Rb deletion in mouse mammary progenitors induces luminal-B or basal-like/EMT tumor subtypes depending on p53 status
Zhe Jiang, … , Charles M. Perou, Eldad Zacksenhaus
Zhe Jiang, … , Charles M. Perou, Eldad Zacksenhaus
Published August 2, 2010
Citation Information: J Clin Invest. 2010;120(9):3296-3309. https://doi.org/10.1172/JCI41490.
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Research Article Oncology

Rb deletion in mouse mammary progenitors induces luminal-B or basal-like/EMT tumor subtypes depending on p53 status

Abstract

Breast cancer is a highly heterogeneous disease, with several different subtypes being characterized by distinct histology, gene expression patterns, and genetic alterations. The tumor suppressor gene retinoblastoma 1 (RB1) is frequently lost in both luminal-B and triple-negative tumor (TNT; i.e., estrogen receptor–, progesterone receptor–, and human epidermal growth factor receptor 2–negative) breast cancer subtypes. However, a causal role for RB1 loss in different subtypes remains undefined. Here we report that deletion of Rb alone or together with its relative p107 in mouse mammary stem/bipotent progenitor cells induced focal acinar hyperplasia with squamous metaplasia. These lesions progressed into histologically diverse, transplantable mammary tumors with features of either luminal-B or TNT subtypes. The TNTs included basal-like tumors as well as tumors that exhibited epithelial-to-mesenchymal transition (EMT). The EMT-type tumors and a subset of the basal-like tumors, but not luminal-B–like tumors, expressed mutant forms of the tumor suppressor p53. Accordingly, targeted deletion of both Rb and p53 in stem/bipotent progenitors led to histologically uniform, aggressive, EMT-type tumors. Reintroduction of Rb into these tumor cells suppressed growth in vitro and tumor formation in vivo. These results establish a causal role for Rb loss in breast cancer in mice and demonstrate that cooperating oncogenic events, such as mutations in p53, dictate tumor subtype after Rb inactivation.

Authors

Zhe Jiang, Tao Deng, Robert Jones, Huiqin Li, Jason I. Herschkowitz, Jeff C. Liu, Victor J. Weigman, Ming-Sound Tsao, Timothy F. Lane, Charles M. Perou, Eldad Zacksenhaus

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Figure 3

Differential effects of MMTV-Cre and WAP-Cre on Rb deletion and stem/bipotent cell compartments.

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Differential effects of MMTV-Cre and WAP-Cre on Rb deletion and stem/bip...
(A) Whole-mount X-gal staining of a lactating WAP-Cre:ROSA26 gland. (B) X-gal staining of developing endbuds and ducts during ductal morphogenesis (left, cross section; center, transverse section), and lobuloalveoli during lactation (right, whole-mount) in MMTV-CreNLST:ROSA26 mice. (C) CD24-CD49f FACS profile of multiparous Lin normal mammary epithelium and gating used for cell sorting, and immunofluorescent staining for SMA, CK14, and CK18 on the indicated cell populations. DP, CD24+CD49f+ double positive. (D) Schematic representation of floxed Rb exon 19 and primers used to detect WT Rb, Rbfl, and recombined RbΔfl alleles. (E) PCR analysis of DNA extracted from pooled, sorted Lin mammary epithelium from multiparous WAP-Cre:Rbfl/fl:p107–/– (n = 5) or MMTV-Cre:Rbfl/fl:p107–/– (n = 4) mice. Cells were gated as in C. Blot at bottom right shows overexposure after loading twice as much DNA, revealing low-level recombination in CD24+ cells. (F) Densitometry analysis of RbΔfl and Rbfl PCR fragments from E. DN, double negative. (G) Percentage of LinCD24+CD49f+ cells in multiparous WAP-Cre:Rbfl/fl:p107–/– (n = 5) and MMTV-Cre:Rbfl/fl:p107–/– (n = 5) mice relative to control. *P = 0.034, 1-tailed paired Student’s t test. Original magnification, ×63 (A); ×100 (B, left); ×400 (B, center, and C); ×50 (B, right).