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ABSTRACT
Introduction: MicroRNAs (miRNAs) are key non-coding RNA post-transcriptional regulators of messenger RNAs (mRNAs), and are deeply dysregulated in human cancer. A rising body of evidence indicates that miRNAs represent valuable therapeutic targets. In this light, the cluster miR-221/222 are of particular relevance, given that they are strongly upregulated in a variety of solid and hematologic malignancies.
Area covered: This review summarizes recent findings on the roles played by miR-221/222 in human cancer and their potential clinical value as promising targets for therapeutic studies.
Expert opinion: The rising body of advanced preclinical evidence on the biological significance of miR-221/222 in a variety of malignancies indicates that they will play a crucial role in the future of innovative therapeutic strategies, both as validated biomarkers and targets.
Article highlights
MicroRNAs (miRNAs) are non-coding RNAs, key post-transcriptional regulators of messenger RNAs, and deeply dysregulated in human cancer.
Dysregulated miRNAs may provide novel and valuable therapeutic targets.
miR-221/222 are of relevant interest since they are strongly upregulated in a variety of solid and hematologic malignancies.
The wide biological relevance of miR-221/222 in human cancer and their potential clinical value make them promising targets for therapeutic studies.
A growing body of evidence indicates that miR-221/222 inhibitors exert antitumor activity against different malignancies and overcome resistance to cytotoxic agents.
Promising results on circulating miR-221/222 point further investigation for diagnostic and predictive purposes.
All the reported findings strongly support the role of miR-221/222 as a promising target for innovative therapeutics and at the same time as a promising biomarker for precision medicine approaches in cancer management.
This box summarizes key points contained in the article.
Declaration of interest
This paper was supported with funding from the AIRC (the Italian Association for Cancer Research, a non profit organization, PI: PT. ‘Special Program Molecular Clinical Oncology - 5 per mille’ n. 9980, 2010/15). The authors have no other relevant affiliations or financial involvement with any organization or entity with a financial interest in or financial conflict with the subject matter or materials discussed in the manuscript apart from those disclosed.