Progesterone Inhibits Endometrial Cancer Invasiveness by Inhibiting the TGFβ Pathway

Bokhari, Amber A.; Lee, Laura R.; Raboteau, Dewayne; Hamilton, Chad A.; Maxwell, G. Larry; Rodriguez, Gustavo C.; Syed, Viqar

doi:10.1158/1940-6207.capr-14-0054

Cited by 39 publications

(43 citation statements)

References 48 publications

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“…Previously we have shown enhanced proliferation and invasive potential of endometrial cells in response to TGF-β1 [38]. Here we substantiated the direct interaction between Nestin and TGF-β in Nestin overexpressing cells by demonstrating a marked increase in Nestin expression which was associated with enhanced proliferation and invasive potential in response to TGF-β1 exposure.…”

Section: Discussionsupporting

confidence: 85%

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Nestin suppression attenuates invasive potential of endometrial cancer cells by downregulating TGF-β signaling pathway

et al. 2016

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Nestin, an intermediate filament protein and a stem cell marker is expressed in several tumors. Until recently, little was known about the expression levels and the role of Nestin in endometrial cancer. Compared to the immortalized endometrial epithelial cell line EM-E6/E7-TERT, endometrial cancer cell lines express high to moderate levels of Nestin. Furthermore, endometrial tumors and tumor cell lines have a cancer stem-like cell subpopulation expressing CD133. Among the cancer lines, AN3CA and KLE cells exhibited both a significantly higher number of CD133+ cells and expressed Nestin at higher levels than Ishikawa cells. Knockdown of Nestin in AN3CA and KLE increased cells in G0/G1 phase of the cell cycle, whereas overexpression in Ishikawa decreased cells in G0/G1 phase and increased cells in S-phase. Nestin knockdown cells showed increased p21, p27, and PNCA levels and decreased expression of cyclin-D1 and D3. In contrast, Nestin overexpression revealed an inverse expression pattern of cell cycle regulatory proteins. Nestin knockdown inhibited cancer cell growth and invasive potential by downregulating TGF-β signaling components, MMP-2, MMP-9, vimentin, SNAIL, SLUG, Twist, N-cadherin, and upregulating the epithelial cell marker E-cadherin whereas the opposite was observed with Nestin overexpressing Ishikawa cells. Nestin knockdown also inhibited, while overexpression promoted invadopodia formation and pFAK expression. Knockdown of Nestin significantly reduced tumor volume in vivo. Finally, progesterone inhibited Nestin expression in endometrial cancer cells. These results suggest that Nestin can be a therapeutic target for cancer treatment.

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Section: Discussionsupporting

confidence: 85%

“…We and others have previously shown that TGF-β signaling pathway is activated in endometrial cancer cells [22, 23, 38]. Our findings suggest that elevated levels of Nestin in endometrial cancer cells can stimulate cell proliferation and invasion by stimulating TGF-β signaling pathway.…”

Section: Discussionsupporting

confidence: 66%

Nestin suppression attenuates invasive potential of endometrial cancer cells by downregulating TGF-β signaling pathway

et al. 2016

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“…We previously reported that progesterone-mediated upregulation of vitamin D receptor (VDR) levels increases calcitriol-induced growth inhibition in endometrial cancer cells [9, 10]. Here, we expand upon our previous work by examining the effects of calcitriol and progesterone, both alone and in combination, on CYP24A1.…”

Section: Introductionmentioning

confidence: 84%

“…Combining a low dose of progesterone with a low dose of calcitriol, a vitamin D metabolite, might be more effective for treating endometrial cancer than higher doses of either agent alone. In vitro and in vivo studies from our laboratory and others have shown that progesterone and other chemopreventive agents enhance the antitumor effects of calcitriol [7–10]. …”

Section: Introductionmentioning

confidence: 99%

Progesterone potentiates the growth inhibitory effects of calcitriol in endometrial cancer via suppression of CYP24A1

et al. 2016

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Here, we evaluated the expression of CYP24A1, a protein that inactivates vitamin D in tissues. CYP24A1 expression was increased in advanced-stage endometrial tumors compared to normal tissues. Similarly, endometrial cancer cells expressed higher levels of CYP24A1 than immortalized endometrial epithelial cells. RT-PCR and Western blotting were used to examine CYP24A1 mRNA and protein levels in endometrial cancer cells after 8, 24, 72, and 120 h of exposure to progesterone, progestin derivatives and calcitriol, either alone or in combination. Progestins inhibited calcitriol-induced expression of CYP24A1 and splice variant CYP24SV mRNA and protein in cancer cells. Furthermore, actinomycin D, but not cycloheximide, blocked calcitriol-induced CYP24A1 splicing. siRNA-induced knockdown of CYP24A1 expression sensitized endometrial cancer cells to calcitriol-induced growth inhibition. These data suggest that CYP24A1 overexpression reduces the antitumor effects of calcitriol in cancer cells and that progestins may be beneficial for maintaining calcitriol's anti-endometrial cancer activity.

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“…Recently, progesterone was shown to inhibit basal and TGFB1 induced cancer cell viability and invasion, which was accompanied by increased E-cadherin and decreased vimentin expression (Bokhari et al 2014). Chaudhry et al (2014) observed that TGFB upregulates the expression of prostate apoptosis response-4, a tumor suppressor protein, with simultaneous induction of EMT in endometrial and cervical cancer cells.…”

Section: Cell Signaling Pathwaysmentioning

confidence: 99%

Tumor progression, metastasis, and modulators of epithelial–mesenchymal transition in endometrioid endometrial carcinoma: an update

Makker

Goel

2015

Endocrine-Related Cancer

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Endometrioid endometrial carcinoma (EEC), also known as type 1 endometrial cancer (EC), accounts for over 70-80% of all cases that are usually associated with estrogen stimulation and often develops in a background of atypical endometrial hyperplasia. The increased incidence of EC is mainly confined to this type of cancer. Most EEC patients present at an early stage and generally have a favorable prognosis; however, up to 30% of EEC present as high risk tumors, which have invaded deep into the myometrium at diagnosis and progressively lead to local or extra pelvic metastasis. The poor survival of advanced EC is related to the lack of effective therapies, which can be attributed to poor understanding of the molecular mechanisms underlying the progression of disease toward invasion and metastasis. Multiple lines of evidence illustrate that epithelial-mesenchymal transition (EMT)-like events are central to tumor progression and malignant transformation, endowing the incipient cancer cell with invasive and metastatic properties. The aim of this review is to summarize the current knowledge on molecular events associated with EMT in progression, invasion, and metastasis of EEC. Further, the role of epigenetic modifications and microRNA regulation, tumor microenvironment, and microcystic elongated and fragmented glands like invasion pattern have been discussed. We believe this article may perhaps stimulate further research in this field that may aid in identifying high risk patients within this clinically challenging patient group and also lead to the recognition of novel targets for the prevention of metastasis -the most fatal consequence of endometrial carcinogenesis.

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Progesterone Inhibits Endometrial Cancer Invasiveness by Inhibiting the TGFβ Pathway

Cited by 39 publications

References 48 publications

Nestin suppression attenuates invasive potential of endometrial cancer cells by downregulating TGF-β signaling pathway

Nestin suppression attenuates invasive potential of endometrial cancer cells by downregulating TGF-β signaling pathway

Progesterone potentiates the growth inhibitory effects of calcitriol in endometrial cancer via suppression of CYP24A1

Tumor progression, metastasis, and modulators of epithelial–mesenchymal transition in endometrioid endometrial carcinoma: an update

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