The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine Complexes

The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine Complexes

Metallation of biomacromolecular species forms the basis for the anticancer activity of many metallodrugs. A major limitation of these compounds is that their reactivity is indiscriminate and can, in principle, occur in healthy tissue as well as cancerous tissue, potentially leading to side effects...

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Main Authors: Samuel A. Kemp, Timothy J. Prior, Huguette Savoie, Ross W. Boyle, Benjamin S. Murray
Format: Article
Language:English
Published: MDPI AG 2020-01-01
Series:Molecules
Subjects:
metallodrugs
bioorganometallic chemistry
ruthenium
cancer
sulfonamide
Online Access:https://www.mdpi.com/1420-3049/25/2/244
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spelling doaj-0832581b2899437281487000a970769d2020-11-25T02:13:03ZengMDPI AGMolecules1420-30492020-01-0125224410.3390/molecules25020244molecules25020244The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine ComplexesSamuel A. Kemp0Timothy J. Prior1Huguette Savoie2Ross W. Boyle3Benjamin S. Murray4Department of Chemistry and Biochemistry, University of Hull, Cottingham Road, Hull HU6 7RX, UKDepartment of Chemistry and Biochemistry, University of Hull, Cottingham Road, Hull HU6 7RX, UKDepartment of Chemistry and Biochemistry, University of Hull, Cottingham Road, Hull HU6 7RX, UKDepartment of Chemistry and Biochemistry, University of Hull, Cottingham Road, Hull HU6 7RX, UKDepartment of Chemistry and Biochemistry, University of Hull, Cottingham Road, Hull HU6 7RX, UKMetallation of biomacromolecular species forms the basis for the anticancer activity of many metallodrugs. A major limitation of these compounds is that their reactivity is indiscriminate and can, in principle, occur in healthy tissue as well as cancerous tissue, potentially leading to side effects in vivo. Here we present pH-dependent intramolecular coordination of an arene-tethered sulfonamide functionality in organometallic ruthenium(II) ethylenediamine complexes as a route to controlling the coordination environment about the central metal atom. Through variation of the sulfonamide R group and the length of the tether linking it to the arene ligand the acidity of the sulfonamide NH group, and hence the pH-region over which regulation of metal coordination occurs, can be modulated. Intramolecular sulfonamide ligation controlled the reactivity of complex <b>4</b> within the physiologically relevant pH-region, rendering it more reactive towards 5ʹ-GMP in mildly acidic pH-conditions typical of tumour tissue compared to the mildly alkaline pH-conditions typical of healthy tissue. However, the activation of <b>4</b> by ring-opening of the chelate was found to be a slow process relative to the timescale of typical cell culture assays and members of this series of complexes were found not to be cytotoxic towards the HT-29 cell line. These complexes provide the basis for the development of analogues of increased potency where intramolecular sulfonamide ligation regulates reactivity and therefore cytotoxicity in a pH-dependent, and potentially, tissue-dependent manner.https://www.mdpi.com/1420-3049/25/2/244metallodrugsbioorganometallic chemistryrutheniumcancersulfonamide
collection DOAJ
language English
format Article
sources DOAJ
author Samuel A. Kemp
Timothy J. Prior
Huguette Savoie
Ross W. Boyle
Benjamin S. Murray
spellingShingle Samuel A. Kemp
Timothy J. Prior
Huguette Savoie
Ross W. Boyle
Benjamin S. Murray
The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine Complexes
Molecules
metallodrugs
bioorganometallic chemistry
ruthenium
cancer
sulfonamide
author_facet Samuel A. Kemp
Timothy J. Prior
Huguette Savoie
Ross W. Boyle
Benjamin S. Murray
author_sort Samuel A. Kemp
title The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine Complexes
title_short The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine Complexes
title_full The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine Complexes
title_fullStr The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine Complexes
title_full_unstemmed The Application of Reversible Intramolecular Sulfonamide Ligation to Modulate Reactivity in Organometallic Ruthenium(II) Diamine Complexes
title_sort application of reversible intramolecular sulfonamide ligation to modulate reactivity in organometallic ruthenium(ii) diamine complexes
publisher MDPI AG
series Molecules
issn 1420-3049
publishDate 2020-01-01
description Metallation of biomacromolecular species forms the basis for the anticancer activity of many metallodrugs. A major limitation of these compounds is that their reactivity is indiscriminate and can, in principle, occur in healthy tissue as well as cancerous tissue, potentially leading to side effects in vivo. Here we present pH-dependent intramolecular coordination of an arene-tethered sulfonamide functionality in organometallic ruthenium(II) ethylenediamine complexes as a route to controlling the coordination environment about the central metal atom. Through variation of the sulfonamide R group and the length of the tether linking it to the arene ligand the acidity of the sulfonamide NH group, and hence the pH-region over which regulation of metal coordination occurs, can be modulated. Intramolecular sulfonamide ligation controlled the reactivity of complex <b>4</b> within the physiologically relevant pH-region, rendering it more reactive towards 5ʹ-GMP in mildly acidic pH-conditions typical of tumour tissue compared to the mildly alkaline pH-conditions typical of healthy tissue. However, the activation of <b>4</b> by ring-opening of the chelate was found to be a slow process relative to the timescale of typical cell culture assays and members of this series of complexes were found not to be cytotoxic towards the HT-29 cell line. These complexes provide the basis for the development of analogues of increased potency where intramolecular sulfonamide ligation regulates reactivity and therefore cytotoxicity in a pH-dependent, and potentially, tissue-dependent manner.
topic metallodrugs
bioorganometallic chemistry
ruthenium
cancer
sulfonamide
url https://www.mdpi.com/1420-3049/25/2/244
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