4.6 Article

Systematic discrimination of the repetitive genome in proximity of ferroptosis genes and a novel prognostic signature correlating with the oncogenic lncRNA CRNDE in multiple myeloma

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FRONTIERS IN ONCOLOGY
卷 12, 期 -, 页码 -

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FRONTIERS MEDIA SA
DOI: 10.3389/fonc.2022.1026153

关键词

ferroptosis; lncRNA; long noncoding RNA; repetitive genome; multiple myeloma; gene signature; prognosis

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资金

  1. Key R & D plan of Jiangxi Province of China [20202BBGL73111]
  2. National Natural Science Foundation of China [82260030]
  3. Central Guidance of Local Science and Technology Development Fund [20211ZDG02002]
  4. Translational Research Grant of NCRCH [2021WWA02]

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New insights into iron-dependent form of regulated cell death ferroptosis in cancer have shown its potential use in cancer therapy. Systematic profiling of ferroptosis gene signatures as prognostic factors has gained attention in several cancers. In this study, the presence of repetitive genomes near ferroptosis genes and a prognostic gene signature associated with multiple myeloma (MM) were investigated.
Emerging insights into iron-dependent form of regulated cell death ferroptosis in cancer have opened a perspective for its use in cancer therapy. Of interest, a systematic profiling of ferroptosis gene signatures as prognostic factors has gained special attention in several cancers. Herein, we sought to investigate the presence of repetitive genomes in the vicinity of ferroptosis genes that may influence their expression and to establish a prognostic gene signature associated with multiple myeloma (MM). Our analysis showed that genes associated with ferroptosis were enriched with the repetitive genome in their vicinity, with a strong predominance of the SINE family, followed by LINE, of which the most significant discriminant values were SINE/Alu and LINE/L1, respectively. In addition, we examined in detail the performance of these genes as a cancer risk prediction model and specified fourteen ferroptosis-related gene signatures, which identified MM high-risk patients with lower immune/stromal scores with higher tumor purity in their immune microenvironment. Of interest, we also found that lncRNA CRNDE correlated with a risk score and was highly associated with the majority of genes comprising the signature. Taken together, we propose to investigate the molecular impact of the repetitive genome we have highlighted on the local transcriptome of ferroptosis genes in cancer. Furthermore, we revealed a genomic signature/biomarker related to ferroptosis that can be used to predict the risk of survival in MM patients.

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