Affiliation:
1. Ruđer Bošković Institute 1 Division of Molecular Medicine , , Bijenička c. 54, 10000 Zagreb , Croatia
2. GENOS, Glycoscience Research Laboratory 2 , Borongajska c. 83, 10000 Zagreb , Croatia
Abstract
ABSTRACT
Epithelial-to-mesenchymal transition (EMT) gives rise to cells with properties similar to cancer stem cells (CSCs). Targeting the EMT program to selectively eliminate CSCs is a promising way to improve cancer therapy. Salinomycin (Sal), a K+/H+ ionophore, was identified as highly selective towards CSC-like cells, but its mechanism of action and selectivity remains elusive. Here, we show that Sal, similar to monensin and nigericin, disturbs the function of the Golgi. Sal alters the expression of Golgi-related genes and leads to marked changes in Golgi morphology, particularly in cells that have undergone EMT. Moreover, Golgi-disturbing agents severely affect post-translational modifications of proteins, including protein processing, glycosylation and secretion. We discover that the alterations induced by Golgi-disturbing agents specifically affect the viability of EMT cells. Collectively, our work reveals a novel vulnerability related to the EMT, suggesting an important role for the Golgi in the EMT and that targeting the Golgi could represent a novel therapeutic approach against CSCs.
Funder
Hrvatska Zaklada za Znanost
Seventh Framework Programme
European Structural and Investment Funds IRI
Publisher
The Company of Biologists
Cited by
4 articles.
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