Issue 25, 2010
From the journal:

Dalton Transactions

The C terminus of HspA—a potential target for native Ni(ii) and Bi(iii)anti-ulcer drugs

Magdalena Rowinska-Zyrek,a   Danuta Witkowska,a   Daniela Valensin,b   Wojciech Kamyszc  and  Henryk Kozlowski*a  

* Corresponding authors

a Faculty of Chemistry, University of Wrocław, F. Joliot-Curie 14, Wroclaw, Poland
E-mail: henrykoz@wchuwr.chem.uni.wroc.pl

b Department of Chemistry, University of Siena, Via Aldo Moro, Siena, Italy

c Department of Inorganic Chemistry, Faculty of Pharmacy, Medical University of Gdańsk, Al. Gen. Hallera 107, Gdańsk, Poland

Abstract

HspA, a protein crucial for nickel homeostasis in Helicobacter pylori (H. pylori), has a unique histidine- and cysteine-rich domain at the C terminus. In this work, we compared the coordination of nickel (the natural co-factor) and bismuth (inhibitor) to this domain (Ac-ACCHDHKKH-NH2) and to a reference peptide (Ac-CHCH-NH2). Potentiometric, CD, UV-Vis spectroscopic and NMR methods have shown that bismuth binds incomparably stronger than nickel; the same data shows the impact of histidines on such a binding. Our results are in good agreement with earlier biological data and suggest that HspA can be a potential target of the bismuth anti-ulcer drug against H. pylori.

Graphical abstract: The C terminus of HspA—a potential target for native Ni(ii) and Bi(iii) anti-ulcer drugs

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Article information

DOI
https://doi.org/10.1039/C0DT00013B
Article type
Paper
Submitted
22 Feb 2010
Accepted
26 Apr 2010
First published
25 May 2010

Dalton Trans., 2010,39, 5814-5826

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The C terminus of HspA—a potential target for native Ni(II) and Bi(III) anti-ulcer drugs

M. Rowinska-Zyrek, D. Witkowska, D. Valensin, W. Kamysz and H. Kozlowski, Dalton Trans., 2010, 39, 5814 DOI: 10.1039/C0DT00013B

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