Biopathological Significance of PIWI–piRNA Pathway Deregulation in Invasive Breast Carcinomas

SIMPLE SUMMARY: The PIWI-piRNA ribonucleoproteic complexes are pivotal regulators of genome integrity, differentiation and homeostasis and their dysregulation has recently been implicated in carcinogenesis. The aim of this study was to analyze the four PIWILs gene expression in invasive breast carci...

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Autores principales: Meseure, Didier, Vacher, Sophie, Boudjemaa, Sabah, Laé, Marick, Nicolas, André, Leclere, Renaud, Chemlali, Walid, Champenois, Gabriel, Schnitzler, Anne, Lesage, Laetitia, Dubois, Thierry, Bieche, Ivan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7600338/
https://www.ncbi.nlm.nih.gov/pubmed/33008024
http://dx.doi.org/10.3390/cancers12102833
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author Meseure, Didier
Vacher, Sophie
Boudjemaa, Sabah
Laé, Marick
Nicolas, André
Leclere, Renaud
Chemlali, Walid
Champenois, Gabriel
Schnitzler, Anne
Lesage, Laetitia
Dubois, Thierry
Bieche, Ivan
author_facet Meseure, Didier
Vacher, Sophie
Boudjemaa, Sabah
Laé, Marick
Nicolas, André
Leclere, Renaud
Chemlali, Walid
Champenois, Gabriel
Schnitzler, Anne
Lesage, Laetitia
Dubois, Thierry
Bieche, Ivan
author_sort Meseure, Didier
collection PubMed
description SIMPLE SUMMARY: The PIWI-piRNA ribonucleoproteic complexes are pivotal regulators of genome integrity, differentiation and homeostasis and their dysregulation has recently been implicated in carcinogenesis. The aim of this study was to analyze the four PIWILs gene expression in invasive breast carcinomas (IBC) at RNA level using quantitative RT-PCR and protein level using immunohistochemistry. In normal breast tissue, PIWILs 2 and 4 were solely expressed, whereas an abnormal emergence of PIWIL1 and 3 was observed in respectively 30% and 6% of IBCs. Conversely, PIWIL2 was underexpressed in 48.3% and PIWIL4 downregulated in 43.3% of IBCs. Similar patterns of PIWIL deregulation were observed in a multitumoral panel, suggesting a generic mechanism in most cancers. PIWIL2 underexpression was significantly associated with DNA methylation and strong cytotoxic immune response. Characterization of the newly recognized PIWIL-piRNA pathway in IBCs opens interesting therapeutic perspectives using piRNAs, hypomethylating drugs, checkpoints immunotherapies and anti-PIWIL 1–3 antibodies. ABSTRACT: The PIWI proteins emerging in the development of human cancers, edify PIWI-piRNA ribonucleoproteic complexes acting as pivotal regulators of genome integrity, differentiation and homeostasis. The aim of this study is to analyze the four PIWILs gene expression in invasive breast carcinomas (IBCs): at RNA level using quantitative RT-PCR (n = 526) and protein level using immunohistochemistry (n = 150). In normal breast tissue, PIWILs 2 and 4 were solely expressed, whereas an abnormal emergence of PIWIL1 and 3 was observed in respectively 30% and 6% of IBCs. Conversely, PIWIL2 was underexpressed in 48.3% and PIWIL4 downregulated in 43.3% of IBCs. Significant positive associations were observed between PIWIL4 underexpression, HR+ status and HR+ ERBB2+ molecular subtype and PIWIL2 underexpression, PR- status, ERBB2- status and molecular subtype. Similar patterns of PIWIL deregulation were observed in a multitumoral panel, suggesting a generic mechanism in most cancers. PIWIL2-4 underexpression was mainly regulated at epigenetic or post-transcriptional levels. PIWIL2 underexpression was significantly associated with DNA methylation and strong cytotoxic immune response. PIWIL2-4 were mainly associated with genes implicated in cell proliferation. As a result of this study, characterization of the PIWIL-piRNA pathway in IBCs opens interesting therapeutic perspectives using piRNAs, hypomethylating drugs, checkpoints immunotherapies and anti-PIWIL 1–3 antibodies.
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spelling pubmed-76003382020-11-01 Biopathological Significance of PIWI–piRNA Pathway Deregulation in Invasive Breast Carcinomas Meseure, Didier Vacher, Sophie Boudjemaa, Sabah Laé, Marick Nicolas, André Leclere, Renaud Chemlali, Walid Champenois, Gabriel Schnitzler, Anne Lesage, Laetitia Dubois, Thierry Bieche, Ivan Cancers (Basel) Article SIMPLE SUMMARY: The PIWI-piRNA ribonucleoproteic complexes are pivotal regulators of genome integrity, differentiation and homeostasis and their dysregulation has recently been implicated in carcinogenesis. The aim of this study was to analyze the four PIWILs gene expression in invasive breast carcinomas (IBC) at RNA level using quantitative RT-PCR and protein level using immunohistochemistry. In normal breast tissue, PIWILs 2 and 4 were solely expressed, whereas an abnormal emergence of PIWIL1 and 3 was observed in respectively 30% and 6% of IBCs. Conversely, PIWIL2 was underexpressed in 48.3% and PIWIL4 downregulated in 43.3% of IBCs. Similar patterns of PIWIL deregulation were observed in a multitumoral panel, suggesting a generic mechanism in most cancers. PIWIL2 underexpression was significantly associated with DNA methylation and strong cytotoxic immune response. Characterization of the newly recognized PIWIL-piRNA pathway in IBCs opens interesting therapeutic perspectives using piRNAs, hypomethylating drugs, checkpoints immunotherapies and anti-PIWIL 1–3 antibodies. ABSTRACT: The PIWI proteins emerging in the development of human cancers, edify PIWI-piRNA ribonucleoproteic complexes acting as pivotal regulators of genome integrity, differentiation and homeostasis. The aim of this study is to analyze the four PIWILs gene expression in invasive breast carcinomas (IBCs): at RNA level using quantitative RT-PCR (n = 526) and protein level using immunohistochemistry (n = 150). In normal breast tissue, PIWILs 2 and 4 were solely expressed, whereas an abnormal emergence of PIWIL1 and 3 was observed in respectively 30% and 6% of IBCs. Conversely, PIWIL2 was underexpressed in 48.3% and PIWIL4 downregulated in 43.3% of IBCs. Significant positive associations were observed between PIWIL4 underexpression, HR+ status and HR+ ERBB2+ molecular subtype and PIWIL2 underexpression, PR- status, ERBB2- status and molecular subtype. Similar patterns of PIWIL deregulation were observed in a multitumoral panel, suggesting a generic mechanism in most cancers. PIWIL2-4 underexpression was mainly regulated at epigenetic or post-transcriptional levels. PIWIL2 underexpression was significantly associated with DNA methylation and strong cytotoxic immune response. PIWIL2-4 were mainly associated with genes implicated in cell proliferation. As a result of this study, characterization of the PIWIL-piRNA pathway in IBCs opens interesting therapeutic perspectives using piRNAs, hypomethylating drugs, checkpoints immunotherapies and anti-PIWIL 1–3 antibodies. MDPI 2020-09-30 /pmc/articles/PMC7600338/ /pubmed/33008024 http://dx.doi.org/10.3390/cancers12102833 Text en © 2020 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
Meseure, Didier
Vacher, Sophie
Boudjemaa, Sabah
Laé, Marick
Nicolas, André
Leclere, Renaud
Chemlali, Walid
Champenois, Gabriel
Schnitzler, Anne
Lesage, Laetitia
Dubois, Thierry
Bieche, Ivan
Biopathological Significance of PIWI–piRNA Pathway Deregulation in Invasive Breast Carcinomas
title Biopathological Significance of PIWI–piRNA Pathway Deregulation in Invasive Breast Carcinomas
title_full Biopathological Significance of PIWI–piRNA Pathway Deregulation in Invasive Breast Carcinomas
title_fullStr Biopathological Significance of PIWI–piRNA Pathway Deregulation in Invasive Breast Carcinomas
title_full_unstemmed Biopathological Significance of PIWI–piRNA Pathway Deregulation in Invasive Breast Carcinomas
title_short Biopathological Significance of PIWI–piRNA Pathway Deregulation in Invasive Breast Carcinomas
title_sort biopathological significance of piwi–pirna pathway deregulation in invasive breast carcinomas
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7600338/
https://www.ncbi.nlm.nih.gov/pubmed/33008024
http://dx.doi.org/10.3390/cancers12102833
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