m6A-related lncRNA-based immune infiltration characteristic analysis and prognostic model for colonic adenocarcinoma.

IF 2.7 3区生物学

Hereditas Pub Date : 2023-02-09 DOI:10.1186/s41065-023-00267-y

Hao-Lun Wang, Zhuo-Miao Ye, Zi-Yun He, Lu Huang, Zhi-Hui Liu

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引用次数: 0

Abstract

Background: Colonic adenocarcinoma (COAD) is a common gastrointestinal tract tumor, and its occurrence and progression are typically associated with genomic instability, tumor-suppressor gene and oncogene mutations, and tumor mutational load. N6-methyladenosine (m⁶A) modification of RNAs and long non-coding RNA (lncRNA) expression are important in tumorigenesis and progression. However, the regulatory roles of m⁶A-associated lncRNAs in the tumor microenvironment, stratification of prognosis, and immunotherapy are unclear.

Methods: We screened 43 prognostic lncRNAs linked to m⁶A and performed consistent molecular typing of COAD using consensus clustering. The single-sample Gene Set Enrichment Analysis and ESTIMATE algorithms were used to assess the immune characteristics of different subgroups. Covariation between methylation-related prognostic lncRNAs was eliminated by least absolute shrinkage and selection operator Cox regression. A nomogram was created and evaluated by combining the methylation-related prognostic lncRNA model with other clinical factors. The relationship between the prognostic model grouping and microsatellite instability, immunophenotype score, and tumor mutation burden was validated using R scripts. Finally, we used a linkage map to filter sensitive medicines to suppress the expression of high-risk genes. Three m⁶A-associated lncRNA modes were identified in 446 COAD specimens with different clinical endpoints and biological statuses. Risk scores were constructed based on the m⁶A-associated lncRNA signature genes. Patients with lower risk scores showed superior immunotherapy responses and clinical benefits compared to those with higher risk scores. Lower risk scores were also correlated with higher immunophenotype scores, tumor mutation burden, and mutation rates in significantly mutated genes (e.g., FAT4 and MUC16). Piperidolate, quinostatin, and mecamylamin were screened for their abilities to suppress the expression of high-risk genes in the model.

Conclusions: Quantitative assessment of m⁶A-associated lncRNAs in single tumors can enhance the understanding of tumor microenvironment profiles. The prognostic model constructed using m⁶A-associated lncRNAs may facilitate prognosis and immunotherapy stratification of patients with COAD; finally, three drugs with potential therapeutic value were screened based on the model.

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基于m6a相关lncrna的结肠腺癌免疫浸润特征分析及预后模型

背景:结肠腺癌(Colonic adenocaroma, COAD)是一种常见的胃肠道肿瘤，其发生和进展通常与基因组不稳定性、肿瘤抑制基因和癌基因突变以及肿瘤突变负荷有关。n6 -甲基腺苷(m6A)修饰RNA和长链非编码RNA (lncRNA)表达在肿瘤发生和发展中起重要作用。然而，m6a相关lncrna在肿瘤微环境、预后分层和免疫治疗中的调节作用尚不清楚。方法:我们筛选了43个与m6A相关的预后lncrna，并使用共识聚类对COAD进行了一致的分子分型。采用单样本基因集富集分析和ESTIMATE算法评估不同亚群的免疫特性。通过最小绝对收缩和选择算子Cox回归消除了甲基化相关预后lncrna之间的协变。通过将甲基化相关预后lncRNA模型与其他临床因素相结合，创建并评估了nomogram。使用R脚本验证预后模型分组与微卫星不稳定性、免疫表型评分和肿瘤突变负担之间的关系。最后，我们使用连锁图谱筛选敏感药物来抑制高危基因的表达。在446例不同临床终点和生物学状态的COAD标本中鉴定出三种m6a相关的lncRNA模式。基于m6a相关的lncRNA特征基因构建风险评分。与风险评分较高的患者相比，风险评分较低的患者表现出更好的免疫治疗反应和临床获益。较低的风险评分也与较高的免疫表型评分、肿瘤突变负担和显著突变基因(如FAT4和MUC16)的突变率相关。在模型中筛选哌啶酸酯、喹诺他汀和甲amylamin抑制高危基因表达的能力。结论:定量评估单个肿瘤中m6a相关lncrna可以增强对肿瘤微环境谱的认识。m6a相关lncrna构建的预后模型有助于COAD患者的预后和免疫治疗分层;最后，根据模型筛选出3种具有潜在治疗价值的药物。

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来源期刊

Hereditas Biochemistry, Genetics and Molecular Biology-Genetics

CiteScore

3.80

自引率

3.70%

发文量

期刊介绍： For almost a century, Hereditas has published original cutting-edge research and reviews. As the Official journal of the Mendelian Society of Lund, the journal welcomes research from across all areas of genetics and genomics. Topics of interest include human and medical genetics, animal and plant genetics, microbial genetics, agriculture and bioinformatics.