Epithelial-Mesenchymal Transition Markers in Breast Cancer and Pathological Responseafter Neoadjuvant Chemotherapy

Elzamly, Shaimaa; Badri, Nabeel; Padilla, Osvaldo; Dwivedi, Alok; Alvarado, Luis; Hamilton, Matthew J.; Diab, Nabih; Rock, Crosby D.; Elfar, Ahmed; Teleb, Marwa; Sánchez, Luis A.; Nahleh, Zeina

doi:10.1177/1178223418788074

Cited by 28 publications

(25 citation statements)

References 45 publications

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“…The EMT process is a prerequisite for metastatic spread of the tumor from the primary site (breast) to distant organs (i.e., lymph nodes, bone, brain, lung, or liver). Data suggest that positive regulation of SLUG by Jagged1-mediated activation of Notch IC results in the repression of E-cadherin, thus allowing for EMT in breast cancer cells [ 50 , 51 , 52 ]. Jagged1 overexpression alone is associated with increased bone metastasis, and disruption of the Notch pathway by using the γ-secretase inhibitor (GSI) MRK-003 reversed Jagged-1-mediated bone metastasis in mice [ 53 , 54 ].…”

Section: A Role For Notch In Breast Cancermentioning

confidence: 99%

Notch Signaling in Breast Cancer: A Role in Drug Resistance

BeLow

Osipo

2020

Cells

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Breast cancer is a heterogeneous disease that can be subdivided into unique molecular subtypes based on protein expression of the Estrogen Receptor, Progesterone Receptor, and/or the Human Epidermal Growth Factor Receptor 2. Therapeutic approaches are designed to inhibit these overexpressed receptors either by endocrine therapy, targeted therapies, or combinations with cytotoxic chemotherapy. However, a significant percentage of breast cancers are inherently resistant or acquire resistance to therapies, and mechanisms that promote resistance remain poorly understood. Notch signaling is an evolutionarily conserved signaling pathway that regulates cell fate, including survival and self-renewal of stem cells, proliferation, or differentiation. Deregulation of Notch signaling promotes resistance to targeted or cytotoxic therapies by enriching of a small population of resistant cells, referred to as breast cancer stem cells, within the bulk tumor; enhancing stem-like features during the process of de-differentiation of tumor cells; or promoting epithelial to mesenchymal transition. Preclinical studies have shown that targeting the Notch pathway can prevent or reverse resistance through reduction or elimination of breast cancer stem cells. However, Notch inhibitors have yet to be clinically approved for the treatment of breast cancer, mainly due to dose-limiting gastrointestinal toxicity. In this review, we discuss potential mechanisms of Notch-mediated resistance in breast cancer cells and breast cancer stem cells, and various methods of targeting Notch through γ-secretase inhibitors, Notch signaling biologics, or transcriptional inhibitors. We also discuss future plans for identification of novel Notch-targeted therapies, in order to reduce toxicity and improve outcomes for women with resistant breast cancer.

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Section: A Role For Notch In Breast Cancermentioning

confidence: 99%

Notch Signaling in Breast Cancer: A Role in Drug Resistance

BeLow

Osipo

2020

Cells

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“…In BC patients, elevated Jagged1 expression and hyperactive Notch signaling has been shown to be predictive of poor prognosis. One study suggests that Jagged1-mediated Notch activation triggers the process of EMT via the repression of E-cadherin by Slug [26,27]. The NICD positively regulates Slug expression by stimulating Slug promoter activation.…”

Section: Notch-mediated Emt In Breast Cancermentioning

confidence: 99%

A “NOTCH” Deeper into the Epithelial-To-Mesenchymal Transition (EMT) Program in Breast Cancer

Kar

Jha

et al. 2019

Genes

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Notch signaling is a primitive signaling pathway having various roles in the normal origin and development of each multicellular organisms. Therefore, any aberration in the pathway will inevitably lead to deadly outcomes such as cancer. It has now been more than two decades since Notch was acknowledged as an oncogene in mouse mammary tumor virus-infected mice. Since that discovery, activated Notch signaling and consequent up-regulation of tumor-promoting Notch target genes have been observed in human breast cancer. Moreover, consistent over-expression of Notch ligands and receptors has been shown to correlate with poor prognosis in human breast cancer. Notch regulates a number of key processes during breast carcinogenesis, of which, one key phenomenon is epithelial–mesenchymal transition (EMT). EMT is a key process for large-scale cell movement during morphogenesis at the time of embryonic development. Cancer cells aided by transcription factors usurp this developmental program to execute the multi-step process of tumorigenesis and metastasis. In this review, we recapitulate recent progress in breast cancer research that has provided new perceptions into the molecular mechanisms behind Notch-mediated EMT regulation during breast tumorigenesis.

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“…Another protein implicated in the pro-tumorigenic effects of p62 is Vimentin, a protein involved in tumor progression. Vimentin is a Type III intermediate filament that regulates cell shape, motility, and adhesion during EMT, processes implicated in cell invasion and aggressiveness in cancer cells ( 93 , 94 ). In the highly metastatic MDA-MB-231 breast cancer cell line, vimentin co-immunoprepicitates with endogenous p62.…”

Section: Molecular Features Of Autophagy Cytosolic Receptorsmentioning

confidence: 99%

Pro-Tumoral Functions of Autophagy Receptors in the Modulation of Cancer Progression

2021

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Cancer progression involves a variety of pro-tumorigenic biological processes including cell proliferation, migration, invasion, and survival. A cellular pathway implicated in these pro-tumorigenic processes is autophagy, a catabolic route used for recycling of cytoplasmic components to generate macromolecular building blocks and energy, under stress conditions, to remove damaged cellular constituents to adapt to changing nutrient conditions and to maintain cellular homeostasis. During autophagy, cells form a double-membrane sequestering a compartment termed the phagophore, which matures into an autophagosome. Following fusion with the lysosome, the cargo is degraded inside the autolysosomes and the resulting macromolecules released back into the cytosol for reuse. Cancer cells use this recycling system during cancer progression, however the key autophagy players involved in this disease is unclear. Accumulative evidences show that autophagy receptors, crucial players for selective autophagy, are overexpressed during cancer progression, yet the mechanisms whereby pro-tumorigenic biological processes are modulated by these receptors remains unknown. In this review, we summarized the most important findings related with the pro-tumorigenic role of autophagy receptors p62/SQSTM1, NBR1, NDP52, and OPTN in cancer progression. In addition, we showed the most relevant cargos degraded by these receptors that have been shown to function as critical regulators of pro-tumorigenic processes. Finally, we discussed the role of autophagy receptors in the context of the cellular pathways implicated in this disease, such as growth factors signaling, oxidative stress response and apoptosis. In summary, we highlight that autophagy receptors should be considered important players of cancer progression, which could offer a niche for the development of novel diagnosis and cancer treatment strategies.

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Epithelial-Mesenchymal Transition Markers in Breast Cancer and Pathological Responseafter Neoadjuvant Chemotherapy

Cited by 28 publications

References 45 publications

Notch Signaling in Breast Cancer: A Role in Drug Resistance

Notch Signaling in Breast Cancer: A Role in Drug Resistance

A “NOTCH” Deeper into the Epithelial-To-Mesenchymal Transition (EMT) Program in Breast Cancer

Pro-Tumoral Functions of Autophagy Receptors in the Modulation of Cancer Progression

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