Epithelial-to-Mesenchymal Transition Activates PERK–eIF2α and Sensitizes Cells to Endoplasmic Reticulum Stress

Feng, Yuxiong; Sokol, Ethan S.; Vecchio, Catherine A. Del; Sanduja, Sandhya; Claessen, Jasper H.L.; Proia, Theresa A.; Jin, Dexter X.; Reinhardt, Ferenc; Ploegh, Hidde L.; Wang, Qiu; Gupta, Piyush B.

doi:10.1158/2159-8290.cd-13-0945

Cited by 264 publications

(264 citation statements)

References 50 publications

(40 reference statements)

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“…We found that NACA deficiency does trigger the UPR in zebrafish larvae, and that treatment of naca mutants with the chemical chaperon 4-PBA significantly suppressed SRC apoptosis, and restored CHT haematopoiesis. Interestingly, EMT-derived mesenchymal cells in general were recently shown to be exquisitely sensitive to ER stress-induced apoptosis 30 . This feature was shown to be linked to their high level of extracellular matrix secretory activity, which involves steady ER development.…”

Section: Discussionmentioning

confidence: 99%

NACA deficiency reveals the crucial role of somite-derived stromal cells in haematopoietic niche formation

et al. 2015

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Section: Discussionmentioning

confidence: 99%

NACA deficiency reveals the crucial role of somite-derived stromal cells in haematopoietic niche formation

et al. 2015

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“…In vivo and 3D hydrogel studies were performed as previously described (18,28). All computational analyses, reagents, public datasets used, and other protocols are described in SI Materials and Methods.…”

Section: Methodsmentioning

confidence: 99%

SMARCE1 is required for the invasive progression of in situ cancers

Sokol

Feng

Jin

et al. 2017

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

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Advances in mammography have sparked an exponential increase in the detection of early-stage breast lesions, most commonly ductal carcinoma in situ (DCIS). More than 50% of DCIS lesions are benign and will remain indolent, never progressing to invasive cancers. However, the factors that promote DCIS invasion remain poorly understood. Here, we show that SMARCE1 is required for the invasive progression of DCIS and other early-stage tumors. We show that SMARCE1 drives invasion by regulating the expression of secreted proteases that degrade basement membrane, an ECM barrier surrounding all epithelial tissues. In functional studies, SMARCE1 promotes invasion of in situ cancers growing within primary human mammary tissues and is also required for metastasis in vivo. Mechanistically, SMARCE1 drives invasion by forming a SWI/SNF-independent complex with the transcription factor ILF3. In patients diagnosed with early-stage cancers, SMARCE1 expression is a strong predictor of eventual relapse and metastasis. Collectively, these findings establish SMARCE1 as a key driver of invasive progression in early-stage tumors.T he past two decades have brought an exponential increase in the diagnosis of early-stage breast lesions, most commonly ductal carcinoma in situ (DCIS). DCIS remains encapsulated within the ductal-lobular architecture of mammary epithelium; in contrast, invasive breast cancers have escaped this architecture by breaking through the basement membrane, a layer of ECM rich in collagen (IV) and laminins that separates epithelial tissues from the adjacent stromal microenvironment ( Fig. S1A) (1). This distinction has a critical impact on patient prognosis: whereas women with DCIS show no reduction in survival 5 y after diagnosis, those with invasive cancers have a 15-74% reduction in 5-y survival rates depending on the extent of tumor invasion at diagnosis (2). Given these observations, there is significant interest in finding genes that promote the invasive progression of early-stage tumors (3). Previous studies have sought molecular alterations present in invasive tumors but not DCIS, leading to the identification of hundreds of genomic and gene-expression alterations specifically associated with invasive cancers (4-6). However, it is unclear if genes that are amplified or up-regulated in invasive cancers also functionally drive DCIS invasion. In large part, the difficulty in addressing this question can be traced to a paucity of experimental systems that model cancer invasion within a microenvironment that faithfully replicates human breast tissue.The treatment of early-stage cancers remains an unresolved issue. Women with early-stage breast cancers-which include DCIS and stage I tumors that have not entered the lymph nodesare typically treated by lumpectomy followed by localized radiation. However, recurrence with metastasis occurs in a significant fraction of women with stage I cancers; if such tumors could be prospectively identified, it would be possible to preemptively adopt a more aggressive therapy. Conver...

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“…This molecule induces cell death in a CHOP-dependent manner in a number of cell lines, and there is enthusiastic support to develop this molecule for cancer therapy. A recent study also suggests that modulation of ER stress could be a selective target for cancer cells that undergo EMT (Feng et al 2014). During EMT, cells secrete more secretory molecules, such as extracellular matrix proteins, which provokes eIF2α phosphorylation and subsequent ATF4 induction.…”

Section: Therapeutic Implicationsmentioning

confidence: 99%

“…Thus, cells undergoing EMT are more sensitive to ER stress compared with cells without EMT. This selective toxicity of cells stressed by a harsh environment or protein misfolding offers a selective advantage to using these agents to uniquely destroy tumor cells (Feng et al 2014).…”

Section: Therapeutic Implicationsmentioning

confidence: 99%

Physiological/pathological ramifications of transcription factors in the unfolded protein response

2017

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Numerous environmental, physiological, and pathological insults disrupt protein-folding homeostasis in the endoplasmic reticulum (ER), referred to as ER stress. Eukaryotic cells evolved a set of intracellular signaling pathways, collectively termed the unfolded protein response (UPR), to maintain a productive ER protein-folding environment through reprogramming gene transcription and mRNA translation. The UPR is largely dependent on transcription factors (TFs) that modulate expression of genes involved in many physiological and pathological conditions, including development, metabolism, inflammation, neurodegenerative diseases, and cancer. Here we summarize the current knowledge about these mechanisms, their impact on physiological/pathological processes, and potential therapeutic applications.

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Epithelial-to-Mesenchymal Transition Activates PERK–eIF2α and Sensitizes Cells to Endoplasmic Reticulum Stress

Cited by 264 publications

References 50 publications

NACA deficiency reveals the crucial role of somite-derived stromal cells in haematopoietic niche formation

NACA deficiency reveals the crucial role of somite-derived stromal cells in haematopoietic niche formation

SMARCE1 is required for the invasive progression of in situ cancers

Physiological/pathological ramifications of transcription factors in the unfolded protein response

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