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Binding of Gold(III) Porphyrin by the Pro-metastatic Regulatory Protein Human Galectin-3

Gold(III) porphyrin presents an attractive alternative to the use of, for example, cisplatin in chemotherapy. However, approaches that allow to selectively target cancer cells are highly sought. Many plant and mammalian lectins have been shown to bind oligosaccharide sequences of the aberrant glycos...

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Autores principales: Bogoeva, Vanya, Rangelov, Miroslav, Todorova, Nadezhda, Lambert, Annie, Bridot, Clarisse, Yordanova, Anna, Roos, Goedele, Grandjean, Cyrille, Bouckaert, Julie
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6943629/
https://www.ncbi.nlm.nih.gov/pubmed/31842510
http://dx.doi.org/10.3390/molecules24244561
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author Bogoeva, Vanya
Rangelov, Miroslav
Todorova, Nadezhda
Lambert, Annie
Bridot, Clarisse
Yordanova, Anna
Roos, Goedele
Grandjean, Cyrille
Bouckaert, Julie
author_facet Bogoeva, Vanya
Rangelov, Miroslav
Todorova, Nadezhda
Lambert, Annie
Bridot, Clarisse
Yordanova, Anna
Roos, Goedele
Grandjean, Cyrille
Bouckaert, Julie
author_sort Bogoeva, Vanya
collection PubMed
description Gold(III) porphyrin presents an attractive alternative to the use of, for example, cisplatin in chemotherapy. However, approaches that allow to selectively target cancer cells are highly sought. Many plant and mammalian lectins have been shown to bind oligosaccharide sequences of the aberrant glycosylation pattern found on cancerous tumors. For example human galectin-3, of the galectin family specific for β-galactoside, is overexpressed in the extracellular matrix of tumorigenous and metastatic tissues. We searched for non-carbohydrate ligands for galectin-3 that can guide a cytotoxic drug to the cancer cells by maintaining its affinity for tumor associated carbohydrate antigens. Previous findings showed that zinc tetrasulfonatophenylporphyrin can bind galectin-3 with sub-micromolar affinity without disturbing lactose binding. Gold(III) porphyrin is not only cytotoxic to cancer cells, it knows also a potential application as photosensitiser in photodynamic therapy. We investigated the binding of gold(III) porphyrin to galectin-3 using different biophysical interaction techniques and demonstrated a low micromolar affinity of human galectin-3 for the cytotoxic compound. Co-crystallization attempts in order to understand the binding mode of gold porphyrin to galectin-3 failed, but molecular docking emphasized a highly populated secondary binding site that does not hinder lactose or Thomsen Friendenreich disaccharide binding. This suggests that gold(III) porphyrin might significantly enhance its concentration and delivery to cancer cells by binding to human galectin-3 that keeps its orientation towards tumor associated carbohydrate antigens.
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spelling pubmed-69436292020-01-10 Binding of Gold(III) Porphyrin by the Pro-metastatic Regulatory Protein Human Galectin-3 Bogoeva, Vanya Rangelov, Miroslav Todorova, Nadezhda Lambert, Annie Bridot, Clarisse Yordanova, Anna Roos, Goedele Grandjean, Cyrille Bouckaert, Julie Molecules Article Gold(III) porphyrin presents an attractive alternative to the use of, for example, cisplatin in chemotherapy. However, approaches that allow to selectively target cancer cells are highly sought. Many plant and mammalian lectins have been shown to bind oligosaccharide sequences of the aberrant glycosylation pattern found on cancerous tumors. For example human galectin-3, of the galectin family specific for β-galactoside, is overexpressed in the extracellular matrix of tumorigenous and metastatic tissues. We searched for non-carbohydrate ligands for galectin-3 that can guide a cytotoxic drug to the cancer cells by maintaining its affinity for tumor associated carbohydrate antigens. Previous findings showed that zinc tetrasulfonatophenylporphyrin can bind galectin-3 with sub-micromolar affinity without disturbing lactose binding. Gold(III) porphyrin is not only cytotoxic to cancer cells, it knows also a potential application as photosensitiser in photodynamic therapy. We investigated the binding of gold(III) porphyrin to galectin-3 using different biophysical interaction techniques and demonstrated a low micromolar affinity of human galectin-3 for the cytotoxic compound. Co-crystallization attempts in order to understand the binding mode of gold porphyrin to galectin-3 failed, but molecular docking emphasized a highly populated secondary binding site that does not hinder lactose or Thomsen Friendenreich disaccharide binding. This suggests that gold(III) porphyrin might significantly enhance its concentration and delivery to cancer cells by binding to human galectin-3 that keeps its orientation towards tumor associated carbohydrate antigens. MDPI 2019-12-12 /pmc/articles/PMC6943629/ /pubmed/31842510 http://dx.doi.org/10.3390/molecules24244561 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Bogoeva, Vanya
Rangelov, Miroslav
Todorova, Nadezhda
Lambert, Annie
Bridot, Clarisse
Yordanova, Anna
Roos, Goedele
Grandjean, Cyrille
Bouckaert, Julie
Binding of Gold(III) Porphyrin by the Pro-metastatic Regulatory Protein Human Galectin-3
title Binding of Gold(III) Porphyrin by the Pro-metastatic Regulatory Protein Human Galectin-3
title_full Binding of Gold(III) Porphyrin by the Pro-metastatic Regulatory Protein Human Galectin-3
title_fullStr Binding of Gold(III) Porphyrin by the Pro-metastatic Regulatory Protein Human Galectin-3
title_full_unstemmed Binding of Gold(III) Porphyrin by the Pro-metastatic Regulatory Protein Human Galectin-3
title_short Binding of Gold(III) Porphyrin by the Pro-metastatic Regulatory Protein Human Galectin-3
title_sort binding of gold(iii) porphyrin by the pro-metastatic regulatory protein human galectin-3
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6943629/
https://www.ncbi.nlm.nih.gov/pubmed/31842510
http://dx.doi.org/10.3390/molecules24244561
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