The Selectivity for Tumor Cells of Nuclear-Directed Cytotoxic RNases Is Mediated by the Nuclear/Cytoplasmic Distribution of p27(KIP1)

Although single targeted anti-cancer drugs are envisaged as safer treatments because they do not affect normal cells, cancer is a very complex disease to be eradicated with a single targeted drug. Alternatively, multi-targeted drugs may be more effective and the tumor cells may be less prone to deve...

Descripción completa

Detalles Bibliográficos
Autores principales: García-Galindo, Glòria, Castro, Jessica, Matés, Jesús, Bravo, Marlon, Ribó, Marc, Vilanova, Maria, Benito, Antoni
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7957890/
https://www.ncbi.nlm.nih.gov/pubmed/33801209
http://dx.doi.org/10.3390/molecules26051319
_version_ 1783664751249719296
author García-Galindo, Glòria
Castro, Jessica
Matés, Jesús
Bravo, Marlon
Ribó, Marc
Vilanova, Maria
Benito, Antoni
author_facet García-Galindo, Glòria
Castro, Jessica
Matés, Jesús
Bravo, Marlon
Ribó, Marc
Vilanova, Maria
Benito, Antoni
author_sort García-Galindo, Glòria
collection PubMed
description Although single targeted anti-cancer drugs are envisaged as safer treatments because they do not affect normal cells, cancer is a very complex disease to be eradicated with a single targeted drug. Alternatively, multi-targeted drugs may be more effective and the tumor cells may be less prone to develop drug resistance although these drugs may be less specific for cancer cells. We have previously developed a new strategy to endow human pancreatic ribonuclease with antitumor action by introducing in its sequence a non-classical nuclear localization signal. These engineered proteins cleave multiple species of nuclear RNA promoting apoptosis of tumor cells. Interestingly, these enzymes, on ovarian cancer cells, affect the expression of multiple genes implicated in metabolic and signaling pathways that are critic for the development of cancer. Since most of these targeted pathways are not highly relevant for non-proliferating cells, we envisioned the possibility that nuclear directed-ribonucleases were specific for tumor cells. Here, we show that these enzymes are much more cytotoxic for tumor cells in vitro. Although the mechanism of selectivity of NLSPE5 is not fully understood, herein we show that p27(KIP1) displays an important role on the higher resistance of non-tumor cells to these ribonucleases.
format Online
Article
Text
id pubmed-7957890
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-79578902021-03-16 The Selectivity for Tumor Cells of Nuclear-Directed Cytotoxic RNases Is Mediated by the Nuclear/Cytoplasmic Distribution of p27(KIP1) García-Galindo, Glòria Castro, Jessica Matés, Jesús Bravo, Marlon Ribó, Marc Vilanova, Maria Benito, Antoni Molecules Article Although single targeted anti-cancer drugs are envisaged as safer treatments because they do not affect normal cells, cancer is a very complex disease to be eradicated with a single targeted drug. Alternatively, multi-targeted drugs may be more effective and the tumor cells may be less prone to develop drug resistance although these drugs may be less specific for cancer cells. We have previously developed a new strategy to endow human pancreatic ribonuclease with antitumor action by introducing in its sequence a non-classical nuclear localization signal. These engineered proteins cleave multiple species of nuclear RNA promoting apoptosis of tumor cells. Interestingly, these enzymes, on ovarian cancer cells, affect the expression of multiple genes implicated in metabolic and signaling pathways that are critic for the development of cancer. Since most of these targeted pathways are not highly relevant for non-proliferating cells, we envisioned the possibility that nuclear directed-ribonucleases were specific for tumor cells. Here, we show that these enzymes are much more cytotoxic for tumor cells in vitro. Although the mechanism of selectivity of NLSPE5 is not fully understood, herein we show that p27(KIP1) displays an important role on the higher resistance of non-tumor cells to these ribonucleases. MDPI 2021-03-02 /pmc/articles/PMC7957890/ /pubmed/33801209 http://dx.doi.org/10.3390/molecules26051319 Text en © 2021 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
García-Galindo, Glòria
Castro, Jessica
Matés, Jesús
Bravo, Marlon
Ribó, Marc
Vilanova, Maria
Benito, Antoni
The Selectivity for Tumor Cells of Nuclear-Directed Cytotoxic RNases Is Mediated by the Nuclear/Cytoplasmic Distribution of p27(KIP1)
title The Selectivity for Tumor Cells of Nuclear-Directed Cytotoxic RNases Is Mediated by the Nuclear/Cytoplasmic Distribution of p27(KIP1)
title_full The Selectivity for Tumor Cells of Nuclear-Directed Cytotoxic RNases Is Mediated by the Nuclear/Cytoplasmic Distribution of p27(KIP1)
title_fullStr The Selectivity for Tumor Cells of Nuclear-Directed Cytotoxic RNases Is Mediated by the Nuclear/Cytoplasmic Distribution of p27(KIP1)
title_full_unstemmed The Selectivity for Tumor Cells of Nuclear-Directed Cytotoxic RNases Is Mediated by the Nuclear/Cytoplasmic Distribution of p27(KIP1)
title_short The Selectivity for Tumor Cells of Nuclear-Directed Cytotoxic RNases Is Mediated by the Nuclear/Cytoplasmic Distribution of p27(KIP1)
title_sort selectivity for tumor cells of nuclear-directed cytotoxic rnases is mediated by the nuclear/cytoplasmic distribution of p27(kip1)
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7957890/
https://www.ncbi.nlm.nih.gov/pubmed/33801209
http://dx.doi.org/10.3390/molecules26051319
work_keys_str_mv AT garciagalindogloria theselectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT castrojessica theselectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT matesjesus theselectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT bravomarlon theselectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT ribomarc theselectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT vilanovamaria theselectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT benitoantoni theselectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT garciagalindogloria selectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT castrojessica selectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT matesjesus selectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT bravomarlon selectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT ribomarc selectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT vilanovamaria selectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1
AT benitoantoni selectivityfortumorcellsofnucleardirectedcytotoxicrnasesismediatedbythenuclearcytoplasmicdistributionofp27kip1

Ejemplares similares