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用于预测结肠癌转移的微小RNA分类器和列线图

MicroRNA classifier and nomogram for metastasis prediction in colon cancer.

作者信息

Goossens-Beumer Inès J, Derr Remco S, Buermans Henk P J, Goeman Jelle J, Böhringer Stefan, Morreau Hans, Nitsche Ulrich, Janssen Klaus-Peter, van de Velde Cornelis J H, Kuppen Peter J K

机构信息

Department of Surgery, Leiden University Medical Center, Leiden, the Netherlands.

Department of Human Genetics/Leiden Genome Technology Center, Leiden University Medical Center, Leiden, the Netherlands.

出版信息

Cancer Epidemiol Biomarkers Prev. 2015 Jan;24(1):187-97. doi: 10.1158/1055-9965.EPI-14-0544-T. Epub 2014 Oct 14.

Abstract

BACKGROUND

Colon cancer prognosis and treatment are currently based on a classification system still showing large heterogeneity in clinical outcome, especially in TNM stages II and III. Prognostic biomarkers for metastasis risk are warranted as development of distant recurrent disease mainly accounts for the high lethality rates of colon cancer. miRNAs have been proposed as potential biomarkers for cancer. Furthermore, a verified standard for normalization of the amount of input material in PCR-based relative quantification of miRNA expression is lacking.

METHODS

A selection of frozen tumor specimens from two independent patient cohorts with TNM stage II-III microsatellite stable primary adenocarcinomas was used for laser capture microdissection. Next-generation sequencing was performed on small RNAs isolated from colorectal tumors from the Dutch cohort (N = 50). Differential expression analysis, comparing in metastasized and nonmetastasized tumors, identified prognostic miRNAs. Validation was performed on colon tumors from the German cohort (N = 43) using quantitative PCR (qPCR).

RESULTS

miR25-3p and miR339-5p were identified and validated as independent prognostic markers and used to construct a multivariate nomogram for metastasis risk prediction. The nomogram showed good probability prediction in validation. In addition, we recommend combination of miR16-5p and miR26a-5p as standard for normalization in qPCR of colon cancer tissue-derived miRNA expression.

CONCLUSIONS

In this international study, we identified and validated a miRNA classifier in primary cancers, and propose a nomogram capable of predicting metastasis risk in microsatellite stable TNM stage II-III colon cancer.

IMPACT

In conjunction with TNM staging, by means of a nomogram, this miRNA classifier may allow for personalized treatment decisions based on individual tumor characteristics.

摘要

背景

目前结肠癌的预后和治疗基于一种分类系统,该系统在临床结果上仍显示出很大的异质性,尤其是在TNM分期的II期和III期。由于远处复发性疾病的发生是导致结肠癌高致死率的主要原因,因此转移风险的预后生物标志物很有必要。miRNA已被提议作为癌症的潜在生物标志物。此外,在基于PCR的miRNA表达相对定量中,缺乏用于标准化输入材料量的经过验证的标准。

方法

从两个独立的患者队列中选取TNM分期为II - III期的微卫星稳定原发性腺癌的冷冻肿瘤标本,用于激光捕获显微切割。对从荷兰队列(N = 50)的结直肠癌中分离出的小RNA进行下一代测序。通过比较转移和未转移肿瘤的差异表达分析,确定预后性miRNA。使用定量PCR(qPCR)在德国队列(N = 43)的结肠肿瘤上进行验证。

结果

miR25 - 3p和miR339 - 5p被鉴定并验证为独立的预后标志物,并用于构建转移风险预测的多变量列线图。该列线图在验证中显示出良好的概率预测能力。此外,我们建议将miR16 - 5p和miR26a - 5p的组合作为结肠癌组织来源miRNA表达qPCR标准化的标准。

结论

在这项国际研究中,我们在原发性癌症中鉴定并验证了一种miRNA分类器,并提出了一种能够预测微卫星稳定的TNM II - III期结肠癌转移风险的列线图。

影响

结合TNM分期,通过列线图,这种miRNA分类器可以根据个体肿瘤特征做出个性化的治疗决策。

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