αB-Crystallin is a novel oncoprotein that predicts poor clinical outcome in breast cancer
Jose V. Moyano, … , Charles M. Perou, Vincent L. Cryns
Jose V. Moyano, … , Charles M. Perou, Vincent L. Cryns
Published January 4, 2006
Citation Information: J Clin Invest. 2006;116(1):261-270. https://doi.org/10.1172/JCI25888.
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Research Article Oncology

αB-Crystallin is a novel oncoprotein that predicts poor clinical outcome in breast cancer

Abstract

Recent gene profiling studies have identified a new breast cancer subtype, the basal-like group, which expresses genes characteristic of basal epithelial cells and is associated with poor clinical outcomes. However, the genes responsible for the aggressive behavior observed in this group are largely unknown. Here we report that the small heat shock protein α-basic–crystallin (αB-crystallin) was commonly expressed in basal-like tumors and predicted poor survival in breast cancer patients independently of other prognostic markers. We also demonstrate that overexpression of αB-crystallin transformed immortalized human mammary epithelial cells (MECs). In 3D basement membrane culture, αB-crystallin overexpression induced luminal filling and other neoplastic-like changes in mammary acini, while silencing αB-crystallin by RNA interference inhibited these abnormalities. αB-Crystallin overexpression also induced EGF- and anchorage-independent growth, increased cell migration and invasion, and constitutively activated the MAPK kinase/ERK (MEK/ERK) pathway. Moreover, the transformed phenotype conferred by αB-crystallin was suppressed by MEK inhibitors. In addition, immortalized human MECs overexpressing αB-crystallin formed invasive mammary carcinomas in nude mice that recapitulated aspects of human basal-like breast tumors. Collectively, our results indicate that αB-crystallin is a novel oncoprotein expressed in basal-like breast carcinomas that independently predicts shorter survival. Our data also implicate the MEK/ERK pathway as a potential therapeutic target for these tumors.

Authors

Jose V. Moyano, Joseph R. Evans, Feng Chen, Meiling Lu, Michael E. Werner, Fruma Yehiely, Leslie K. Diaz, Dmitry Turbin, Gamze Karaca, Elizabeth Wiley, Torsten O. Nielsen, Charles M. Perou, Vincent L. Cryns

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Figure 5

MCF-10A cells overexpressing αB-crystallin form invasive mammary carcinomas in nude mice.

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MCF-10A cells overexpressing αB-crystallin form invasive mammary carcino...
(A) Left: Mean tumor volume ± SEM at weekly intervals in female athymic nude mice inoculated with MCF-10A pools. Right: Volume of tumors in each group at week 10; horizontal line indicates the median tumor volume in each group. Ratios at top indicate the number of tumors per total inoculation sites. **P < 0.01 versus αB-3XSE. (B) H&E staining of representative mammary tumors at 5 (upper panels) and 10 weeks (lower panels) from nude mice inoculated with MCF-10A–αB-WT cells. Upper left panel: Prominent elongated spindle cells and atypical epithelial components with tumor invasion of muscle and fat. Upper middle panel: Mesenchymal spindle cells. Upper right panel: Atypical epithelial components. At 10 weeks, we observed epithelioid cells with pleomorphic high grade nuclei and mitoses (thin arrow) that form glandular like structures (thick arrow, lower left panel) and high nuclear grade spindle cells (lower right panel). (C) Representative IHC of the mammary carcinomas shown in B. Original magnification, ×100 (B, upper left panel), ×200 (B, remaining panels, and C).