Copper(II) complexes of rat amylin fragments

Csilla Kállay; Agnes Dávid; Sarolta Timári; Eszter Márta Nagy; Daniele Sanna; Eugenio Garribba; Giovanni Micera; Paolo De Bona; Giuseppe Pappalardo; Enrico Rizzarelli; Imre Sóvágó

doi:10.1039/c1dt10835b

Copper(II) complexes of rat amylin fragments

Dalton Trans. 2011 Oct 14;40(38):9711-21. doi: 10.1039/c1dt10835b. Epub 2011 Aug 22.

Authors

Csilla Kállay¹, Agnes Dávid, Sarolta Timári, Eszter Márta Nagy, Daniele Sanna, Eugenio Garribba, Giovanni Micera, Paolo De Bona, Giuseppe Pappalardo, Enrico Rizzarelli, Imre Sóvágó

Affiliation

¹ Department of Inorganic and Analytical Chemistry, University of Debrecen, Hungary. kallay.csilla@science.unideb.hu

PMID: 21858342
DOI: 10.1039/c1dt10835b

Abstract

The fragments of rat amylin rIAPP(17-29) (Ac-VRSSNNLGPVLPP-NH(2)), rIAPP(17-22) (Ac-VRSSNN-NH(2)), rIAPP(19-22) (Ac-SSNN-NH(2)) and rIAPP(17-20) (Ac-VRSS-NH(2)) together with the related mutant peptides (Ac-VASS-NH(2) and Ac-VRAA-NH(2)) have been synthesized and their copper(II) complexes studied by potentiometric, UV-Vis, CD and EPR spectroscopic methods. Despite the lack of any common strongly coordinating donor functions some of these fragments are able to bind copper(II) ions in the physiological pH range. The longest fragment rat amylin(17-29) keeps one equivalent copper(II) ion in solution in the whole pH range, while two other peptides Ac-VRSSNN-NH(2) and Ac-SSNN-NH(2) are also able to interact with copper(II) ions in the slightly alkaline pH range. According to the spectral parameters of the complexes, the peptides can be classified into two different categories: (i) the tetrapeptides Ac-VRSS-NH(2), Ac-VASS-NH(2) and Ac-VRAA-NH(2) can interact with copper(II) only under strongly alkaline conditions (pH > 10.0) and the formation of only one species with four amide nitrogen coordination can be detected; (ii) the peptides Ac-VRSSNNLGPVLPP-NH(2), Ac-VRSSNN-NH(2) and Ac-SSNN-NH(2) can form complexes above pH 6.0 with the major stoichiometries [CuH(-2)L], [CuH(-3)L](-) and [CuH(-4)L](2-). These data support that rIAPP(17-29) can interact with copper(II) ions under physiological conditions and the SSNN tetrapeptide fragment can be considered as the shortest sequence responsible for metal binding. Density functional theory (DFT) calculations provide some information on the possible coordination modes of Ac-SSNN-NH(2) towards the copper(II) ion and suggest that for [CuH(-2)L], [CuH(-3)L](-) and [CuH(-4)L](2-), the binding of two, three and four deprotonated amide nitrogens, with NH(-) of the side chain of asparagine as anchoring group, is probable. Moreover, these data reveal that peptides can be effective metal binding ligands even in the absence of anchoring groups, if more polar side chains are present in a specific sequence.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amino Acid Sequence
Animals
Copper / chemistry*
Humans
Islet Amyloid Polypeptide / chemistry*
Ligands
Molecular Sequence Data
Molecular Structure
Organometallic Compounds / chemical synthesis
Organometallic Compounds / chemistry*
Organometallic Compounds / pharmacology
Quantum Theory
Rats

Substances

Islet Amyloid Polypeptide
Ligands
Organometallic Compounds
Copper