Oncogenic role of DDX3 in breast cancer biogenesis

Botlagunta, Mahendran; Vesuna, Farhad; Mironchik, Yelena; Raman, Avi; Lisok, Ala; Winnard, Paul T.; Mukadam, S; Diest, Paul van; Chen, J H; Farabaugh, Philip J.; Patel, Arvind H.; Raman, Venu

doi:10.1038/onc.2008.33

Cited by 195 publications

(249 citation statements)

References 38 publications

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“…For example, upon HIV infection and in a number of cancers, including acute myeloid leukemia and breast cancer, DDX3 expression is greatly upregulated. [37][38][39] Consequently, it would be of interest to investigate whether elevated levels of DDX3 might have any effect on cellular translation activities during HIV infection and during cancer progression.…”

Section: Discussionmentioning

confidence: 99%

“…Finally, DDX3, like Ded1p, has been implicated in cell growth control, although whether it plays a positive or negative role remains unclear. 22,30,37,46 At least in some cases, increased expression of DDX3 was found to promote cell growth, proliferation and even transformation. 22,30,37,46 Because a number of cellular proteins involved in regulating cell growth and programmed cell death are produced via IRES-mediated translation under stressed conditions, 47 it would be of interest to examine whether and how DDX3 participates in such cellular IRES-mediated translation.…”

Section: Nuclear Export Of Metazoan Ded1p/ddx3 Homologsmentioning

confidence: 99%

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The current understanding of Ded1p/DDX3 homologs from yeast to human

Tarn¹

2009

RNA Biology

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Section: Discussionmentioning

confidence: 99%

Section: Nuclear Export Of Metazoan Ded1p/ddx3 Homologsmentioning

confidence: 99%

The current understanding of Ded1p/DDX3 homologs from yeast to human

Tarn¹

2009

RNA Biology

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“…Many characterized RNA helicases have been found to be fundamental in essential cellular processes (1,26). In recent years, a few RNA helicases have been found to participate in cancer development even though their detailed molecular mechanisms remain largely undiscovered (27)(28)(29)(30)(31)(32)(33). Furthermore, despite the characterization of several DEAD/DEAH proteins, few specific inhibitors targeting these ATP-dependent helicases have been developed.…”

Section: Discussionmentioning

confidence: 99%

DHX33 Transcriptionally Controls Genes Involved in the Cell Cycle

Yuan

Wang

Fan

et al. 2016

Molecular and Cellular Biology

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The RNA helicase DHX33 has been shown to be a critical regulator of cell proliferation and growth. However, the underlying mechanisms behind DHX33 function remain incompletely understood. We present original evidence in multiple cell lines that DHX33 transcriptionally controls the expression of genes involved in the cell cycle, notably cyclin, E2F1, cell division cycle (CDC), and minichromosome maintenance (MCM) genes. DHX33 physically associates with the promoters of these genes and controls the loading of active RNA polymerase II onto these promoters. DHX33 deficiency abrogates cell cycle progression and DNA replication and leads to cell apoptosis. In zebrafish, CRISPR-mediated knockout of DHX33 results in downregulation of cyclin A2, cyclin B2, cyclin D1, cyclin E2, cdc6, cdc20, E2F1, and MCM complexes in DHX33 knockout embryos. Additionally, we found the overexpression of DHX33 in a subset of non-small-cell lung cancers and in Ras-mutated human lung cancer cell lines. Forced reduction of DHX33 in these cancer cells abolished tumor formation in vivo. Our study demonstrates for the first time that DHX33 acts as a direct transcriptional regulator to promote cell cycle progression and plays an important role in driving cell proliferation during both embryo development and tumorigenesis.

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Section: Introductionmentioning

confidence: 99%

“…Moreover, elevated expression of DDX3 was found in a highly aggressive metastatic breast cancer cell line, MDA-MB-231, as compared with non-metastatic MCF-7 cells, which show its potential role in aggressive breast cancers and associated metastasis. 5,6 We have previously reported that overexpression of DDX3 in immortalized non-turmorigenic MCF10A cells promoted neoplastic transformation as indicated by down regulation of a cell adhesion molecule, E-cadherin.5 Down-regulation of E-cadherin is a common feature of a variety of metastatic epithelial tumors, including those of the lung, breast and prostate cancer.5,7-9 Hypoxic regions of solid tumors were considered to be the primary sites for the generation of the metastatic phenotype and have been demonstrated to be chemo and radio-resistant. [10][11][12][13][14] We have also reported that hypoxia inducible factor (HIF-1) induce the expression of DDX3 in two different breast cell lines by binding directly or indirectly to the hypoxia-response element (HRE) in the DDX3 proximal promoter.…”

mentioning

confidence: 99%

In vitro Anti-Cancer Activity of Rosuvastatin and Ketorolac Nanoformulations against DDX3

Bheemanapally¹,

Thimmaraju²,

Kasagoni³

et al. 2017

JYP

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INTRODUCTIONHuman DDX3 gene encodes a polypeptide of 662 amino acids and this protein plays an important role in several aspects of RNA metabolism. 1,2 This protein has two clear distinguishable domains comprised of N-terminal DEAD box domain 1 (211-403 residues) and C-terminal helicase domain 2 (411-575 residues). Both domains displayed RecA-like folds comprising a central β-sheet flanked by α-helices connected by a noncanonical linker of 11 amino acids.3 Expression of DDX3 was detected in several tissues such as testis, colon, lung, liver, skeletal muscle, and kidney 2,4 indicating the universal role of DDX3 in cellular homeostasis. Moreover, elevated expression of DDX3 was found in a highly aggressive metastatic breast cancer cell line, MDA-MB-231, as compared with non-metastatic MCF-7 cells, which show its potential role in aggressive breast cancers and associated metastasis. 5,6 We have previously reported that overexpression of DDX3 in immortalized non-turmorigenic MCF10A cells promoted neoplastic transformation as indicated by down regulation of a cell adhesion molecule, E-cadherin.5 Down-regulation of E-cadherin is a common feature of a variety of metastatic epithelial tumors, including those of the lung, breast and prostate cancer.5,7-9 Hypoxic regions of solid tumors were considered to be the primary sites for the generation of the metastatic phenotype and have been demonstrated to be chemo and radio-resistant. [10][11][12][13][14] We have also reported that hypoxia inducible factor (HIF-1) induce the expression of DDX3 in two different breast cell lines by binding directly or indirectly to the hypoxia-response element (HRE) in the DDX3 proximal promoter. 15 On the other hand, a significant down regulation of DDX3 expression is found in hepatocellular carcinoma (HCCs) from the hepatitis B virus (HBV) positive patients, but not from HCV positive in comparison to the corresponding non tumor tissues. 16 In the hepatocellular carcinoma model, DDX3 was found to act as a tumor suppressor by activating the expression of cyclin dependent kinase inhibitor p21 cip1 . 17 Besides cancer, induced expression of DDX3 was also found in HIV-1 infected cells. 18,19 Overall, it suggests that DDX3 is a multifunctional protein and it plays a specific role in regulatory mechanisms and signaling pathways. Apart from embryonic development, this gene is also involved in multiple diseases like HIV, Neuro-degenerative diseases, hepatocellular carcinoma and brain and breast cancer. Several Synthetic compounds have been discovered to inhibit the function of DDX3 by blocking the function of helicase activity. [20][21][22][23][24] Synthetic drugs are those substances that are produced entirely from chemical reactions in a laboratory. Synthetic drugs most often have shown to suppress the immune system by paralyzing the bone marrow. 25,26 Moreover, it takes an average of about 8 to 12 years from the time a cancer drug enters into clinical trials from the research lab.27,28 Therefore, we focused to identify FDA approved drugs against D...

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Oncogenic role of DDX3 in breast cancer biogenesis

Cited by 195 publications

References 38 publications

The current understanding of Ded1p/DDX3 homologs from yeast to human

The current understanding of Ded1p/DDX3 homologs from yeast to human

DHX33 Transcriptionally Controls Genes Involved in the Cell Cycle

In vitro Anti-Cancer Activity of Rosuvastatin and Ketorolac Nanoformulations against DDX3

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