Construct of qualitative diagnostic biomarkers specific for glioma by pairing serum microRNAs

Hongdong Li; Liyuan Ma; Fengyuan Luo; Wenkai Liu; Na Li; Tao Hu; Haijian Zhong; You Guo; Guini Hong

doi:10.1186/s12864-023-09203-w

Construct of qualitative diagnostic biomarkers specific for glioma by pairing serum microRNAs

BMC Genomics. 2023 Mar 2;24(1):96. doi: 10.1186/s12864-023-09203-w.

Authors

Hongdong Li¹, Liyuan Ma¹, Fengyuan Luo¹, Wenkai Liu¹, Na Li¹, Tao Hu¹, Haijian Zhong¹, You Guo², Guini Hong³

Affiliations

¹ School of Medical Information Engineering, Gannan Medical University, Ganzhou, 341000, China.
² Medical Big Data and Bioinformatics Research Centre at First Affiliated Hospital of Gannan Medical University, Ganzhou, 341000, China. gy@gmu.edu.cn.
³ School of Medical Information Engineering, Gannan Medical University, Ganzhou, 341000, China. hongguini08@gmail.com.

Abstract

Background: Serum microRNAs (miRNAs) are promising non-invasive biomarkers for diagnosing glioma. However, most reported predictive models are constructed without a large enough sample size, and quantitative expression levels of their constituent serum miRNAs are susceptible to batch effects, decreasing their clinical applicability.

Methods: We propose a general method for detecting qualitative serum predictive biomarkers using a large cohort of miRNA-profiled serum samples (n = 15,460) based on the within-sample relative expression orderings of miRNAs.

Results: Two panels of miRNA pairs (miRPairs) were developed. The first was composed of five serum miRPairs (5-miRPairs), reaching 100% diagnostic accuracy in three validation sets for distinguishing glioma and non-cancer controls (n = 436: glioma = 236, non-cancers = 200). An additional validation set without glioma samples (non-cancers = 2611) showed a predictive accuracy of 95.9%. The second panel included 32 serum miRPairs (32-miRPairs), reaching 100% diagnostic performance in training set on specifically discriminating glioma from other cancer types (sensitivity = 100%, specificity = 100%, accuracy = 100%), which was reproducible in five validation datasets (n = 3387: glioma = 236, non-glioma cancers = 3151, sensitivity> 97.9%, specificity> 99.5%, accuracy> 95.7%). In other brain diseases, the 5-miRPairs classified all non-neoplastic samples as non-cancer, including stroke (n = 165), Alzheimer's disease (n = 973), and healthy samples (n = 1820), and all neoplastic samples as cancer, including meningioma (n = 16), and primary central nervous system lymphoma samples (n = 39). The 32-miRPairs predicted 82.2 and 92.3% of the two kinds of neoplastic samples as positive, respectively. Based on the Human miRNA tissue atlas database, the glioma-specific 32-miRPairs were significantly enriched in the spinal cord (p = 0.013) and brain (p = 0.015).

Conclusions: The identified 5-miRPairs and 32-miRPairs provide potential population screening and cancer-specific biomarkers for glioma clinical practice.

Keywords: Diagnostic biomarker; Glioma; Relative expression ordering; Serum microRNA.

MeSH terms

Alzheimer Disease*
Biomarkers, Tumor / genetics
Brain
Databases, Factual
Humans
MicroRNAs* / genetics

Substances

MicroRNAs
Biomarkers, Tumor