Estrogen promotes the survival and pulmonary metastasis of tuberin-null cells

Yu, Jane; Robb, Victoria A.; Morrison, Tasha; Ariazi, Eric A.; Karbowniczek, Magdalena; Astrinidis, Aristotelis; Wang, Chunrong; Hernandez-Cuebas, Lisa; Seeholzer, Laura F.; Nicolas, Émmanuelle; Hensley, Harvey H.; Jordan, V. Craig; Walker, Cheryl L.; Henske, Elizabeth P.

doi:10.1073/pnas.0810790106

Cited by 150 publications

(209 citation statements)

References 37 publications

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“…E 2 , upon binding to its estrogen receptor (ER), has been reported to regulate transcriptiondependent and -independent signaling events (14). Thus, in addition to its ability to promote changes in gene expression (10,(15)(16)(17)(18), E 2 can induce the activation of signaling proteins such as Src, Akt, and ERK-MAP kinase (14). The importance of ERK-MAP kinase in LAM was suggested by a recent report showing that E 2 promoted the MEK-dependent invasion of cells derived from Eker rat uterine leiomyoma (ELT3 cells) into the lungs of ovariectomized mice (18).…”

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confidence: 99%

“…Thus, in addition to its ability to promote changes in gene expression (10,(15)(16)(17)(18), E 2 can induce the activation of signaling proteins such as Src, Akt, and ERK-MAP kinase (14). The importance of ERK-MAP kinase in LAM was suggested by a recent report showing that E 2 promoted the MEK-dependent invasion of cells derived from Eker rat uterine leiomyoma (ELT3 cells) into the lungs of ovariectomized mice (18). However, the molecular basis for E 2 -dependent ERK contribution to the enhanced invasive phenotype in the presence of constitutively activated mTORC1 was not defined, and whether E 2 promoted a similar response in patient-derived cells remained to be determined.…”

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confidence: 99%

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Integration of mTOR and estrogen–ERK2 signaling in lymphangioleiomyomatosis pathogenesis

Ilter

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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Lymphangioleiomyomatosis (LAM) is a destructive lung disease of women associated with the metastasis of tuberin-null cells with hyperactive mammalian target of rapamycin complex 1 (mTORC1) activity. Clinical trials with the mTORC1 inhibitor rapamycin have revealed partial efficacy but are not curative. Pregnancy appears to exacerbate LAM, suggesting that estrogen (E 2 ) may play a role in the unique features of LAM. Using a LAM patient-derived cell line (bearing biallelic Tuberin inactivation), we demonstrate that E 2 stimulates a robust and biphasic activation of ERK2 and transcription of the late response-gene Fra1 associated with epithelialto-mesenchymal transition. In a carefully orchestrated collaboration, activated mTORC1/S6K1 signaling enhances the efficiency of Fra1 translation of Fra1 mRNA transcribed by the E 2 -ERK2 pathway, through the phosphorylation of the S6K1-dependent eukaryotic translation initiation factor 4B. Our results indicate that targeting the E 2 -ERK pathway in combination with the mTORC1 pathway may be an effective combination therapy for LAM.estrogen signaling | mTORC1 signaling | ERK signaling | EMT

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Integration of mTOR and estrogen–ERK2 signaling in lymphangioleiomyomatosis pathogenesis

Ilter

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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“…[136][137][138][139] Separate studies suggested that prolactin stimulates mTOR, and modifies STAT1 activity in mTOR-dependent fashion. 140,141 Further studies are required to better understand how mTORCs interact with androgen or estrogen signaling pathways.…”

Section: Other Emerging Mtor Targets In Lammentioning

confidence: 99%

mTOR Signaling in Lymphangioleiomyomatosis

Kristof

2010

Lymphatic Research and Biology

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The protein mammalian target of rapamycin (mTOR) plays a central role in cell growth and proliferation. Excessive mTOR activity is a prominent feature of many neoplasms and hamartoma syndromes, including lymphangioleiomyomatosis (LAM), a destructive lung disease that causes progressive respiratory failure in women. Although pharmacological inhibitors of mTOR should directly target the pathogenesis of these disorders, their clinical efficacy has been suboptimal. Recent scientific findings reviewed here have greatly improved our understanding of mTOR signaling mechanisms, provided new insights into the control of cell growth and proliferation, and facilitated the development of new therapeutic approaches in LAM, as well as other neoplastic disorders that exhibit excessive mTOR activity.

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“…Estrogen also enhances the number of circulating tumor cells and the survival of intravenously injected ELT3 -cells. 38 In vitro, estrogen-treated ELT3 cells exhibit induced resistance to anoikis and decreased levels of caspase-3 cleavage. Using the Xenogen bioluminescent imaging (Caliper Life Sciences, Hopkinton, MA), estrogen treatment causes a twofold increase in lung colonization of intravenously injected ELT3-luciferase cells at 3 h, and a five-fold increase at 24 h (Fig.…”

Section: Estrogen Promotes the Survival And Metastasis Of Tsc2-null Cmentioning

confidence: 99%

mTOR Activation, Lymphangiogenesis, and Estrogen-Mediated Cell Survival: The “Perfect Storm” of Pro-Metastatic Factors in LAM Pathogenesis

Henske

2010

Lymphatic Research and Biology

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Research interest in lymphangioleiomyomatosis (LAM) has grown dramatically in the past decade, particularly among cancer biologists. There are at least two reasons for this: first, the discovery in the year 2000 that LAM cells carry TSC2 gene mutations, linking LAM with cellular pathways including the PI3K=Akt=mTOR axis, and allowing the Tuberous Sclerosis Complex (TSC)-regulated pathways that are believed to underlie LAM pathogenesis to be studied in cells, yeast, Drosophila, and mice. A second reason for the rising interest in LAM is the discovery that LAM cells can travel to the lung, including repopulating a donor lung after lung transplantation, despite the fact that LAM cells are histologically benign. This ''benign metastasis'' underpinning suggests that elucidating LAM pathogenesis will unlock a set of fundamental mechanisms that underlie metastatic potential in the context of a cell that has not yet undergone malignant transformation. Here, we will outline the data supporting the metastatic model of LAM, consider the biochemical and cellular mechanisms that may enable LAM cells to metastasize, including both cell autonomous and non-cell autonomous factors, and highlight a mouse model in which estrogen promotes the metastasis and survival of TSC2-deficient cells in a MEKdependent manner. We propose a multistep model of LAM cell metastasis that highlights multiple opportunities for therapeutic intervention. Taken together, the metastatic behavior of LAM cells and the involvement of tumorrelated signaling pathways lead to optimism that cancer-related paradigms for diagnosis, staging, and therapy will lead to therapeutic breakthroughs for women living with LAM.

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Estrogen promotes the survival and pulmonary metastasis of tuberin-null cells

Cited by 150 publications

References 37 publications

Integration of mTOR and estrogen–ERK2 signaling in lymphangioleiomyomatosis pathogenesis

Integration of mTOR and estrogen–ERK2 signaling in lymphangioleiomyomatosis pathogenesis

mTOR Signaling in Lymphangioleiomyomatosis

mTOR Activation, Lymphangiogenesis, and Estrogen-Mediated Cell Survival: The “Perfect Storm” of Pro-Metastatic Factors in LAM Pathogenesis

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