Mature microRNA-binding protein QKI promotes microRNA-mediated gene silencing

Author:

Min Kyung-Won,Jo Myung Hyun,Song Minsuk,Ko Seungbeom,Lee Ji Won,Shim Min Ji,Kim Kyungmin,Park Hyun Bong,Ha Shinwon,Mun Hyejin,Polash Ahsan,Hafner MarkusORCID,Cho Jung-Hyun,Kim Dong-San,Hohng Sungchul,Kang Sung-Ung,Yoon Je-HyunORCID

Abstract

ABSTRACTAlthough Argonaute (AGO) proteins have been the focus of microRNA (miRNA) studies, we observed AGO-free mature miRNAs directly interacting with RNA-binding proteins, implying the sophisticated nature of fine-tuning gene regulation by miRNAs. To investigate microRNA-binding proteins (miRBPs) globally, we analyzed PAR-CLIP data sets to identify RBP quaking (QKI) as a novel miRBP for let-7b. Potential existence of AGO-free miRNAs were further verified in genetically engineered AGO-depleted human and mouse cells. We have shown that QKI serves as an auxiliary factor empowering AGO2/let-7b-mediated gene silencing. Depletion of QKI decreases interaction of AGO2 with let-7b and target mRNA, consequently controlling target mRNA decay. QKI, however, also suppresses the dissociation of let-7b from AGO2, and slows assembly of AGO2/miRNA/target mRNA complexes at the single-molecule level. We also revealed that QKI suppresses cMYC expression at post-transcriptional level, and decreases proliferation and migration of HeLa cells, demonstrating that QKI is a tumor suppressor gene by in part augmenting let-7b activity. Our data show that QKI is a new type of RBP implicated in the versatile regulation of miRNA-mediated gene silencing.

Publisher

Cold Spring Harbor Laboratory

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