PML represses lung cancer metastasis by suppressing the nuclear EGFR-mediated transcriptional activation of<i>MMP2</i>

Kuo, Hong Yi; Huang, Ya‐Fang; Tseng, Chin Hsiu; Chen, Yi‐Chen; Chang, Yu Wei; Shih, Hsiu Ming; Wu, Cheng‐Wen

doi:10.4161/15384101.2014.949212

Cited by 22 publications

(18 citation statements)

References 51 publications

(54 reference statements)

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“…It has been reported that nEGFR is involved in regulating MMP2 promotera ctivity. [29] We found that 1 resulted in significant downregulationo f MMP2 expression ands ignificantly suppressed invasion in H1299c ells. NuclearE GFR has also been shown to regulate the proteins that cause tumor invasion, such as cyclin D1 and iNOS.…”

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confidence: 61%

“…EGFR contentsa lso decreased in the nucleus after KPNB1 knockdown to levels similar to those observed after using 100 nm 1;t his is consistent with our findings from confocal microscopy.T ogether,t hese data show that 1 significantly inhibits KPNB1-mediated nucleari mport of EGFR in H1299 cells. It has been reported that nuclear EGFR binds to AT-rich sequence (ATR) in the promoter of matrix metalloprotease-2 (MMP2), [29] which is important for cancerm etastasis, [30] resultingi nt he expression of MMP2.B ecause 1 inhibits the translocation of EGFR to the nucleus, the regulation of MMP2 and the influenceo fM MP2 on invasion by 1 were examined by meanso ft he quantitative reverse-transcription polymerase chain reaction (qRT-PCR). As shown in Figure 3A,t reatment with 20 nm 1 resulted in significantly lower levels of MMP2 expression compared with that of the control value.…”

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confidence: 99%

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A Small Organic Molecule Blocks EGFR Transport into the Nucleus by the Nonclassical Pathway Resulting in Repression of Cancer Invasion

Jeong

et al. 2017

ChemBioChem

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In addition to the traditional epidermal growth factor receptor (EGFR) signaling pathways, nuclear EGFR has been shown to control multiple cellular functions, including cell proliferation and invasion. It has been reported that EGFR is transported into the nucleus after forming a complex with KPNA/KPNB1 or KPNB1. Herein, it is shown that EGFR can interact with both KP and KPNA, but EGF-activated EGFR mostly binds with KPNB1 through the pull-down assay. Also, a small organic molecule (1), an effective binder of KPNB1, inhibits the interaction between EGFR and KPNB1 in the nonclassical transport pathway, but not KPNA. Furthermore, treatment of cancer cells with 1 noticeably blocks the nuclear entry of EGFR, which results in significant suppression of invasion by lung cancer H1299 cells. These findings show that 1 is an effective inhibitor of EGFR/KPNB1 interactions in vitro, it may be used in cellular studies as a tool to determine the role of nuclear EGFR, and it is a drug candidate.

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confidence: 61%

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confidence: 99%

A Small Organic Molecule Blocks EGFR Transport into the Nucleus by the Nonclassical Pathway Resulting in Repression of Cancer Invasion

Jeong

et al. 2017

ChemBioChem

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“…The antibody against mouse WDR4 was described previously (39). Other antibodies used in this study are the expression of MMP2 and integrin β1 in certain cell types (10,49), their expression was not significantly induced by the WDR4/ PML axis in our cell system. Instead, our study suggests that the WDR4/PML axis acts through uPAR and SAA2 to influence the activity of integrin and MMPs.…”

Section: Methodsmentioning

confidence: 99%

Ubiquitination of tumor suppressor PML regulates prometastatic and immunosuppressive tumor microenvironment

Wang

Chen

Chang

et al. 2017

Journal of Clinical Investigation

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“…Interestingly, members of the RTK sub‐families are also present in the nucleus, and are referred to as ‘membrane receptor in the nucleus' or MRINs . Accumulating evidence indicates that at least 12 RTK families contain MRINs that exist either as a holoreceptor or in a truncated form with novel non‐canonical functions in transcriptional regulation, DNA damage and repair, and cell proliferation and invasion . In various cancer types, nuclear RTK expression is associated with poor prognosis .…”

Section: Introductionmentioning

confidence: 99%

Proteolytic cleavage, trafficking, and functions of nuclear receptor tyrosine kinases

Chen

Hung

2015

The FEBS Journal

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Over three quarters of receptor tyrosine kinase (RTK) families are reported to have intracellular localization in response to environmental stimuli. Internalized RTK can bind to non-canonical substrates and affect various cellular processes. Many of the intracellular RTKs exist as fragmented forms that are generated by γ-secretase cleavage of the full-length receptor, shedding, alternative splicing, or alternative translation initiation. Soluble RTK fragments are stabilized and intracellularly transported into subcellular compartments, such as the nucleus, by binding to chaperon or transcription factors while membrane-bound RTKs (full-length or truncated) are transported from the plasma membrane to the endoplasmic reticulum (ER) through the well-established Rab- or clathrin adaptor protein (AP)-coated vesicle retrograde trafficking pathway. Subsequent nuclear transport of membrane-bound RTK can occur via two pathways, INFS and INTERNET, with the former characterized by the release of receptors from ER into the cytosol and the latter by the release of membrane-bound transport from the ER into the nucleoplasm through the inner nuclear membrane. While most non-canonical intracellular RTK signaling is related to transcriptional regulation, there may be other functions that have yet to be discovered. In this review, we summarize the proteolytic processing, intracellular trafficking, and nuclear functions of RTKs and discuss how they promote cancer progression and their clinical implications.

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PML represses lung cancer metastasis by suppressing the nuclear EGFR-mediated transcriptional activation ofMMP2

Cited by 22 publications

References 51 publications

A Small Organic Molecule Blocks EGFR Transport into the Nucleus by the Nonclassical Pathway Resulting in Repression of Cancer Invasion

A Small Organic Molecule Blocks EGFR Transport into the Nucleus by the Nonclassical Pathway Resulting in Repression of Cancer Invasion

Ubiquitination of tumor suppressor PML regulates prometastatic and immunosuppressive tumor microenvironment

Proteolytic cleavage, trafficking, and functions of nuclear receptor tyrosine kinases

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