RNA and DNA G-quadruplexes bind to human dicer and inhibit its activity.
Natalia KoralewskaAgnieszka SzczepanskaKinga CiechanowskaMarta WojnickaMaria PokornowskaMarek C MilewskiDorota GudanisDaniel BaranowskiChandran NithinJanusz M BujnickiZofia GdaniecMarek FiglerowiczAnna Kurzynska-KokorniakPublished in: Cellular and molecular life sciences : CMLS (2021)
Guanine (G)-rich single-stranded nucleic acids can adopt G-quadruplex structures. Accumulating evidence indicates that G-quadruplexes serve important regulatory roles in fundamental biological processes such as DNA replication, transcription, and translation, while aberrant G-quadruplex formation is linked to genome instability and cancer. Understanding the biological functions played by G-quadruplexes requires detailed knowledge of their protein interactome. Here, we report that both RNA and DNA G-quadruplexes are bound by human Dicer in vitro. Using in vitro binding assays, mutation studies, and computational modeling we demonstrate that G-quadruplexes can interact with the Platform-PAZ-Connector helix cassette of Dicer, the region responsible for anchoring microRNA precursors (pre-miRNAs). Consequently, we show that G-quadruplexes efficiently and stably inhibit the cleavage of pre-miRNA by Dicer. Our data highlight the potential of human Dicer for binding of G-quadruplexes and allow us to propose a G-quadruplex-driven sequestration mechanism of Dicer regulation.