Published 2017 | Version v1
Publication Metadata-only

SGK1 affects RAN/RANBP1/RANGAP1 via SP1 to play a critical role in pre-miRNA nuclear export: A new route of epigenomic regulation

Dattilo, Vincenzo
D'Antona, Lucia
Talarico, Cristina
Capula, Mjriam
Catalogna, Giada
Iuliano, Rodolfo
SCHENONE, SILVIA
Roperto, Sante
Bianco, Cataldo
Perrotti, Nicola
Amato, Rosario
Others:
Dattilo, Vincenzo
D'Antona, Lucia
Talarico, Cristina
Capula, Mjriam
Catalogna, Giada
Iuliano, Rodolfo
Schenone, Silvia
Roperto, Sante
Bianco, Cataldo
Perrotti, Nicola
Amato, Rosario

Description

The serum- and glucocorticoid-regulated kinase (SGK1) controls cell transformation and tumor progression. SGK1 affects mitotic stability by regulating the expression of RANBP1/RAN. Here, we demonstrate that SGK1 fluctuations indirectly modify the maturation of pre-miRNAs, by modulating the equilibrium of the RAN/RANBP1/RANGAP1 axis, the main regulator of nucleo-cytoplasmic transport. The levels of pre-miRNAs and mature miRNAs were assessed by qRT-PCR, in total extracts and after differential nuclear/cytoplasmic extraction. RANBP1 expression is the limiting step in the regulation of SGK1-SP1 dependent nuclear export. These results were validated in unrelated tumor models and primary human fibroblasts and corroborated in tumor-engrafted nude mice. The levels of pri-miRNAs, DROSHA, DICER and the compartmental distribution of XPO5 were documented. Experiments using RANGTP conformational antibodies confirmed that SGK1, through RANBP1, decreases the level of the GTP-bound state of RAN. This novel mechanism may play a role in the epigenomic regulation of cell physiology and fate.

Additional details

Identifiers Origin repository
Created:
April 14, 2023
Modified:
November 29, 2023