Over the last decades, the rich knowledge about human diseases gained from extensive basic, preclinical, and clinical research and the rapid development of biotechnology have paved the way towards precision medicine. Different from EBM, precision medicine is a new paradigm of medicine empowered by comprehensive molecular and clinical profiling of patients.⁵ It tailors precise disease diagnosis, prognosis, and therapeutics to the individuals based on (epi-)genetic, phenotypic, and clinical characteristics and eventually aims to achieve the right treatment, to the right patient, at the right time.^5,6 Recent advances achieved in multiple related fields have collectively laid a strong foundation for the development of precision medicine in the coming decades. On the one hand, the rapid development of biotechnologies contributes significantly to reduction in the cost of high-throughput sequencing, enabling the generation of multi-omic profiles for patients on a large scale. On the other hand, the fast-growing computing power and development of analytical methods has made it possible to store, transfer, analyze, and interpret the ‘big’ biomedical data generated. More recently, artificial intelligence (AI) has demonstrated unprecedented performance in various preclinical and clinical studies,⁷ providing new opportunities to develop automated, intelligent systems in the clinic.

Among the broad spectrum of research areas in cancer precision medicine, biomarker development is a central mission. A biomarker is a biological substance that can be measured and evaluated as an indicator of normal or abnormal conditions or a sign of disease condition.⁸ It can be found in tissues, blood, or other body fluids. Molecules such as DNA, mRNA, miRNA, and proteins, as well as metabolites and microorganisms, can all be exploited as biomarkers. Numerous biomarkers have been developed for cancer screening, diagnosis, prognosis, and prediction of therapy response as well as disease monitoring. Importantly, tailored for specific clinical applications, molecular biomarkers can be customized based on a selection of different types of clinical specimens, diverse biomolecules to test, and various high- or low-throughput platforms for profiling.⁹

MicroRNAs (miRNAs) are small regulatory non-coding RNAs that can downregulate gene expression mainly via base pairing to 3′ untranslated regions of target mRNAs. These small molecules influence almost every cancer-related process involving cell proliferation, apoptosis, metastasis, and angiogenesis.^10,15 Compared to other molecules, miRNAs are relatively stable and abundant in various clinical specimens, presenting promising candidates for biomarker development. In the last decade, miRNAs have been exploited as valuable diagnostic, prognostic, and predictive biomarkers in various cancer types.¹⁶ Recently, the growing interest in ‘liquid biopsies’ has also put circulating miRNAs to the forefront of biomarker discovery and development.

In this chapter, we will first summarize miRNA-based biomarkers for various clinical applications based on a substantial literature review and discuss the potential limitations of traditional approaches. Recent years have seen large-scale cohort studies generating vast amounts of omics data, which will continue to grow exponentially in the following decades.¹⁷ These ‘big’ multi-omic datasets, together with histopathological reports and medical records, provide tremendous opportunities for biomarker discovery and in silico validations. Next, we will introduce a data-driven methodology for biomarker development and the major steps involved. Furthermore, we will summarize the major advantages of the data-driven methodology and discuss the main challenges limiting its implementation, possible solutions, and emerging opportunities.