Embryonic Morphogen Nodal Promotes Breast Cancer Growth and Progression

Daniela F Quail,Dylan Z Dieters-Castator,Lynne-Marie Postovit,David M Putman,Guihua Zhang,Scott D Findlay,Logan A Walsh,David A Hess,Gabrielle M Siegers,Heather Broughton,Katriina Aalto-Setala

doi:10.1371/journal.pone.0048237

Daniela F Quail, Dylan Z Dieters-Castator + Show 9 more

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https://doi.org/10.1371/journal.pone.0048237

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Abstract

Breast cancers expressing human embryonic stem cell (hESC)-associated genes are more likely to progress than well-differentiated cancers and are thus associated with poor patient prognosis. Elevated proliferation and evasion of growth control are similarly associated with disease progression, and are classical hallmarks of cancer. In the current study we demonstrate that the hESC-associated factor Nodal promotes breast cancer growth. Specifically, we show that Nodal is elevated in aggressive MDA-MB-231, MDA-MB-468 and Hs578t human breast cancer cell lines, compared to poorly aggressive MCF-7 and T47D breast cancer cell lines. Nodal knockdown in aggressive breast cancer cells via shRNA reduces tumour incidence and significantly blunts tumour growth at primary sites. In vitro, using Trypan Blue exclusion assays, Western blot analysis of phosphorylated histone H3 and cleaved caspase-9, and real time RT-PCR analysis of BAX and BCL2 gene expression, we demonstrate that Nodal promotes expansion of breast cancer cells, likely via a combinatorial mechanism involving increased proliferation and decreased apopotosis. In an experimental model of metastasis using beta-glucuronidase (GUSB)-deficient NOD/SCID/mucopolysaccharidosis type VII (MPSVII) mice, we show that although Nodal is not required for the formation of small (<100 cells) micrometastases at secondary sites, it supports an elevated proliferation:apoptosis ratio (Ki67:TUNEL) in micrometastatic lesions. Indeed, at longer time points (8 weeks), we determined that Nodal is necessary for the subsequent development of macrometastatic lesions. Our findings demonstrate that Nodal supports tumour growth at primary and secondary sites by increasing the ratio of proliferation:apoptosis in breast cancer cells. As Nodal expression is relatively limited to embryonic systems and cancer, this study establishes Nodal as a potential tumour-specific target for the treatment of breast cancer.

Highlights

Two classical and fundamental hallmarks of cancer include enhanced proliferation and evasion of apoptotic signals [1,2]
Through Western blot analyses, we determined that Nodal protein is elevated in cell lysates and in conditioned media from poorly-differentiated Hs578t, MDA-MB-231 and MDA-MB-468 breast cancer cell lines compared to well-differentiated MCF-7 and T47D cell lines (Fig. 1A,B)
This is consistent with previous reports that show high Nodal expression in aggressive melanoma, prostate, and breast cancer cell lines compared to poorly aggressive lines [7,9,11,18]

Summary

Introduction

Two classical and fundamental hallmarks of cancer include enhanced proliferation and evasion of apoptotic signals [1,2]. In addition to enhanced proliferation and evasion of apoptosis during cancer progression, aberrant expression of stem cell factors within breast tumours sustains aggressive phenotypes, and is associated with growth-promoting profiles in tumour cells and their microenvironments. Nodal, Cripto, ALK4, and SMAD4 are upregulated during lactational expansion of alveolar epithelial tissue, and downregulated during involution (marked by widespread apoptosis) in BalbC mice [16,17]. Together, these studies suggest that Nodal may play a role in promoting proliferative phenotypes in dynamic epithelial cell types

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