Detailed investigation of the binding abilities of the heterodomain of a multiHis cyclopeptide toward Cu(II) ions

Author:

Bortolus Marco1,Kotynia Aleksandra2,Saielli Giacomo13,Ruzza Paolo4,Di Valentin Marilena1,Carraro Mauro13ORCID,Brasuń Justyna2

Affiliation:

1. Department of Chemical Sciences University of Padova Padova Italy

2. Department of Basic Chemical Sciences Wroclaw Medical University Wroclaw Poland

3. Padova Unit Institute on Membrane Technology of CNR Padova Italy

4. Padova Unit Institute of Biomolecular Chemistry of CNR Padova Italy

Abstract

Cyclopeptides hold significant relevance in various fields of science and medicine, due to their unique structural properties and diverse biological activities. Cyclic peptides, characterized by intrinsically higher conformational order, exhibit remarkable stability and resistance to proteolytic degradation, making them attractive candidates for developing targeted drug delivery systems. The aim of this work is to elucidate the unique coordination properties of the multi‐His cyclic peptide with c(HDHKHPHHKHHP) sequence (HDCP – heterodomain cyclopeptide). This peptide, indeed, is able to form homo‐ and hetero‐dinuclear complexes in a wide pH range, being thus a good chelator for Cu(II) ions. Herein, we present the results of a combined study, involving potentiometric, spectroscopic (UV–Vis, CD, and EPR), and computational investigations, on its coordination properties. To better understand the interaction pattern with Cu(II) metal ions, two other peptides, each one bearing only one of the two binding domains of HDCP are also considered in this study: c(HDHKHPGGKGGP) = CP1, c(GKGGKPHHKHHP) = CP2, which share sequence fragments of HDCP and allow separate investigations of its coordination domains.

Funder

Dipartimento di Scienze Chimiche, Università degli Studi di Padova

Murphy Institute, Tulane University

Publisher

Wiley

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