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Metal ion binding to amyloid peptide fragments: Biochemical and biomedical involvement
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Chemical Sciences Journal

ISSN: 2150-3494

Open Access

Metal ion binding to amyloid peptide fragments: Biochemical and biomedical involvement


8th European Chemistry Congress

June 21-23, 2018 | Paris, France

Marius Closca, M Murariu, M Manea and GDrochioiu

Al I Cuza University of Iasi, Romania
Petru Poni Institute of Macromolecular Chemistry of Iasi, Romania
Konstanz University, Germany

Posters & Accepted Abstracts: Chem Sci J

Abstract :

Biochemistry of Alzheimerâ��s disease (AD) is related to the conformational changes of amyloid-�² peptides, which result in peptide oligomerization and fibril formation and, finally, in the appearance of senile plaques and extensive neuronal loss. Unfortunately, the factors regulating the process of plaque-associated beta-amyloid peptide (A�²) aggregation are only partly understood. �²-Amyloid peptide fragments have been synthesized by SPPS according to Boc/Bzl strategy. Binding of metal ions to �²-amyloid peptides was studied at pH 7.4 or 6.6. It was found that A�²(1-10) peptide binds only one Cu(II) ion at pH 7.4. However, the intensity of peak corresponding to the doubly charged ion [M+Cu]2+ increases significantly with time and copper concentration. A�²(1-16) peptide may bind one Cu(II) at 1:1 and 1:2 peptide-Cu ratio, and one and two Cu(II) at a peptide-Cu ratio of 1:10. Copper binding to A�² fragments changed much the peptide conformation. MS spectra showed metal-induced aggregation, especially at pH 7.4. During the binding of Cu(II) to N-terminal truncated �²-amyloid peptides, no copper ion was found to bind to A�²(31-40) at 1:1 and 1:2 peptide: Cu(II) ratios. At 1:10 peptide-metal ion ratio, a low intense peak corresponding to [M+Cu]2+ ion was detected by ESI-MS after 7-8 min incubation of peptide-metal ion. A close relationship between pH, metal concentration and the proportion of conformers of A�² fragments was found, as well. Copper ions bind strongly and specifically to �²-amyloid(1-40) peptide and to its N- and C-terminal truncated versions. Our ESIMS investigation showed that the C-terminal 31-40 sequence is not involved in copper binding. Our results also prove that Zn(II) has lower affinity toward A�²-peptides as compared to Cu(II). At 1:10 peptide-Zn(II), no peaks corresponding to the A�²-peptides was detected by ESI-MS, were an aggregation process was suspected. Our data is discussed in the light of recent literature on neurodegeneration biochemistry.

Biography :

Marius Closca is a PhD student of Alexandru Ioan Cuza University of Iasi, Romania, department of chemistry in the field of biochemistry 2017 to present. The short scientific experience is confirmed by the scientific results obtained in the field of organic chemistry and biochemistry, results included in one paper in Journals accredited by CNCSIS (category B and C) and a participation at the conference of faculty of chemistry Iasi CHEM 2017, IaÃ?Â?i, Romania, 26-28 October 2017.

E-mail: marius.chc@gmail.com

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Citations: 912

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