Membrane-Initiated Estradiol Signaling of Epithelial-Mesenchymal Transition-Associated Mechanisms Through Regulation of Tight Junctions in Human Breast Cancer Cells

Jiménez-Salazar, Javier Esteban; Posadas-Rodríguez, Pedro; Lazzarini‐Lechuga, Roberto; Luna–López, Armando; Zentella‐Dehesa, Alejandro; Gómez-Quiroz, Luís Enrique; Königsberg, Mina; Domínguez-Gómez, Guadalupe; Damián-Matsumura, Pablo

doi:10.1007/s12672-014-0180-3

Cited by 34 publications

(29 citation statements)

References 44 publications

(55 reference statements)

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“…The role of chlamydia-inducible, cytokines such as TNF-alpha and TGF-beta in EMT and fibrosis has been well established [ 86 ]. Thus, the ability of estrogen to induce EMT involving miRNA alterations [ 87 ], and our results showing that chlamydia induced EMT and estrogen receptors, would suggest that chlamydia may induce EMT via the estrogen receptor-signaling pathway. Consistent with the miRNA profiles and up-regulation of pro-EMT proteins, our results further showed that the chlamydial down-regulated proteins are those that maintain epithelial integrity, support reproductive fertility, control fibrosis and act as tumor suppressors.…”

Section: Discussionmentioning

confidence: 88%

Role of Epithelial-Mesenchyme Transition in Chlamydia Pathogenesis

et al. 2015

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Chlamydia trachomatis genital infection in women causes serious adverse reproductive complications, and is a strong co-factor for human papilloma virus (HPV)-associated cervical epithelial carcinoma. We tested the hypothesis that Chlamydia induces epithelial-mesenchyme transition (EMT) involving T cell-derived TNF-alpha signaling, caspase activation, cleavage inactivation of dicer and dysregulation of micro-RNA (miRNA) in the reproductive epithelium; the pathologic process of EMT causes fibrosis and fertility-related epithelial dysfunction, and also provides the co-factor function for HPV-related cervical epithelial carcinoma. Using a combination of microarrays, immunohistochemistry and proteomics, we showed that chlamydia altered the expression of crucial miRNAs that control EMT, fibrosis and tumorigenesis; specifically, miR-15a, miR-29b, miR-382 and MiR-429 that maintain epithelial integrity were down-regulated, while miR-9, mi-R-19a, miR-22 and miR-205 that promote EMT, fibrosis and tumorigenesis were up-regulated. Chlamydia induced EMT in vitro and in vivo, marked by the suppression of normal epithelial cell markers especially E-cadherin but up-regulation of mesenchymal markers of pathological EMT, including T-cadherin, MMP9, and fibronectin. Also, Chlamydia upregulated pro-EMT regulators, including the zinc finger E-box binding homeobox protein, ZEB1, Snail1/2, and thrombospondin1 (Thbs1), but down-regulated anti-EMT and fertility promoting proteins (i.e., the major gap junction protein connexin 43 (Cx43), Mets1, Add1Scarb1 and MARCKSL1). T cell-derived TNF-alpha signaling was required for chlamydial-induced infertility and caspase inhibitors prevented both infertility and EMT. Thus, chlamydial-induced T cell-derived TNF-alpha activated caspases that inactivated dicer, causing alteration in the expression of reproductive epithelial miRNAs and induction of EMT. EMT causes epithelial malfunction, fibrosis, infertility, and the enhancement of tumorigenesis of HPV oncogene-transformed epithelial cells. These findings provide a novel understanding of the molecular pathogenesis of chlamydia-associated diseases, which may guide a rational prevention strategy.

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Section: Discussionmentioning

confidence: 88%

Role of Epithelial-Mesenchyme Transition in Chlamydia Pathogenesis

et al. 2015

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“…Epithelial–mesenchymal transition (EMT), a feature of metastatic cells, has previously been described in the context of tumor budding [ 22 ] and could be consistent with the observed association to both LVI and lymph node positivity but requires further analysis. A recent report also demonstrated that estrogen is involved in EMT in breast cancer cell lines with stem cell properties [ 23 ] and it was shown that estrogen is involved in disruption of tight-junction and increased cell motility [ 24 ]. We suspect that ER-positive tumors with high tumor budding may be undergoing a high degree of EMT and therefore have more metastatic potential.…”

Section: Discussionmentioning

confidence: 99%

High tumor budding stratifies breast cancer with metastatic properties

Salhia

Trippel

Pfaltz

et al. 2015

Breast Cancer Res Treat

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Tumor budding refers to single or small cluster of tumor cells detached from the main tumor mass. In colon cancer high tumor budding is associated with positive lymph nodes and worse prognosis. Therefore, we investigated the value of tumor budding as a predictive feature of lymph node status in breast cancer (BC). Whole tissue sections from 148 surgical resection specimens (SRS) and 99 matched preoperative core biopsies (CB) with invasive BC of no special type were analyzed on one slide stained with pan-cytokeratin. In SRS, the total number of intratumoral (ITB) and peripheral tumor buds (PTB) in ten high-power fields (HPF) were counted. A bud was defined as a single tumor cell or a cluster of up to five tumor cells. High tumor budding equated to scores averaging >4 tumor buds across 10HPFs. In CB high tumor budding was defined as ≥10 buds/HPF. The results were correlated with pathological parameters. In SRS high PTB stratified BC with lymph node metastases (p ≤ 0.03) and lymphatic invasion (p ≤ 0.015). In CB high tumor budding was significantly (p = 0.0063) associated with venous invasion. Pathologists are able, based on morphology, to categorize BC into a high and low risk groups based in part on lymph node status. This risk assessment can be easily performed during routine diagnostics and it is time and cost effective. These results suggest that high PTB is associated with loco-regional metastasis, highlighting the possibility that this tumor feature may help in therapeutic decision-making.

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“…The basis of these observations is not clear. However, it was recently reported that oestrogen is involved in EMT in breast cancer cell lines with stem cell properties ( Sun et al , 2014 ) and that oestrogen is involved in disruption of tight junction and increased cell motility ( Sanchez et al , 2010 ; Jiménez-Salazar et al , 2014 ). Therefore, this may suggest that ER-positive tumours with high tumour budding may be undergoing a higher degree of EMT and as a result more metastatic potential.…”

Section: Discussionmentioning

confidence: 99%

The relationship between tumour budding, the tumour microenvironment and survival in patients with invasive ductal breast cancer

et al. 2015

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Background:Tumour budding has previously been reported to predict survival in several solid organ tumours, including breast; however, whether this is independent of other aspects of the tumour microenvironment is unknown. In the present study, the relationship between tumour budding, the tumour microenvironment and survival was examined in patients with invasive ductal breast cancer.Methods:Patients presenting between 1995 and 1998 were studied (n=474). Using routine pathological sections, tumour budding was measured at the invasive margin and its association with clinicopathological characteristics and cancer-specific survival (CSS) was examined.Results:Tumour budding was associated with several adverse pathological characteristics, including lymph node involvement, lymph vessel invasion (LVI), increased tumour stroma percentage (TSP) and weaker local inflammatory infiltrative. Tumour budding was associated with reduced CSS (hazard ratio (HR) 2.08, 95% confidence interval (CI) 1.14–3.09, P=0.004), independent of nodal status, molecular subtypes, tumour necrosis, CD8+, CD138+, LVI, blood vessel invasion and TSP. Further, tumour budding was independently associated with reduced CSS in node-negative patients (HR 2.63, 95% CI 1.16–5.92, P=0.020) and those who have low TSP (HR 1.98, 95% CI 1.09–3.57, P=0.024) and high-grade local inflammatory infiltrative (HR 2.27, 95% CI 1.35–5.36, P=0.014).Conclusions:Tumour budding was a significant predictor of survival in patients with invasive ductal breast cancer, independent of adverse pathological characteristics and components of tumour microenvironment. The present study further confirms the clinical utility of both tumour and host-based factors of tumour microenvironment.

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Membrane-Initiated Estradiol Signaling of Epithelial-Mesenchymal Transition-Associated Mechanisms Through Regulation of Tight Junctions in Human Breast Cancer Cells

Cited by 34 publications

References 44 publications

Role of Epithelial-Mesenchyme Transition in Chlamydia Pathogenesis

Role of Epithelial-Mesenchyme Transition in Chlamydia Pathogenesis

High tumor budding stratifies breast cancer with metastatic properties

The relationship between tumour budding, the tumour microenvironment and survival in patients with invasive ductal breast cancer

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