Lovastatin reduces PEL cell survival by phosphorylating ERK1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21

Statins are inhibitors of the mevalonate pathway that besides being cholesterol lowering agents, display anti‐cancer properties. This is because cholesterol is an essential component of cell membranes but also because the mevalonate pathway controls protein farnesylation and geranylation, processes...

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Autores principales: Santarelli, Roberta, Pompili, Chiara, Gilardini Montani, Maria Saveria, Romeo, Maria Anele, Gonnella, Roberta, D'Orazi, Gabriella, Cirone, Mara
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley & Sons, Inc. 2021
Materias:
Research Communications
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8361952/
https://www.ncbi.nlm.nih.gov/pubmed/33987937
http://dx.doi.org/10.1002/iub.2503
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author Santarelli, Roberta
Pompili, Chiara
Gilardini Montani, Maria Saveria
Romeo, Maria Anele
Gonnella, Roberta
D'Orazi, Gabriella
Cirone, Mara
author_facet Santarelli, Roberta
Pompili, Chiara
Gilardini Montani, Maria Saveria
Romeo, Maria Anele
Gonnella, Roberta
D'Orazi, Gabriella
Cirone, Mara
author_sort Santarelli, Roberta
collection PubMed
description Statins are inhibitors of the mevalonate pathway that besides being cholesterol lowering agents, display anti‐cancer properties. This is because cholesterol is an essential component of cell membranes but also because the mevalonate pathway controls protein farnesylation and geranylation, processes essential for the activity of GTPase family proteins. In this study, we found that Lovastatin exerted a dose‐ and time‐dependent cytotoxic effect against PEL cells, an aggressive B cell lymphoma strictly associated with the gammaherpesvirus KSHV and characterized by a poor response to conventional chemotherapies. At molecular level, Lovastatin by dephosphorylating STAT3, induced ERK1/2 activation that inhibited autophagy and phosphorylated p53ser15 that in turn maintained ERK1/2 activated and up‐regulated p21. However, p21 played a pro‐survival role in this setting, as its inhibition by UC2288 further reduced cell survival in PEL cells undergoing Lovastatin treatment. In conclusion, this study suggests that Lovastatin may represent a valid therapeutic alternative against PEL cells, especially if used in combination with p21 inhibitors.
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spelling pubmed-83619522021-08-17 Lovastatin reduces PEL cell survival by phosphorylating ERK1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21 Santarelli, Roberta Pompili, Chiara Gilardini Montani, Maria Saveria Romeo, Maria Anele Gonnella, Roberta D'Orazi, Gabriella Cirone, Mara IUBMB Life Research Communications Statins are inhibitors of the mevalonate pathway that besides being cholesterol lowering agents, display anti‐cancer properties. This is because cholesterol is an essential component of cell membranes but also because the mevalonate pathway controls protein farnesylation and geranylation, processes essential for the activity of GTPase family proteins. In this study, we found that Lovastatin exerted a dose‐ and time‐dependent cytotoxic effect against PEL cells, an aggressive B cell lymphoma strictly associated with the gammaherpesvirus KSHV and characterized by a poor response to conventional chemotherapies. At molecular level, Lovastatin by dephosphorylating STAT3, induced ERK1/2 activation that inhibited autophagy and phosphorylated p53ser15 that in turn maintained ERK1/2 activated and up‐regulated p21. However, p21 played a pro‐survival role in this setting, as its inhibition by UC2288 further reduced cell survival in PEL cells undergoing Lovastatin treatment. In conclusion, this study suggests that Lovastatin may represent a valid therapeutic alternative against PEL cells, especially if used in combination with p21 inhibitors. John Wiley & Sons, Inc. 2021-05-21 2021-07 /pmc/articles/PMC8361952/ /pubmed/33987937 http://dx.doi.org/10.1002/iub.2503 Text en © 2021 The Authors. IUBMB Life published by Wiley Periodicals LLC on behalf of International Union of Biochemistry and Molecular Biology. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Communications
Santarelli, Roberta
Pompili, Chiara
Gilardini Montani, Maria Saveria
Romeo, Maria Anele
Gonnella, Roberta
D'Orazi, Gabriella
Cirone, Mara
Lovastatin reduces PEL cell survival by phosphorylating ERK1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21
title Lovastatin reduces PEL cell survival by phosphorylating ERK1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21
title_full Lovastatin reduces PEL cell survival by phosphorylating ERK1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21
title_fullStr Lovastatin reduces PEL cell survival by phosphorylating ERK1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21
title_full_unstemmed Lovastatin reduces PEL cell survival by phosphorylating ERK1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21
title_short Lovastatin reduces PEL cell survival by phosphorylating ERK1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21
title_sort lovastatin reduces pel cell survival by phosphorylating erk1/2 that blocks the autophagic flux and engages a cross‐talk with p53 to activate p21
topic Research Communications
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8361952/
https://www.ncbi.nlm.nih.gov/pubmed/33987937
http://dx.doi.org/10.1002/iub.2503
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