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

Yu, Bin; Zhou, Shaolin; Long, Dakun; Ning, Yuxiang; Yao, Hanlin; Zhou, Encheng; Wang, Yanfeng

doi:10.1111/cas.15393

Cited by 10 publications

(6 citation statements)

References 72 publications

(173 reference statements)

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“…Two recent studies reported that the human Spb4 homolog DDX55 is strongly upregulated in various lung cancers and hepatocellular carcinoma (HCC) tissues promoting HCC cell proliferation and migration ( Cui et al, 2021 ; Yu et al, 2022 ). Thus, the obtained insights into the Spb4 function for ribosome biogenesis could be of relevance for medical studies and treatment of such cancer types.…”

Section: Discussionmentioning

confidence: 99%

Concurrent remodelling of nucleolar 60S subunit precursors by the Rea1 ATPase and Spb4 RNA helicase

Mitterer

Thoms²,

Buschauer³

et al. 2023

eLife

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Biogenesis intermediates of nucleolar ribosomal 60S precursor particles undergo a number of structural maturation steps before they transit to the nucleoplasm and are finally exported into the cytoplasm. The AAA+-ATPase Rea1 participates in the nucleolar exit by releasing the Ytm1-Erb1 heterodimer from the evolving pre-60S particle. Here, we show that the DEAD-box RNA helicase Spb4 with its interacting partner Rrp17 is further integrated into this maturation event. Spb4 binds to a specific class of late nucleolar pre-60S intermediates, whose cryo-EM structure revealed how its helicase activity facilitates melting and restructuring of 25S rRNA helices H62 and H63/H63a prior to Ytm1-Erb1 release. In vitro maturation of such Spb4-enriched pre-60S particles, incubated with purified Rea1 and its associated pentameric Rix1-complex in the presence of ATP, combined with cryo-EM analysis depicted the details of the Rea1-dependent large-scale pre-ribosomal remodelling. Our structural insights unveil how the Rea1 ATPase and Spb4 helicase remodel late nucleolar pre-60S particles by rRNA restructuring and dismantling of a network of several ribosomal assembly factors.

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Section: Discussionmentioning

confidence: 99%

Concurrent remodelling of nucleolar 60S subunit precursors by the Rea1 ATPase and Spb4 RNA helicase

Mitterer

Thoms²,

Buschauer³

et al. 2023

eLife

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“…Oxeiptosis is a specific cellular response to ROS generated by oxidative stress with the potential to induce In this study, the enrichment analysis of biological functions and signaling pathways, the results seem to indicate that OCGs are closely related to both cell proliferation and death, including biological processes such as chromosome structure, mitotic processes, and cell cycle. We noticed that OCGs contain members of several gene families participate in many malignancy-related biological processes, including T-complexpolypeptide1 family, [24,25] Dead-box family [26][27][28][29] and heterogeneous nuclear ribonucleoprotein (hnRNPs) family. hnRNPs is a class of RNA-binding proteins that acts synergistically with the dead-box family in eukaryotes.…”

Section: Discussionmentioning

confidence: 99%

Oxeiptosis core genes and their multi-omics analysis in hepatocellular carcinoma

Lin,

Li,

Zhao

et al. 2023

Medicine

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Oxeiptosis is a recently discovered caspase-independent, non-inflammatory programmed cell death modality. Current studies suggest that oxeiptosis has crucial effects on biological processes in a variety of diseases. However, the mechanism of oxeiptosis in hepatocellular carcinoma (HCC) remains unclear and no relevant studies have been published. Therefore, this study is intended to investigate the mechanism and prognostic role of oxeiptosis-related genes in HCC. We explored the mechanisms and molecular phenotypes underlying the role of oxeiptosis in HCC through multi-omics analysis. Firstly, we obtained RNA-sequencing and clinical data from public database and divided the samples into trial and validation cohorts in subsequent analyses. We then screened oxeiptosis core genes (OCGs) and screened prognosis-related genes. Based on different molecular markers, we identified the molecular phenotypes of HCC, and the potential OCGs molecular mechanisms were explored. Subsequently, we construct a prognostic prediction system for HCC. Finally, we analyzed the tumor microenvironment and the immune escape phenomenon. We screened a total of 69 OCGs, most of which were prognostic risk factors for HCC. A majority of OCGs were enriched in cell cycle regulation and mitotic processes, which were related to both tumor cell proliferation and death. We identified 2 different molecular typing options with significant differences in prognosis, function, and signaling pathway enrichment between different molecular subtypes. The prognostic prediction model combined with molecular phenotypes and had a good predictive effect. Finally, we found CD4 + T-cell exhaustion in samples with specific molecular phenotypes. Through multi-omics analysis of OCGs, we not only revealed the possible molecular mechanisms of OCGs in HCC but also provided a prognostic prediction system for clinical application through molecular typing and risk scoring model. Meanwhile, we found immune escape mechanisms in HCC.

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“…TMPRSS2-enriched exosomes were found to suppress the packaging of pro-tumoral nidogen into exosomes and inhibit proliferation and migration of immortalized hepatic cell ( 12 ). In addition, various molecules, including DEAD-box helicase 55 (DDX55), CPE, miR-3129, LINC00161, clathrin light chain A (CTLA), and miR-25, were found to be enriched in cancer-derived exosomes and induce cell proliferation ( 10 , 19 , 21 – 24 ). Signaling alterations upon sEV treatment primarily involved EMT markers, Wnt/β-catenin signaling, and cell cycle pathways ( 19 , 21 , 23 ).…”

Section: Sevs Derived From Hcc Cancer Cells and Cancer Stemnessmentioning

confidence: 99%

“…In addition, various molecules, including DEAD-box helicase 55 (DDX55), CPE, miR-3129, LINC00161, clathrin light chain A (CTLA), and miR-25, were found to be enriched in cancer-derived exosomes and induce cell proliferation ( 10 , 19 , 21 – 24 ). Signaling alterations upon sEV treatment primarily involved EMT markers, Wnt/β-catenin signaling, and cell cycle pathways ( 19 , 21 , 23 ). These findings suggest potential mechanisms behind the crosstalk between drug resistance pathways and proliferation signaling via sEVs in HCC.…”

Section: Sevs Derived From Hcc Cancer Cells and Cancer Stemnessmentioning

confidence: 99%

Extracellular vesicles and cancer stemness in hepatocellular carcinoma – is there a link?

Tian,

Lu,

2024

Front. Immunol.

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Hepatocellular carcinoma (HCC) is a highly aggressive malignancy, with high recurrence rates and notorious resistance to conventional chemotherapy. Cancer stemness refers to the stem-cell-like phenotype of cancer cells and has been recognized to play important roles in different aspects of hepatocarcinogenesis. Small extracellular vesicles (sEVs) are small membranous particles secreted by cells that can transfer bioactive molecules, such as nucleic acids, proteins, lipids, and metabolites, to neighboring or distant cells. Recent studies have highlighted the role of sEVs in modulating different aspects of the cancer stemness properties of HCC. Furthermore, sEVs derived from diverse cellular sources, such as cancer cells, stromal cells, and immune cells, contribute to the maintenance of the cancer stemness phenotype in HCC. Through cargo transfer, specific signaling pathways are activated within the recipient cells, thus promoting the stemness properties. Additionally, sEVs can govern the secretion of growth factors from non-cancer cells to further maintain their stemness features. Clinically, plasma sEVs may hold promise as potential biomarkers for HCC diagnosis and treatment prediction. Understanding the underlying mechanisms by which sEVs promote cancer stemness in HCC is crucial, as targeting sEV-mediated communication may offer novel strategies in treatment and improve patient outcome.

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

Cited by 10 publications

References 72 publications

Concurrent remodelling of nucleolar 60S subunit precursors by the Rea1 ATPase and Spb4 RNA helicase

Concurrent remodelling of nucleolar 60S subunit precursors by the Rea1 ATPase and Spb4 RNA helicase

Oxeiptosis core genes and their multi-omics analysis in hepatocellular carcinoma

Extracellular vesicles and cancer stemness in hepatocellular carcinoma – is there a link?

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