4.7 Review

MicroRNA and cyclooxygenase-2 in breast cancer

Journal

CLINICA CHIMICA ACTA
Volume 522, Issue -, Pages 36-44

Publisher

ELSEVIER
DOI: 10.1016/j.cca.2021.08.007

Keywords

breast cancer; microRNAs; cyclooxygenase-2; cyclooxygenase-2 inhibitors; therapeutic target; biomarker

Funding

  1. Clinical Medical Technol-ogy Innovation Guidance Project in Hunan Province [2018SK51702]

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Breast cancer is among the most common cancers in women worldwide, and miRNAs and COX-2 are new diagnostic and therapeutic biomarkers for monitoring BC. COX-2 is associated with tumor growth and metastasis, while MiRs show differential expression in breast tumor tissue. Understanding the pathway between miRNAs and COX-2 can lead to the development of new therapeutic approaches for BC.
Cancer remains a major public health problem worldwide and the latest statistics show that breast cancer (BC) is among the most frequent in women. MicroRNAs (miRNAs; miRs) and cyclooxygenase-2 (COX-2) are new diagnostic and therapeutic biomarkers for monitoring BC. COX-2 is a prominent tumor-associated inflammatory factor highly expressed in human tumor cells, including BC. Expression of COX-2 contributes to tumor growth, metastasis and recurrence. MiRs are a group of short (similar to 22 nucleotides), noncoding regulatory RNAs that downregulate gene expression post-transcriptionally and play vital roles in regulating cancer development and progression. Interestingly, there are a group of miRNAs differentially expressed in breast tumor tissue. Under-standing the pathway linking miRNAs to COX-2 can provide novel insight for suppressing COX-2 expression via gene silencing thereby leading to the development of selective miRNA inhibitors. Further research can also reveal key intermediate players and their potential as therapeutic targets. Given the association between different miRNAs and COX-2 expression in BC, this review presents a comprehensive overview of the current literature concerning how miRNAs and COX-2 signaling interact in BC progression.

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