Oncogenic Biogenesis of Pri-miR-17∼92 Reveals Hierarchy and Competition Among Polycistronic MicroRNAs

Overview

Journal Mol Cell

Publisher Cell Press

Specialty Cell Biology

Date 2019 Jun 30

PMID 31253575

Citations 20

Authors

Ariel O Donayo

Radia M Johnson

Hsin-Wei Tseng

Said Izreig

Alexandra Gariepy

Vinay K Mayya

Edlyn Wu

Roshni Alam

Carine Lussier

Russell G Jones

Thomas F Duchaine

Affiliations

Soon will be listed here.

Abstract

The microRNAs encoded by the miR-17∼92 polycistron are commonly overexpressed in cancer and orchestrate a wide range of oncogenic functions. Here, we identify a mechanism for miR-17∼92 oncogenic function through the disruption of endogenous microRNA (miRNA) processing. We show that, upon oncogenic overexpression of the miR-17∼92 primary transcript (pri-miR-17∼92), the microprocessor complex remains associated with partially processed intermediates that aberrantly accumulate. These intermediates reflect a series of hierarchical and conserved steps in the early processing of the pri-miR-17∼92 transcript. Encumbrance of the microprocessor by miR-17∼92 intermediates leads to the broad but selective downregulation of co-expressed polycistronic miRNAs, including miRNAs derived from tumor-suppressive miR-34b/c and from the Dlk1-Dio3 polycistrons. We propose that the identified steps of polycistronic miR-17∼92 biogenesis contribute to the oncogenic re-wiring of gene regulation networks. Our results reveal previously unappreciated functional paradigms for polycistronic miRNAs in cancer.

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