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Potentiometric and spectroscopic data have shown that octarepeat dimer and tetramer are much more effective ligands for Cu(II) ions than simple octapeptide. Thus, the whole N-terminal segment of prion protein due to cooperative effects, could be more effective in binding of Cu(II) than simple peptides containing a His residue. The gain of the Cu(II) binding by longer octarepeat peptides derives from the involvement of up to four imidazoles in the coordination of the first Cu(II) ion. This type of binding increases the order of the peptide structure, which allows successive metal ions for easier coordination.

Valensin, D., Luczkowski, M., Mancini, F., Legowska, A., Gaggelli, E., Rolka, K., et al. (2004). The dimeric and tetrameric octarepeat fragment of prion behaves differently to its monomeric unit. DALTON TRANSACTIONS, 2004(9), 1284-1293 [10.1039/b402090a].

The dimeric and tetrameric octarepeat fragment of prion behaves differently to its monomeric unit

Valensin, Daniela;Gaggelli, Elena;Valensin, Gianni;
2004-01-01

Abstract

Potentiometric and spectroscopic data have shown that octarepeat dimer and tetramer are much more effective ligands for Cu(II) ions than simple octapeptide. Thus, the whole N-terminal segment of prion protein due to cooperative effects, could be more effective in binding of Cu(II) than simple peptides containing a His residue. The gain of the Cu(II) binding by longer octarepeat peptides derives from the involvement of up to four imidazoles in the coordination of the first Cu(II) ion. This type of binding increases the order of the peptide structure, which allows successive metal ions for easier coordination.
2004
DALTON TRANSACTIONS
Valensin, D., Luczkowski, M., Mancini, F., Legowska, A., Gaggelli, E., Rolka, K., et al. (2004). The dimeric and tetrameric octarepeat fragment of prion behaves differently to its monomeric unit. DALTON TRANSACTIONS, 2004(9), 1284-1293 [10.1039/b402090a].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11365/18947
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