Identifying Factors Associated with the Direction and Significance of MicroRNA Tumor-normal Expression Differences in Colorectal Cancer

Overview

Journal BMC Cancer

Publisher Biomed Central

Specialty Oncology

Date 2017 Nov 1

PMID 29084506

Citations 4

Authors

John R Stevens

Jennifer S Herrick

Roger K Wolff

Martha L Slattery

Affiliations

Soon will be listed here.

Abstract

Background: microRNAs are small non-protein-coding RNA molecules that regulate gene expression, and have a potential epigenetic role in disease progression and survival of colorectal cancer. In terms of tumor-normal expression differences, many microRNAs exhibit evidence of being up-regulated in some subjects but down-regulated in others, or are dysregulated only for a subset of the population. We present and implement an approach to identify factors (lifestyle, tumor molecular phenotype, and survival-related) that are associated with the direction and/or significance of these microRNAs' tumor-normal expression differences in colorectal cancer.

Methods: Using expression data for 1394 microRNAs and 1836 colorectal cancer subjects (each with both tumor and normal samples), we perform a dip test to identify microRNAs with multimodal distributions of tumor-normal expression differences. For proximal, distal, and rectal tumor sites separately, these microRNAs are tested for tumor-normal differential expression using a signed rank test, both overall and within levels of each lifestyle, tumor molecular phenotype, and survival-related factor. Appropriate adjustments are made to control the overall FDR.

Results: We identify hundreds of microRNAs whose direction and/or significance of tumor-normal differential expression is associated with one or more lifestyle, tumor molecular phenotype, or survival-related factors.

Conclusions: The results of this study demonstrate the benefit to colorectal cancer researchers to consider multiple subject-level factors when studying dysregulation of microRNAs, whose tumor-related changes in expression can be associated with multiple factors. Our results will serve as a publicly-available resource to provide clarifying information about various factors associated with the direction and significance of tumor-normal differential expression of microRNAs in colorectal cancer.

Citing Articles

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The Differential DNA Hypermethylation Patterns of microRNA-137 and microRNA-342 Locus in Early Colorectal Lesions and Tumours.

Kashani E, Hadizadeh M, Chaleshi V, Mirfakhraie R, Young C, Savabkar S Biomolecules. 2019; 9(10).

PMID: 31546665 PMC: 6843302. DOI: 10.3390/biom9100519.

The functional role of miRNAs in colorectal cancer: insights from a large population-based study.

Mullany L, Slattery M Cancer Biol Med. 2019; 16(2):211-219.

PMID: 31516743 PMC: 6713639. DOI: 10.20892/j.issn.2095-3941.2018.0514.

Power in pairs: assessing the statistical value of paired samples in tests for differential expression.

Stevens J, Herrick J, Wolff R, Slattery M BMC Genomics. 2018; 19(1):953.

PMID: 30572829 PMC: 6302489. DOI: 10.1186/s12864-018-5236-2.

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