DDX54 Plays a Cancerous Role Through Activating P65 and AKT Signaling Pathway in Colorectal Cancer

Yu, Yi; Wang, Jinglong; Meng, Lili; Hu, Chun-Ting; Yan, Zhao-Wen; He, Zhiping; Shi, Xiaoqin; Fu, Guo‐Hui; Zu, Lidong

doi:10.3389/fonc.2021.650360

Cited by 13 publications

(5 citation statements)

References 37 publications

(39 reference statements)

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“…As for the regulatory mechanisms underlying the impact of DDX55 on β‐catenin signaling, we concentrated on the correlation between DDX55 and PIK3CA, an oncogene encoding PI3Kα catalytic subunit and acting as a well‐known activator of AKT in tumorigenesis, under the guidance of the sequencing analysis 51 . Consistent with the existing evidence with regard to the associations between DEAD‐box proteins and the PI3K/Akt pathway, our data demonstrated that DDX55 could significantly enhance PIK3CA expression both at the mRNA and protein levels, and further reinforced β‐catenin protein stability dependent on PI3K/Akt/GSK‐3β pathway activation 46,52–54 . A high percentage of aberrant activation of the Wnt/β‐catenin signaling (30%–40%) and the PI3K/Akt signaling (nearly 50%) have been reported in human HCC samples, which highlights the potential of DDX55 as a valuable therapeutic target in those HCC 34,55 …”

Section: Discussionsupporting

confidence: 72%

“…51 Consistent with the existing evidence with regard to the associations between DEAD-box proteins and the PI3K/ Akt pathway, our data demonstrated that DDX55 could significantly enhance PIK3CA expression both at the mRNA and protein levels, and further reinforced β-catenin protein stability dependent on PI3K/Akt/GSK-3β pathway activation. 46,[52][53][54] A high percentage of aberrant activation of the Wnt/β-catenin signaling (30%-40%) and the PI3K/Akt signaling (nearly 50%) have been reported in human HCC samples, which highlights the potential of DDX55 as a valuable therapeutic target in those HCC. 34,55 Emerging evidence has suggested that DEAD-box proteins generally function as components of multi-protein complexes and act as a transcriptional co-activator in gene expression regulation.…”

Section: Discussionmentioning

confidence: 99%

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DDX55 promotes hepatocellular carcinoma progression by interacting with BRD4 and participating in exosome‐mediated cell‐cell communication

Zhou

Long

et al. 2022

Cancer Science

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The involvement of DEAD‐box helicase 55 (DDX55) in oncogenesis has been suggested, but its biological role in hepatocellular carcinoma (HCC) remains unknown. The present study verified the upregulation of DDX55 in HCC tissues compared with non‐tumor controls. DDX55 displayed the highest prognostic values among the DEAD‐box protein family for recurrence‐free survival and overall survival of HCC patients. In addition, the effects of DDX55 in the promotion of HCC cell proliferation, migration, and invasion were determined ex vivo and in vivo. Mechanistically, we revealed that DDX55 could interact with BRD4 to form a transcriptional regulatory complex that positively regulated PIK3CA transcription. Following that, β‐catenin signaling was activated in a PI3K/Akt/GSK‐3β dependent manner, thus inducing cell cycle progression and epithelial–mesenchymal transition. Intriguingly, both DDX55 mRNA and protein were identified in the exosomes derived from HCC cells. Exosomal DDX55 was implicated in intercellular communication between HCC cells with high or low DDX55 levels and between HCC cells and endothelial cells, thereby promoting the malignant phenotype of HCC cells and angiogenesis. In conclusion, DDX55 may be a valuable prognostic biomarker and therapeutic target in HCC.

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Section: Discussionsupporting

confidence: 72%

Section: Discussionmentioning

confidence: 99%

DDX55 promotes hepatocellular carcinoma progression by interacting with BRD4 and participating in exosome‐mediated cell‐cell communication

Zhou

Long

et al. 2022

Cancer Science

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“…Cao Several DDX family members are known to regulate mRNA translation in cancer cells, and inhibitors targeting DDX proteins are currently under development. DDX54 was reported to play a cancerous role in colorectal cancer [29]. Our data suggest that high DDX54 expression predicts poor PFS and OS in LUAD patients.…”

Section: Discussionmentioning

confidence: 54%

LINC00908 attenuates LUAD tumorigenesis through DEAD-box helicase 54

Zhao

2024

Am J Cancer Res

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Lung adenocarcinoma (LUAD) is one of the leading causes of cancer-related death worldwide. We identified a specific long non-coding RNA (LncRNA), LINC00908, which was downregulated in LUAD tissues and associated with good outcome. LINC00908 inhibited glycolysis by regulating the expression of the DEAD-box helicase 54 (DDX54), which was screened by a nine-gene risk signature, where DDX54 showed a positive correlation with several glycolysis-related genes. Experimental verification confirmed that DDX54 regulated nine key glycolytic enzymes, thereby affecting the level of glycolysis in LUAD. Further, the expression of LINC00908 in LUAD tumorigenesis was modulated by a transcription factor, regulatory factor X2 (RFX2). The RFX2/LINC00908/DDX54 axis regulated LUAD tumor growth, migration, invasion, cell apoptosis and glycolysis both in vitro and in vivo. These results demonstrate that this axis may serve as a novel mediator in LUAD progress and offer a novel therapeutic target for more precise diagnosis and treatment of LUAD.

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“…Furthermore, circ-CELF1 knockdown weakened the binding relation between DDX54 and NFAT5. DDX54 belongs to the RNA helicase family, which affects important cellular process [31]. DDX54 has also been reported to enhance the mRNA stability of SIK2 in triple-negative breast cancer [32].…”

Section: Discussionmentioning

confidence: 99%

circCELF1 Induces the Apoptosis and Autophagy of Astrocytes in Ischemic Stroke via Upregulating NFAT5

Teng²

2022

Cerebrovasc Dis

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Introduction: Ischemic stroke, an abrupt blockage of artery, accounting for the most cases of stroke, causes high neurological mortality across the world. Recent evidence has uncovered that circular RNAs (circRNAs) highly engage in ischemic stroke-related neuronal injury. This study concentrated on a novel circRNA hsa_circ_0000304 (termed as circCELF1), trying to unveil its role and underlying mechanism in ischemic stroke. Methods: RT-qPCR and Western blot assays were conducted to detect the expression levels of RNA and protein, respectively. Functional analysis was performed to evaluate the influences of circCELF1 expression on astrocyte apoptosis and autophagy. Multiple mechanism assays were performed to probe the molecular mechanism underlying circCELF1 regulation. The oxygen-glucose deprivation/reoxygenation (OGD/R)-induced astrocytes model and transient middle cerebral artery occlusion (tMCAO) mouse model were constructed. Results: circCELF1 was found to be upregulated in OGD/R-induced astrocytes, relative to normal astrocytes. circCELF1 knockdown repressed the apoptosis and autophagy of astrocytes. The in vivo study conducted with the tMCAO model also revealed that circCELF1 or NFAT5 deficiency contributed to the suppression of neural injury. Further, circCELF1 was uncovered to elevate NFAT5 expression via recruiting DDX54, functionally promoting astrocyte apoptosis and autophagy. Conclusion: circCELF1 recruits DDX54 to upregulate NFAT5, by which astrocyte apoptosis and autophagy are stimulated.

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DDX54 Plays a Cancerous Role Through Activating P65 and AKT Signaling Pathway in Colorectal Cancer

Cited by 13 publications

References 37 publications

DDX55 promotes hepatocellular carcinoma progression by interacting with BRD4 and participating in exosome‐mediated cell‐cell communication

DDX55 promotes hepatocellular carcinoma progression by interacting with BRD4 and participating in exosome‐mediated cell‐cell communication

LINC00908 attenuates LUAD tumorigenesis through DEAD-box helicase 54

circCELF1 Induces the Apoptosis and Autophagy of Astrocytes in Ischemic Stroke via Upregulating NFAT5

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