid-Cu, b-amyloid-Fe); on the other hand, there was a marked reduction of cellular viability after treatment with b-amyloid-Al complex. In addition, treatment with b-amyloid-Al increased membrane fluidity much more than other b-amyloid-metal complexes, whose contribution was negligible. Furthermore, the cellular morphology, as observed by electron microscopy,was deeply altered by b-amyloid-Al. Importantly, b-amyloid-Al toxicity is closely and significantly associated with a great difference in the structure/aggregation of this complex with respect to that of b-amyloid alone and other b-amyloid-metal complexes. In addition, b-amyloid, as a consequence of Al binding, becomes strongly hydrophobic in character. These findings show a significant involvement of Al, compared to the other metal ions used in our experiments, in promoting a specific amyloid 1-42 aggregation, which is able to produce marked toxic effects on neuroblastoma cells, as clearly demonstrated for the first time in this study (literal)

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