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MED19 Promotes 2’-O-methylation of rRNA to Facilitate IRES-Dependent c-Myc Translation


ABSTRACT: The Mediator is an essential co-factor of Pol II-dependent transcription, and MED19 is a subunit of this complex. MED19 has been reported to overexpress in various cancers to promote cancer progression, although the underlying mechanism remains elusive. Here, we unexpectedly discovered that the MED19 protein can localize to the nucleolus independently of the Mediator complex. The nucleolus localization of MED19 depends on a patch of poly-lysine sequence at its C-terminus, which is important for MED19 to directly bind ribosomal RNA (rRNA) and FBL, the catalytic enzyme of 2'-O-methylation, thus promoting the 2'-O-methylation level of rRNA. Mature ribosomes with highly 2'-O-methylated rRNA can more effectively translate from the internal ribosome entry sites (IRES), while the oncogenic c-Myc contains a typical IRES-element at its 5’ UTR. We show that the knockdown of MED19 significantly reduces the protein abundance of c-Myc without affecting its mRNA level. Pan-cancer analyses further demonstrate a positive correlation between MED19 and c-Myc at the protein but not mRNA level. Collectively, our findings reveal an important role of the Mediator-independent MED19 in translational control of c-Myc, thus providing novel mechanistic insights into the c-Myc-driven tumorigenesis.

ORGANISM(S): Homo sapiens

PROVIDER: GSE282808 | GEO | 2025/11/25

REPOSITORIES: GEO

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