Facile Synthesis of Hemin Derivatives with Modulated Aggregation Behaviour and Enhanced Nitric‐Oxide Scavenging Properties as New Therapeutics for Breast Cancer

Author:

Alsharabasy Amir M.1ORCID,Cherukaraveedu Durgadas1ORCID,Warneke Jonas23ORCID,Warneke Ziyan2,Galán‐Mascarós José Ramón45ORCID,Glynn Sharon A.16ORCID,Farràs Pau17ORCID,Pandit Abhay1ORCID

Affiliation:

1. CÚRAM SFI Research Centre for Medical Devices University of Galway H91 W2TY Galway Ireland

2. Wilhelm‐Ostwald‐Institut für Physikalische und Theoretische Chemie Universität Leipzig 04103 Leipzig Germany

3. Leibniz Institute of Surface Engineering (IOM) Permoserstraße 15 04318 Leipzig Germany

4. Institute of Chemical Research of Catalonia (ICIQ) The Barcelona Institute of Science and Technology (BIST) Av. Països Catalans 16 ES‐43007 Tarragona Spain

5. Catalan Institution for Research and Advanced Studies (ICREA) Passeig Lluis Companys 16 ES‐08007 Barcelona Spain

6. Discipline of Pathology Lambe Institute for Translational Research School of Medicine University of Galway H91 YR71 Galway Ireland

7. School of Biological and Chemical Sciences Ryan Institute University of Galway H91 TK33 Galway Ireland

Abstract

Nitric oxide (NO) plays various pathophysiological roles in breast cancer, significantly influencing the migration of tumour cells through concentration gradients. Therefore, modulating NO levels via selective scavenging presents a promising approach to treating aggressive NO‐dependent cancers, such as triple‐negative breast cancer (TNBC). Hemin emerges as a potential scavenger of NO; however, its metalloporphyrin molecules tend to aggregate in physiological solutions, which limits its biomedical applications. To address this, a modification strategy is employed to minimize aggregation and protect against physiological oxidative degradation while preserving NO‐scavenging properties. This is achieved through a simple chemical transformation that involves hemin conjugation to aromatic residues, tyrosine, and tyramine via carbodiimide reactions. These derivatives exhibit altered electronic properties and oxidation potential compared to hemin, alongside reduced aggregation tendencies and retained NO‐binding affinity in aqueous solutions. Furthermore, depending on the type of hemin derivative, there is an associated inhibition of TNBC cell migration. These model hemin compounds demonstrate varying NO‐binding affinities and resistance levels to oxidative degradation and aggregation, offering insights into the design of NO‐scavenging molecules with enhanced properties for cancer treatment.

Funder

Science Foundation Ireland

Irish Research Council

Ministerio de Ciencia e Innovación

Generalitat de Catalunya

Publisher

Wiley

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