Fangxu Yin, Wenhao Zhao, Chen Ding, Chong Hou, Song Wang, Chao Sun, Zexia Zhao, Zhanrui Zhang, Fan Ren, Yuying Liu, Xuanguang Li
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引用次数: 0
Abstract
Background: Long non-coding RNA (lncRNA), a crucial regulator in breast cancer (BC) development, is intricately linked with cellular senescence. However, there is a lack of cellular senescence-related lncRNAs (CSRLs) signature to evaluate the prognosis of BC patients. Methods: Correlation analysis was conducted to identify lncRNAs associated with cellular senescence. Subsequently, a CSRL signature was crafted in the training cohort. The model's accuracy was evaluated through survival analysis and receiver operating characteristic curves. Furthermore, prognostic nomograms amalgamating cellular senescence and clinical characteristics were devised. Tumor microenvironment and checkpoint disparities were compared between low-risk and high-risk groups. The correlation between these signatures and treatment response in BC patients was also investigated. Finally, functional experiments were conducted for validation. Results: A signature comprising nine CSRLs was devised, which demonstrated adept prognostic capability in BC patients. Functional enrichment analysis revealed that tumor and immune-related pathways were predominantly enriched. Compared to the low-risk group, the high-risk group could benefit more from immunotherapy and certain chemotherapeutic agents. The expression of the 9 CSRLs was validated through in vitro experiments in different subtypes of BC cell lines and tissues. AC098484.1 was specifically verified for its association with senescence-associated secretory phenotypes. Conclusion: The CSRLs signature emerges as a promising prognostic biomarker for BC, with implications for immunological studies and treatment strategies. AC098484.1 has potential relevance in the treatment of BC cell senescence, and these findings improve the clinical treatment levels for BC patients.
背景:长非编码RNA(lncRNA)是乳腺癌(BC)发展过程中的一个关键调控因子,与细胞衰老密切相关。然而,目前还缺乏细胞衰老相关 lncRNAs(CSRLs)特征来评估乳腺癌患者的预后。研究方法进行相关性分析以确定与细胞衰老相关的lncRNAs。随后,在训练队列中建立了CSRL特征。通过生存分析和接收者操作特征曲线评估了模型的准确性。此外,还设计出了将细胞衰老和临床特征相结合的预后提名图。对低风险组和高风险组的肿瘤微环境和检查点差异进行了比较。还研究了这些特征与 BC 患者治疗反应之间的相关性。最后,还进行了功能实验进行验证。结果设计出了一个由九个CSRL组成的特征,该特征显示了对BC患者的良好预后能力。功能富集分析表明,肿瘤和免疫相关通路主要被富集。与低风险组相比,高风险组更能从免疫疗法和某些化疗药物中获益。9个CSRLs的表达在不同亚型的BC细胞系和组织中通过体外实验得到了验证。AC098484.1 与衰老相关的分泌表型的关联得到了特别验证。结论CSRLs特征是一种很有前景的BC预后生物标志物,对免疫学研究和治疗策略具有重要意义。AC098484.1 在治疗 BC 细胞衰老方面具有潜在的相关性,这些发现提高了 BC 患者的临床治疗水平。