Common and Unique microRNAs in Multiple Carcinomas Regulate Similar Network of Pathways to Mediate Cancer Progression

Divya Niveditha,Syamantak Majumder,Rajdeep Chowdhury,Shibasish Chowdhury,Mayank Jasoria,Sudeshna Mukherjee,Jayesh Narayan

doi:10.1038/s41598-020-59142-9

Divya Niveditha, Syamantak Majumder + Show 5 more

Open Access

https://doi.org/10.1038/s41598-020-59142-9

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Abstract

Cancer is a complex disease with a fatal outcome. Early detection of cancer, by monitoring appropriate molecular markers is very important for its therapeutic management. In this regard, the short non-coding RNA molecules, microRNAs (miRNAs) have shown great promise due to their availability in circulating fluids facilitating non-invasive detection of cancer. In this study, an in silico comparative analysis was performed to identify specific signature miRNAs dysregulated across multiple carcinomas and simultaneously identify unique miRNAs for each cancer type as well. The miRNA-seq data of cancer patient was obtained from GDC portal and their differential expressions along with the pathways regulated by both common and unique miRNAs were analyzed. Our studies show twelve miRNAs commonly dysregulated across seven different cancer types. Interestingly, four of those miRNAs (hsa-mir-210, hsa-mir-19a, hsa-mir-7 and hsa-mir-3662) are already reported as circulatory miRNAs (circRNAs); while, the miR-183 cluster along with hsa-mir-93 have been found to be incorporated in exosomes signifying the importance of the identified miRNAs for their use as prospective, non-invasive biomarkers. Further, the target mRNAs and pathways regulated by both common and unique miRNAs were analyzed, which interestingly had significant commonality. This suggests that miRNAs that are commonly de-regulated and specifically altered in multiple cancers might regulate similar pathways to promote cancer. Our data is of significance because we not only identify a set of common and unique miRNAs for multiple cancers but also highlight the pathways regulated by them, which might facilitate the development of future non-invasive biomarkers conducive for early detection of cancers.

Highlights

Cancer has the highest rate in disease-associated deaths worldwide, making it a major public health concern
To study the specific role of microRNAs in the seven different cancer types we obtained their miRNA-Seq data from Genomic Data Commons (GDC) portal
This approach resulted in the identification of 12 miRNAs, which are common among the seven cancer types as well as unique miRNAs, which are specific to each cancer (Fig. 1B)

Summary

Introduction

Cancer has the highest rate in disease-associated deaths worldwide, making it a major public health concern. Even today, the current gold standard for diagnosis of the majority of cancers is histological examination, obtained by radiologically guided biopsy or surgical excision These procedures are moderately inaccurate, invasive, expensive, and not without the risk to the patient. There have been a plethora of publications reporting much exquisite molecular information specific to early detection of cancer cells and usage of biomarkers for screening malignancy and recurrence[1,2,3,4] These markers could be amino acids such as Valine, Leucine and Isoleucine as in case of pancreatic cancers[5], proteins like the CA-125 which are involved in ovarian cancer detection[6], tumour suppressors like. These public portals with miRNA expression data from patients across the globe have been absolutely under-utilized, which demands further analysis followed by experimentation to confirm the role of miRNAs in cancer

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