Abstract

Early detection and targeted treatments have led to a significant decrease in mortality linked to breast cancer (BC), however, important issues need to be addressed in the future. One of them will be to find new triple negative breast cancer (TNBC) therapeutic strategies, since none are currently efficiently targeting this subtype of BC. Since numerous studies have reported the possibility of targeting the autophagy pathway to treat or limit cancer progression, we analyzed the expression of six autophagy genes (ATG9A, ATG9B, BECLIN1, LC3B, NIX and P62/SQSTM1) in breast cancer tissue, and compared their expression with healthy adjacent tissue. In our study, we observed an increase in ATG9A mRNA expression in TNBC samples from our breast cancer cohort. We also showed that this increase of the transcript was confirmed at the protein level on paraffin-embedded tissues. To corroborate these in vivo data, we designed shRNA- and CRISPR/Cas9-driven inhibition of ATG9A expression in the triple negative breast cancer cell line MDA-MB-436, in order to determine its role in the regulation of cancer phenotypes. We found that ATG9A inhibition led to an inhibition of in vitro cancer features, suggesting that ATG9A can be considered as a new marker of TNBC and might be considered in the future as a target to develop new specific TNBC therapies.

Details

Title
ATG9A Is Overexpressed in Triple Negative Breast Cancer and Its In Vitro Extinction Leads to the Inhibition of Pro-Cancer Phenotypes
Author
Claude-Taupin, Aurore 1 ; Fonderflick, Leïla 1 ; Gauthier, Thierry 1 ; Mansi, Laura 1 ; Jean-René Pallandre 1 ; Borg, Christophe 1 ; Perez, Valérie 1 ; Monnien, Franck 2 ; Marie-Paule Algros 2 ; Vigneron, Marc 3 ; Adami, Pascale 1 ; Delage-Mourroux, Régis 1 ; Peixoto, Paul 4 ; Herfs, Michael 5 ; Boyer-Guittaut, Michaël 6 ; Hervouet, Eric 7   VIAFID ORCID Logo 

 INSERM, EFS BFC, UMR1098, Interactions Hôte-Greffon-Tumeur/Ingénierie Cellulaire et Génique, University Bourgogne Franche-Comté F-25000 Besançon, France 
 Department of Pathology, University Hospital of Besançon, F-25000 Besançon, France 
 Team Replisome Dynamics and Cancer. UMR7242 Biotechnologie et Signalisation Cellulaire, CNRS-University Strasbourg, F-67412 Illkirch, France; Ecole Supérieure de Biotechnologie de Strasbourg, University Strasbourg, CNRS, UMR 7242, F-67412 Illkirch, France 
 INSERM, EFS BFC, UMR1098, Interactions Hôte-Greffon-Tumeur/Ingénierie Cellulaire et Génique, University Bourgogne Franche-Comté F-25000 Besançon, France; EPIGENEXP platform, University of Bourgogne Franche-Comté, F-25000 Besançon, France 
 Boratory of Experimental Pathology, GIGA-Cancer, University of Liege, B-4000 Liege, Belgium 
 INSERM, EFS BFC, UMR1098, Interactions Hôte-Greffon-Tumeur/Ingénierie Cellulaire et Génique, University Bourgogne Franche-Comté F-25000 Besançon, France; DimaCell platform, Univ. Bourgogne Franche-Comté, F-25000 Besançon, France 
 INSERM, EFS BFC, UMR1098, Interactions Hôte-Greffon-Tumeur/Ingénierie Cellulaire et Génique, University Bourgogne Franche-Comté F-25000 Besançon, France; Ecole Supérieure de Biotechnologie de Strasbourg, University Strasbourg, CNRS, UMR 7242, F-67412 Illkirch, France; DimaCell platform, Univ. Bourgogne Franche-Comté, F-25000 Besançon, France 
First page
248
Publication year
2018
Publication date
2018
Publisher
MDPI AG
e-ISSN
20734409
Source type
Scholarly Journal
Language of publication
English
DOI
https://doi.org/10.3390/cells7120248
ProQuest document ID
2582798130
Copyright
© 2018 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/). Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.