4.6 Article

Bioinformatic Analyses of the Ferroptosis-Related lncRNAs Signature for Ovarian Cancer

期刊

出版社

FRONTIERS MEDIA SA
DOI: 10.3389/fmolb.2021.735871

关键词

ovarian cancer; ferroptosis; lncRNA; risk model; immune

资金

  1. Medical Scientific Research Foundation of Zhejiang Province [2019KY495]
  2. Natural Science Foundation of Zhejiang Province [LGF18H160087]

向作者/读者索取更多资源

This study constructed an FRL-signature for ovarian cancer (OC) patients, identifying FRLs with significant prognostic value and their association with ferroptosis score, immune factors, and microenvironment cells. The study revealed the regulatory mechanisms of FRLs and provided potential therapeutic targets.
Both ferroptosis and lncRNAs are significant for ovarian cancer (OC). Whereas, the study of ferroptosis-related lncRNAs (FRLs) still few in ovarian cancer. We first constructed an FRL-signature for patients with OC in the study. A total of 548 FRLs were identified for univariate Cox regression analysis, and 21 FRLs with significant prognosis were identified. The prognostic characteristics of nine FRLs was constructed and validated, showing opposite prognosis in two subgroups based on risk scores. The multivariate Cox regression analysis and nomogram further verified the prognostic value of the risk model. By calculating ferroptosis score through ssGSEA, we found that patients with higher risk scores exhibited higher ferroptosis scores, and high ferroptosis score was a risk factor. There were 40 microenvironment cells with significant differences in the two groups, and the difference of Stromal score between the two groups was statistically significant. Six immune checkpoint genes were expressed at different levels in the two groups. In addition, five m6A regulators (FMR1, HNRNPC, METTL16, METTL3, and METTL5) were higher expressed in the low-risk group. GSEA revealed that the risk model was associated with tumor-related pathways and immune-associated pathway. We compared the sensitivity of chemotherapy drugs between the two risk groups. We also explored the co-expression, ceRNA relation, cis and trans interaction of ferroptosis-related genes and lncRNAs, providing a new idea for the regulatory mechanisms of FRLs. Moreover, the nine FRLs were selected for detecting their expression levels in OC cells and tissues.

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