Parity-induced mammary epithelial cells facilitate tumorigenesis in MMTV-neu transgenic mice

Henry, Ma Linda D.; Triplett, Aleata A.; Oh, Keon Bong; Smith, Gilbert H.; Wagner, Kay Uwe

doi:10.1038/sj.onc.1207827

Cited by 118 publications

(121 citation statements)

References 18 publications

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“…Using the mouse model of HER2 breast cancer, mouse mammary tumor virus (MMTV)-driven ErbB2 (homolog of human HER2/ neu), 53 PI-MECs were shown to be cellular targets of HER2-mediated oncogenesis. [54][55][56] Indeed, ErbB2 tumorigenesis in mice increases with parity, and targeted removal of PI-MECs in vivo reduced tumor incidence in ErbB2 mice. [55][56][57] Likewise, clinical studies demonstrate that women during or right after pregnancy (when the number of PI-MECs is highest) have increased susceptibility for HER2 breast cancer.…”

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confidence: 99%

“…[54][55][56] Indeed, ErbB2 tumorigenesis in mice increases with parity, and targeted removal of PI-MECs in vivo reduced tumor incidence in ErbB2 mice. [55][56][57] Likewise, clinical studies demonstrate that women during or right after pregnancy (when the number of PI-MECs is highest) have increased susceptibility for HER2 breast cancer. 58,59 Thus, we hypothesized that p63 hemizygosity would suppress ErbB2-mediated tumorigenesis as a consequence of a reduced PI-MEC pool.…”

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p63 is a prosurvival factor in the adult mammary gland during post-lactational involution, affecting PI-MECs and ErbB2 tumorigenesis

et al. 2014

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In embryogenesis, p63 is essential to develop mammary glands. In the adult mammary gland, p63 is highly expressed in the basal cell layer that comprises myoepithelial and interspersed stem/progenitor cells, and has limited expression in luminal epithelial cells. In adult skin, p63 has a crucial role in the maintenance of epithelial stem cells. However, it is unclear whether p63 also has an equivalent role as a stem/progenitor cell factor in adult mammary epithelium. We show that p63 is essential in vivo for the survival and maintenance of parity-identified mammary epithelial cells (PI-MECs), a pregnancy-induced heterogeneous population that survives post-lactational involution and contain multipotent progenitors that give rise to alveoli and ducts in subsequent pregnancies. p63 þ / À glands are normal in virgin, pregnant and lactating states. Importantly, however, during the apoptotic phase of post-lactational involution p63 þ / À glands show a threefold increase in epithelial cell death, concomitant with increased activation of the oncostatin M/Stat3 and p53 pro-apoptotic pathways, which are responsible for this phase. Thus, p63 is a physiologic antagonist of these pathways specifically in this regressive stage. After the restructuring phase when involution is complete, mammary glands of p63 þ / À mice again exhibit normal epithelial architecture by conventional histology. However, using Rosa LSL-LacZ ;WAP-Cre transgenics (LSL-LacZ, lox-stop-lox b-galactosidase), a genetic in vivo labeling system for PI-MECs, we find that p63 þ / À glands have a 30% reduction in the number of PI-MEC progenitors and their derivatives. Importantly, PI-MECs are also cellular targets of pregnancy-promoted ErbB2 tumorigenesis. Consistent with their PI-MEC pool reduction, one-time pregnant p63 þ / À ErbB2 mice are partially protected from breast tumorigenesis, exhibiting extended tumor-free and overall survival, and reduced tumor multiplicity compared with their p63 þ / þ ErbB2 littermates. Conversely, in virgin ErbB2 mice p63 heterozygosity provides no survival advantage. In sum, our data establish that p63 is an important survival factor for pregnancy-identified PI-MEC progenitors in breast tissue in vivo.

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p63 is a prosurvival factor in the adult mammary gland during post-lactational involution, affecting PI-MECs and ErbB2 tumorigenesis

et al. 2014

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“…Transgenic mice expressing the wild type Her2/neu (ErbB2) oncogene under transcriptional regulation of the MMTV-LTR seem to be suitable for studying the involvement of PI-MEC in pregnancy-associated mammary tumorigenesis since this animal model exhibits a relatively long latency of tumorigenesis (T50 of 205 days). Using this animal model, we demonstrated that: a) multiparous females consistently exhibited accelerated tumorigenesis compared to their nulliparous littermate controls in a mixed genetic background and b) PI-MEC were, indeed, primary targets of neoplastic transformation in this model [19]. The de novo generation and amplification of a large number of hormone-responsive and apoptosisresistant epithelial cells (i.e.…”

Section: Pi-mec and Mammary Tumorigenesismentioning

confidence: 92%

Stem Cells, Hormones, and Mammary Cancer

Smith¹

2008

Hormonal Carcinogenesis V

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Pregnancy and breast cancerThe incidence of breast cancer is influenced by age, genetics, ethnicity, diet, socioeconomic status, and reproductive history. The latter is the strongest and most reliable risk factor besides age and genetic susceptibility [1]. Reproductive factors have been associated with risk for breast cancer since the 17 th century, when the disease was noted to be more prevalent among Catholic nuns. It is now a well-established fact that a full-term pregnancy early in life is associated with a long-term risk reduction for developing breast cancer. A woman who has her first child after the age of 35 has approximately twice the risk of developing breast cancer as a woman who has a child before age 20 (see current NCI Cancer Fact Sheet on Pregnancy and Breast Cancer Risk). Despite this long-term reduction in breast cancer risk in parous women, epidemiologists agreed at a recent NCI-sponsored workshop on "Early Reproductive Events and Breast Cancer" (http://nci.nih.gov/cancerinfo/ere) that each gestation increases temporarily the likelihood for developing breast cancer [2]. This transient increase in breast cancer risk lasts for a few years after a full-term pregnancy.Pregnancy has a very similar dual effect on the etiology of mammary cancer in animal models. Like humans, parous rats and mice have a greatly reduced susceptibility to chemically induced mammary tumorigenesis compared to their nulliparous siblings [3]. Humans who carry germ line mutations in tumor susceptibility genes do not benefit from the protective effects of pregnancy, but have a significantly greater risk of developing the disease following one or multiple gestation cycles [4]. There are, however, conflicting reports whether lactation influences the onset of breast cancer in women with BRCA1 mutations. The current view on breast cancer as a stem cell disease is founded on compelling evidence that many breast cancers may arise as clonal expansions from epithelial progenitors with an infinite lifespan [5]. It has been hypothesized that unique properties of mammary stem cells, such as self-renewal, make this population a prime target for transformation and tumorigenesis. Several experimental breast cancer models support this hypothesis. The most venerable is the mammary tumor virus [6] model in mice, where MMTV proviral insertions produce mutated mammary cells, which attain immortality (escape from growth senescence) and produce clones of mammary cells with increased propensity to develop mammary cancer. Serial transplantations of these preneoplastic lesions result in the formation of hyperplastic/dysplastic ductal trees, suggesting that multipotent cells are affected by MMTV transformation and that they pass on their neoplastic properties to their descendants [7]. Morphologically undifferentiated cells,

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“…Studies at the molecular level using different platforms for global genome analysis have confirmed the universality of this phenomenon in various strains of rats and mice [13][14][15][16][17][18][19][20][21]. Studies in experimental animal models have been useful for uncovering the sequential genomic changes occurring in the mammary gland in response to multiple hormonal stimuli of pregnancy that lead to the imprinting of a permanent genomic signature.…”

Section: Introductionmentioning

confidence: 99%

“…In these models, the initiation of cancer is prevented by the differentiation of the mammary gland induced by pregnancy [11,12]. The molecular changes involved in this phenomenon are just starting to be unraveled [13][14][15][16][17][18]. The protection conferred by pregnancy is age-specific since a delay in childbearing after age 24 progressively increases the risk of cancer development.…”

Section: Introductionmentioning

confidence: 99%

The Genomic Signature of Breast Cancer Prevention

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Abstract:The breast of parous postmenopausal women exhibits a specific signature that has been induced by a full term pregnancy. This signature is centered in chromatin remodeling and the epigenetic changes induced by methylation of specific genes which are important regulatory pathways induced by pregnancy. Through the analysis of the genes found to be differentially methylated between women of varying parity, multiple positions at which beta-catenin production and use is inhibited were recognized. The biological importance of the pathways identified in this specific population cannot be sufficiently emphasized because they could represent a safeguard mechanism mediating the protection of the breast conferred by full term pregnancy.

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Parity-induced mammary epithelial cells facilitate tumorigenesis in MMTV-neu transgenic mice

Cited by 118 publications

References 18 publications

p63 is a prosurvival factor in the adult mammary gland during post-lactational involution, affecting PI-MECs and ErbB2 tumorigenesis

p63 is a prosurvival factor in the adult mammary gland during post-lactational involution, affecting PI-MECs and ErbB2 tumorigenesis

Stem Cells, Hormones, and Mammary Cancer

The Genomic Signature of Breast Cancer Prevention

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