Insight into the mechanism of ferroptosis inhibition by ferrostatin-1

Ferroptosis is a form of cell death primed by iron and lipid hydroperoxides and prevented by GPx4. Ferrostatin-1 (fer-1) inhibits ferroptosis much more efficiently than phenolic antioxidants. Previous studies on the antioxidant efficiency of fer-1 adopted kinetic tests where a diazo compound generat...

Descripción completa

Detalles Bibliográficos
Autores principales: Miotto, Giovanni, Rossetto, Monica, Di Paolo, Maria Luisa, Orian, Laura, Venerando, Rina, Roveri, Antonella, Vučković, Ana-Marija, Bosello Travain, Valentina, Zaccarin, Mattia, Zennaro, Lucio, Maiorino, Matilde, Toppo, Stefano, Ursini, Fulvio, Cozza, Giorgio
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2019
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6812032/
https://www.ncbi.nlm.nih.gov/pubmed/31574461
http://dx.doi.org/10.1016/j.redox.2019.101328
_version_ 1783462589401923584
author Miotto, Giovanni
Rossetto, Monica
Di Paolo, Maria Luisa
Orian, Laura
Venerando, Rina
Roveri, Antonella
Vučković, Ana-Marija
Bosello Travain, Valentina
Zaccarin, Mattia
Zennaro, Lucio
Maiorino, Matilde
Toppo, Stefano
Ursini, Fulvio
Cozza, Giorgio
author_facet Miotto, Giovanni
Rossetto, Monica
Di Paolo, Maria Luisa
Orian, Laura
Venerando, Rina
Roveri, Antonella
Vučković, Ana-Marija
Bosello Travain, Valentina
Zaccarin, Mattia
Zennaro, Lucio
Maiorino, Matilde
Toppo, Stefano
Ursini, Fulvio
Cozza, Giorgio
author_sort Miotto, Giovanni
collection PubMed
description Ferroptosis is a form of cell death primed by iron and lipid hydroperoxides and prevented by GPx4. Ferrostatin-1 (fer-1) inhibits ferroptosis much more efficiently than phenolic antioxidants. Previous studies on the antioxidant efficiency of fer-1 adopted kinetic tests where a diazo compound generates the hydroperoxyl radical scavenged by the antioxidant. However, this reaction, accounting for a chain breaking effect, is only minimally useful for the description of the inhibition of ferrous iron and lipid hydroperoxide dependent peroxidation. Scavenging lipid hydroperoxyl radicals, indeed, generates lipid hydroperoxides from which ferrous iron initiates a new peroxidative chain reaction. We show that when fer-1 inhibits peroxidation, initiated by iron and traces of lipid hydroperoxides in liposomes, the pattern of oxidized species produced from traces of pre-existing hydroperoxides is practically identical to that observed following exhaustive peroxidation in the absence of the antioxidant. This supported the notion that the anti-ferroptotic activity of fer-1 is actually due to the scavenging of initiating alkoxyl radicals produced, together with other rearrangement products, by ferrous iron from lipid hydroperoxides. Notably, fer-1 is not consumed while inhibiting iron dependent lipid peroxidation. The emerging concept is that it is ferrous iron itself that reduces fer-1 radical. This was supported by electroanalytical evidence that fer-1 forms a complex with iron and further confirmed in cells by fluorescence of calcein, indicating a decrease of labile iron in the presence of fer-1. The notion of such as pseudo-catalytic cycle of the ferrostatin-iron complex was also investigated by means of quantum mechanics calculations, which confirmed the reduction of an alkoxyl radical model by fer-1 and the reduction of fer-1 radical by ferrous iron. In summary, GPx4 and fer-1 in the presence of ferrous iron, produces, by distinct mechanism, the most relevant anti-ferroptotic effect, i.e the disappearance of initiating lipid hydroperoxides.
format Online
Article
Text
id pubmed-6812032
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Elsevier
record_format MEDLINE/PubMed
spelling pubmed-68120322019-10-30 Insight into the mechanism of ferroptosis inhibition by ferrostatin-1 Miotto, Giovanni Rossetto, Monica Di Paolo, Maria Luisa Orian, Laura Venerando, Rina Roveri, Antonella Vučković, Ana-Marija Bosello Travain, Valentina Zaccarin, Mattia Zennaro, Lucio Maiorino, Matilde Toppo, Stefano Ursini, Fulvio Cozza, Giorgio Redox Biol Research Paper Ferroptosis is a form of cell death primed by iron and lipid hydroperoxides and prevented by GPx4. Ferrostatin-1 (fer-1) inhibits ferroptosis much more efficiently than phenolic antioxidants. Previous studies on the antioxidant efficiency of fer-1 adopted kinetic tests where a diazo compound generates the hydroperoxyl radical scavenged by the antioxidant. However, this reaction, accounting for a chain breaking effect, is only minimally useful for the description of the inhibition of ferrous iron and lipid hydroperoxide dependent peroxidation. Scavenging lipid hydroperoxyl radicals, indeed, generates lipid hydroperoxides from which ferrous iron initiates a new peroxidative chain reaction. We show that when fer-1 inhibits peroxidation, initiated by iron and traces of lipid hydroperoxides in liposomes, the pattern of oxidized species produced from traces of pre-existing hydroperoxides is practically identical to that observed following exhaustive peroxidation in the absence of the antioxidant. This supported the notion that the anti-ferroptotic activity of fer-1 is actually due to the scavenging of initiating alkoxyl radicals produced, together with other rearrangement products, by ferrous iron from lipid hydroperoxides. Notably, fer-1 is not consumed while inhibiting iron dependent lipid peroxidation. The emerging concept is that it is ferrous iron itself that reduces fer-1 radical. This was supported by electroanalytical evidence that fer-1 forms a complex with iron and further confirmed in cells by fluorescence of calcein, indicating a decrease of labile iron in the presence of fer-1. The notion of such as pseudo-catalytic cycle of the ferrostatin-iron complex was also investigated by means of quantum mechanics calculations, which confirmed the reduction of an alkoxyl radical model by fer-1 and the reduction of fer-1 radical by ferrous iron. In summary, GPx4 and fer-1 in the presence of ferrous iron, produces, by distinct mechanism, the most relevant anti-ferroptotic effect, i.e the disappearance of initiating lipid hydroperoxides. Elsevier 2019-09-20 /pmc/articles/PMC6812032/ /pubmed/31574461 http://dx.doi.org/10.1016/j.redox.2019.101328 Text en © 2019 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Paper
Miotto, Giovanni
Rossetto, Monica
Di Paolo, Maria Luisa
Orian, Laura
Venerando, Rina
Roveri, Antonella
Vučković, Ana-Marija
Bosello Travain, Valentina
Zaccarin, Mattia
Zennaro, Lucio
Maiorino, Matilde
Toppo, Stefano
Ursini, Fulvio
Cozza, Giorgio
Insight into the mechanism of ferroptosis inhibition by ferrostatin-1
title Insight into the mechanism of ferroptosis inhibition by ferrostatin-1
title_full Insight into the mechanism of ferroptosis inhibition by ferrostatin-1
title_fullStr Insight into the mechanism of ferroptosis inhibition by ferrostatin-1
title_full_unstemmed Insight into the mechanism of ferroptosis inhibition by ferrostatin-1
title_short Insight into the mechanism of ferroptosis inhibition by ferrostatin-1
title_sort insight into the mechanism of ferroptosis inhibition by ferrostatin-1
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6812032/
https://www.ncbi.nlm.nih.gov/pubmed/31574461
http://dx.doi.org/10.1016/j.redox.2019.101328
work_keys_str_mv AT miottogiovanni insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT rossettomonica insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT dipaolomarialuisa insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT orianlaura insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT venerandorina insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT roveriantonella insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT vuckovicanamarija insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT bosellotravainvalentina insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT zaccarinmattia insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT zennarolucio insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT maiorinomatilde insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT toppostefano insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT ursinifulvio insightintothemechanismofferroptosisinhibitionbyferrostatin1
AT cozzagiorgio insightintothemechanismofferroptosisinhibitionbyferrostatin1

Ejemplares similares