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Synergy between inhibitors of two mitotic spindle assembly motors undermines an adaptive response.

Authors :
Solon AL
Zaniewski TM
O'Brien P
Clasby M
Hancock WO
Ohi R
Source :
Molecular biology of the cell [Mol Biol Cell] 2022 Dec 01; Vol. 33 (14), pp. ar132. Date of Electronic Publication: 2022 Oct 06.
Publication Year :
2022

Abstract

Mitosis is the cellular process that ensures accurate segregation of the cell's genetic material into two daughter cells. Mitosis is often deregulated in cancer; thus drugs that target mitosis-specific proteins represent attractive targets for anticancer therapy. Numerous inhibitors have been developed against kinesin-5 Eg5, a kinesin essential for bipolar spindle assembly. Unfortunately, Eg5 inhibitors (K5Is) have been largely ineffective in the clinic, possibly due to the activity of a second kinesin, KIF15, that can suppress the cytotoxic effect of K5Is by driving spindle assembly through an Eg5-independent pathway. We hypothesized that pairing of K5Is with small molecule inhibitors of KIF15 will be more cytotoxic than either inhibitor alone. Here we present the results of a high-throughput screen from which we identified two inhibitors that inhibit the motor activity of KIF15 both in vitro and in cells. These inhibitors selectively inhibit KIF15 over other molecular motors and differentially affect the ability of KIF15 to bind microtubules. Finally, we find that chemical inhibition of KIF15 reduces the ability of cells to acquire resistance to K5Is, highlighting the centrality of KIF15 to K5I resistance and the value of these inhibitors as tools with which to study KIF15 in a physiological context.

Details

Language :
English
ISSN :
1939-4586
Volume :
33
Issue :
14
Database :
MEDLINE
Journal :
Molecular biology of the cell
Publication Type :
Academic Journal
Accession number :
36200902
Full Text :
https://doi.org/10.1091/mbc.E22-06-0225