Prolactin Potentiates Transforming Growth Factor α Induction of Mammary Neoplasia in Transgenic Mice

Arendt, Lisa M.; Rose-Hellekant, Teresa A.; Sandgren, Eric P.; Schuler, Linda A.

doi:10.2353/ajpath.2006.050861

Cited by 36 publications

(54 citation statements)

References 57 publications

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“…Recent findings revealing distinctive molecular profiles for ERÀ tumors containing ErbB1 versus ErbB2 (Creighton et al, 2006) may shed light on these differences. Cystic papillary tumors in NRL-TGFa mice resemble those of other TGFa transgenic mice (Humphreys and Hennighausen, 2000;Rose-Hellekant and Sandgren, 2000;Arendt et al, 2006). Concurrent expression of heterozygous p53 results in aggressive solid tumors of varying types reflecting the tumor spectrum of p53 þ /À BALB/c mice (Blackburn et al, 2003;Jerry et al, 2000;Kuperwasser et al, 2000), although relative proportions cannot be determined due to low numbers of p53 þ /À mice in the present study.…”

Section: Discussionmentioning

confidence: 62%

Estrogen receptor-positive mammary tumorigenesis in TGFα transgenic mice progresses with progesterone receptor loss

et al. 2007

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We characterized the novel NRL-transforming growth factor alpha (NRL-TGFa) transgenic mouse model in which growth factor -steroid receptor interactions were explored. The NRL promoter directs transgene expression to mammary ductal and alveolar cells and is nonresponsive to estrogen manipulations in vitro and in vivo. NRL-TGFa mice acquire proliferative hyperplasias as well as cystic and solid tumors. Quantitative transcript analysis revealed a progressive decrease in estrogen receptor alpha (ER) and progesterone receptor (PR) mRNA levels with tumorigenesis. However, ER protein was evident in all lesion types and in surrounding stromal cells using immunohistochemistry. PR protein was identified in normal epithelial cells and in very few cells of small epithelial hyperplasias, but never in stromal or tumor cells. Prophylactic ovariectomy significantly delayed tumor development and decreased incidence. Finally, while heterozygous ( þ /À) p53 mice did not acquire mammary lesions, p53 þ /À mice carrying the NRLTGFa transgene developed ER negative/PR negative undifferentiated carcinomas. These data demonstrate that unregulated TGFa expression in the mammary gland leads to oncogenesis that is dependent on ovarian steroids early in tumorigenesis. Resulting tumors resemble a clinical phenotype of ER þ /PRÀ, and when combined with a heterozygous p53 genotype, ERÀ/PRÀ.

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Section: Discussionmentioning

confidence: 62%

Estrogen receptor-positive mammary tumorigenesis in TGFα transgenic mice progresses with progesterone receptor loss

et al. 2007

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“…16,17 Transgenic virgin female mice that overexpress TGF-␣ under control of the NRL promoter develop mammary tumors and preneoplastic lesions. 18,19 Together, TGF-␣ and PRL potently cooperate; bitransgenic NRL-TGF-␣/PRL females develop mammary tumors similar to those found in NRL-TGF-␣ females with a greatly reduced latency and 100% incidence. 18 This hormone/growth factor interaction is also strongly oncogenic in the male.…”

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“…18,19 Together, TGF-␣ and PRL potently cooperate; bitransgenic NRL-TGF-␣/PRL females develop mammary tumors similar to those found in NRL-TGF-␣ females with a greatly reduced latency and 100% incidence. 18 This hormone/growth factor interaction is also strongly oncogenic in the male. Bitransgenic NRL-TGF-␣/PRL males developed mammary tumors with similar incidence and latency to that found in NRL-TGF-␣/PRL females 18 ; single transgenic males developed no lesions.…”

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confidence: 99%

“…18 This hormone/growth factor interaction is also strongly oncogenic in the male. Bitransgenic NRL-TGF-␣/PRL males developed mammary tumors with similar incidence and latency to that found in NRL-TGF-␣/PRL females 18 ; single transgenic males developed no lesions. Like male breast cancer in humans, the resulting tumors expressed variable levels of both ER-␣ and AR.…”

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confidence: 99%

“…This novel model system offers important insight into PRL, ER-␣, and TGF-␣ interactions in the pathogenesis of this disease in males and suggests therapeutic targets that may enhance survival in male breast cancer. 18,19 were generated as described. All lines were maintained in the FVB/N strain background.…”

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Prolactin Drives Estrogen Receptor-α-Dependent Ductal Expansion and Synergizes with Transforming Growth Factor-α to Induce Mammary Tumors in Males

Arendt

Schuler

2008

The American Journal of Pathology

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Male breast cancer is rare and has been the focus of limited research. Although the etiology is unclear, conditions increasing circulating prolactin (PRL), as well as estrogen, increase the risk of tumorigenesis.We modeled exposure to elevated PRL in transgenic mice, using the mammary-selective, estrogen-insensitive promoter neu-related lipocalin (NRL), to drive PRL expression. Male NRL-PRL mice did not develop mammary tumors. However, in cooperation with the well-characterized oncogene transforming growth factor-␣ (TGF-␣), PRL induced mammary tumors in 100% of male bitransgenic mice. Similar to disease in human males, these tumors expressed variable levels of estrogen receptor-␣ (ER-␣) and androgen receptors. However, carcinogenesis was not responsive to testicular steroids because castration did not alter latency to tumor development or tumor ER-␣ expression. Interestingly, both NRL-TGF-␣/PRL and NRL-PRL males demonstrated increased ductal development, which occurred during puberty, similar to female mice. This outgrowth was diminished in NRL-PRL males treated with ICI 182,780, suggesting that PRL enhances ER-mediated growth. Treatment of MCF-7-derived cells with PRL increased phosphorylation of ER-␣ at residues implicated in unliganded ER-␣ activity. Together, these studies suggest that PRL expands the pool of cells susceptible to tumorigenesis, which is then facilitated by PRL and TGF-␣ cross talk. Activation of ER-␣ is one mechanism by which PRL may contribute to breast cancer and points to other therapeutic strategies for male patients. An estimated 1690 new cases of male breast cancer will be diagnosed in the United States, and 460 men will die as a result of the disease this year. 1 Because it is a rare disease, male breast cancer has been the focus of very limited research. Unlike breast cancer in women, the incidence in men is rising 1.1% annually, and men are more likely to have advanced disease and poorer survival compared to women. 2 Conditions that elevate the ratio of circulating estrogens and androgens and increase the risk for this disease include Klinefelter's syndrome, liver cirrhosis, estrogen therapy for prostate cancer, obesity, and testicular abnormalities. 3,4 Similar to the postmenopausal disease in women, 85 to 91% of male breast cancers are estrogen receptor-␣ (ER-␣)-positive and respond to tamoxifen therapy, although the survival advantage for ER-␣-positive tumors is not as evident in males as females. 5 Androgen receptor (AR) is also expressed in a significant number (39 to 80%) of tumors. 6,7 Hyperprolactinemia is also a significant risk factor. 3,8 At least one-third of a consecutive series of male breast cancer patients had elevated serum levels of prolactin (PRL), which also correlated with the size of the primary tumor. 9 Drug treatments associated with PRL elevation and prolactinomas are also significantly linked to increased breast cancer risk. 10 In a retrospective study, one in three men with breast cancer had detectable PRL receptor in their tumors. 11 To study the effect o...

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Constitutive overexpression of Id‐1 in mammary glands of transgenic mice results in precocious and increased formation of terminal end buds, enhanced alveologenesis, delayed involution

Shin

Jang

Kang

et al. 2011

Journal Cellular Physiology

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Inhibitor of differentiation-1 (Id-1) has been shown to play an essential role in cell proliferation, invasion, migration, and anti-apoptosis. However, the effect of Id-1 in mammary gland development remains unknown. Here, we generated MMTV-Id-1 transgenic mice to study the role of Id-1 in mammary gland development. In virgin mice, Id-1 overexpression led to precocious development and delayed regression of terminal end buds (TEBs) compared with wild-type mice. The number of BrdU-positive cells and the expression of Wnt signaling molecules, β-catenin and cyclin D1, which regulate ductal extension and TEB formation in virgin, were statistically higher in Id-1 transgenic mice than in wild-type mice. Id-1 also had an effect on the formation and proliferation of lobuloalveolar structures during early and mid-pregnancy. Id-1 transgenic mice had more lobulated and prominent alveolar budding than wild-type mice and had significantly greater counts of lobuloalveolar structures in early pregnancy. The expression of BrdU, β-catenin, and cyclin D1 was also predominantly increased in Id-1 transgenic mice. Moreover, Id-1 transgenic mice showed delayed involution. Id-1 regulated the expression levels of anti-apoptotic Bcl-2 and pro-apoptotic Bax, and resulted in delay of apoptotic peak during postlactational involution. We also found that Id-1 was able to modulate expression of the regulators of Wnt/β-catenin signaling such as phospho-Akt, BMP2, FGF3, and RAR-β in tubuloalveolar development of mammary glands. Taken together, our results suggest that Id-1 plays a pivotal role in mammary gland development through Wnt signaling-mediated acceleration of precocity and alveologenesis and Bcl-2 family members-mediated delay of involution.

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Prolactin Potentiates Transforming Growth Factor α Induction of Mammary Neoplasia in Transgenic Mice

Cited by 36 publications

References 57 publications

Estrogen receptor-positive mammary tumorigenesis in TGFα transgenic mice progresses with progesterone receptor loss

Estrogen receptor-positive mammary tumorigenesis in TGFα transgenic mice progresses with progesterone receptor loss

Prolactin Drives Estrogen Receptor-α-Dependent Ductal Expansion and Synergizes with Transforming Growth Factor-α to Induce Mammary Tumors in Males

Constitutive overexpression of Id‐1 in mammary glands of transgenic mice results in precocious and increased formation of terminal end buds, enhanced alveologenesis, delayed involution

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