Loss of periostin/OSF-2 in ErbB2/Neu-driven tumors results in androgen receptor-positive molecular apocrine-like tumors with reduced Notch1 activity

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• 作者：Roshan Sriram (1) <br> Vivian Lo (1) <br> Benjamin Pryce (1) <br> Lilia Antonova (1) <br> Alan J Mears (3) <br> Manijeh Daneshmand (2) <br> Bruce McKay (4) <br> Simon J Conway (5) <br> William J Muller (6) <br> Luc A Sabourin (1) (2) <br><br>1. Department of Cellular and Molecular Medicine ; Faculty of Medicine ; University of Ottawa ; 451 Smyth Road ; Ottawa ; ON ; K1H 8M5 ; Canada <br> 3. Children鈥檚 Hospital of Eastern Ontario ; Research Institute ; 501 Smyth Road ; Ottawa ; ON ; K1H8L6 ; Canada <br> 2. Ottawa Hospital Research Institute ; Cancer Therapeutics ; 501 Smyth Road ; Ottawa ; ON ; K1H 8L6 ; Canada <br> 4. Department of Biology and Institute of Biochemistry ; Carleton University ; 1125 Colonel By Drive ; Ottawa ; ON ; K1S 5B6 ; Canada <br> 5. Developmental Biology and Neonatal Medicine Program ; HB Wells Center for Pediatric Research ; Indiana University School of Medicine ; 705 Riley Hospital Drive ; Indianapolis ; IN ; 46202 ; USA <br> 6. Department of Biochemistry and Goodman Cancer Research Center ; McGill University ; 1200 Pine Avenue West ; Montreal ; QC ; H3G 1A1 ; Canada <br>
• 刊名：Breast Cancer Research
• 出版年：2015
• 出版时间：December 2015
• 年：2015
• 卷：17
• 期：1
• 全文大小：2,073 KB
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• 刊物主题：Cancer Research; Oncology;
• 出版者：BioMed Central
• ISSN：1465-5411

文摘

Introduction Periostin (Postn) is a secreted cell adhesion protein that activates signaling pathways to promote cancer cell survival, angiogenesis, invasion, and metastasis. Interestingly, Postn is frequently overexpressed in numerous human cancers, including breast, lung, colon, pancreatic, and ovarian cancer. Methods Using transgenic mice expressing the Neu oncogene in the mammary epithelium crossed into Postn-deficient animals, we have assessed the effect of Postn gene deletion on Neu-driven mammary tumorigenesis. Results Although Postn is exclusively expressed in the stromal fibroblasts of the mammary gland, Postn deletion does not affect mammary gland outgrowth during development or pregnancy. Furthermore, we find that loss of Postn in the mammary epithelium does not alter breast tumor initiation or growth in mouse mammary tumor virus (MMTV)-Neu expressing mice but results in an apocrine-like tumor phenotype. Surprisingly, we find that tumors derived from Postn-null animals express low levels of Notch protein and Hey1 mRNA but increased expression of androgen receptor (AR) and AR target genes. We show that tumor cells derived from wild-type animals do not proliferate when transplanted in a Postn-null environment but that this growth defect is rescued by the overexpression of active Notch or the AR target gene prolactin-induced protein (PIP/GCDFP-15). Conclusions Together our data suggest that loss of Postn in an ErbB2/Neu/HER2 overexpression model results in apocrine-like tumors that activate an AR-dependent pathway. This may have important implications for the treatment of breast cancers involving the therapeutic targeting of periostin or Notch signaling.