Upregulation of the Oct3/4 Network in Basal Breast Cancer Is Associated with Its Metastatic Potential and Shows Tissue Dependent Variability

Author:

Rajan Robin G.1,Krutilina Raisa I.2ORCID,Ignatova Tatyana N.12,Pavicevich Zoran S.2,Dulatova Galina M.2,Lane Maria A.2,Chatterjee Arindam R.23ORCID,Rooney Robert J.4,Antony Mymoon5,Hagerty Vivian R.6,Kukekov Nickolay V.2,Hanafy Khalid A.6,Vrionis Frank D.16

Affiliation:

1. Helene and Stephen Weicholz Cell Therapy Laboratory, Marcus Neuroscience Institute, 800 Meadows Road, Boca Raton, FL 33486, USA

2. Department of Pathology and Laboratory Medicine, Center for Cancer Research, University of Tennessee Health Sciences Center, 920 Madison Ave., Memphis, TN 38163, USA

3. Mallinckrodt Institute of Radiology, Departments of Neurosurgery and Neurology, Washington University School of Medicine, 660 S. Euclid Ave., St. Louis, MO 63110, USA

4. Le-Bonheur Children’s Outpatient Hospital, 51 N Dunlap St., Memphis, TN 38105, USA

5. Wellington Regional Medical Center, 10101 Forest Hill Blvd, Wellington, FL 33414, USA

6. Department of Biomedical Science, Schmidt College of Medicine, Florida Atlantic University, 777 Glades Road, Boca Raton, FL 33431, USA

Abstract

Adaptive plasticity of Breast Cancer stem cells (BCSCs) is strongly correlated with cancer progression and resistance, leading to a poor prognosis. In this study, we report the expression profile of several pioneer transcription factors of the Oct3/4 network associated with tumor initiation and metastasis. In the triple negative breast cancer cell line (MDA-MB-231) stably transfected with human Oct3/4-GFP, differentially expressed genes (DEGs) were identified using qPCR and microarray, and the resistance to paclitaxel was assessed using an MTS assay. The tumor-seeding potential in immunocompromised (NOD-SCID) mice and DEGs in the tumors were also assessed along with the intra-tumor (CD44+/CD24-) expression using flow cytometry. Unlike 2-D cultures, the Oct3/4-GFP expression was homogenous and stable in 3-D mammospheres developed from BCSCs. A total of 25 DEGs including Gata6, FoxA2, Sall4, Zic2, H2afJ, Stc1 and Bmi1 were identified in Oct3/4 activated cells coupled with a significantly increased resistance to paclitaxel. In mice, the higher Oct3/4 expression in tumors correlated with enhanced tumorigenic potential and aggressive growth, with metastatic lesions showing a >5-fold upregulation of DEGs compared to orthotopic tumors and variability in different tissues with the highest modulation in the brain. Serially re-implanting tumors in mice as a model of recurrence and metastasis highlighted the sustained upregulation of Sall4, c-Myc, Mmp1, Mmp9 and Dkk1 genes in metastatic lesions with a 2-fold higher expression of stem cell markers (CD44+/CD24-). Thus, Oct3/4 transcriptome may drive the differentiation and maintenance of BCSCs, promoting their tumorigenic potential, metastasis and resistance to drugs such as paclitaxel with tissue-specific heterogeneity.

Funder

Department of Neurosurgery, University of Tennessee Health Science Center

Methodist Le-Bonheur Healthcare Foundation

Helene and Stephen Weicholz Foundation Grant

Publisher

MDPI AG

Subject

Inorganic Chemistry,Organic Chemistry,Physical and Theoretical Chemistry,Computer Science Applications,Spectroscopy,Molecular Biology,General Medicine,Catalysis

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