Identification of Cytoskeleton-Associated Proteins Essential for Lysosomal Stability and Survival of Human Cancer Cells

被引:60
|
作者
Groth-Pedersen, Line [1 ]
Aits, Sonja [1 ]
Corcelle-Termeau, Elisabeth [1 ]
Petersen, Nikolaj H. T. [1 ]
Nylandsted, Jesper [1 ]
Jaattela, Marja [1 ]
机构
[1] Danish Canc Soc Res Ctr, Ctr Genotox Stress Res, Copenhagen, Denmark
来源
PLOS ONE | 2012年 / 7卷 / 10期
基金
英国医学研究理事会; 新加坡国家研究基金会;
关键词
KINESIN-LIKE PROTEIN; MYOSIN-I-ALPHA; PLASMA-MEMBRANE; DOWN-REGULATION; MOTOR PROTEINS; DEATH; PATHWAY; ENDOSOMES; GROWTH; MACROAUTOPHAGY;
D O I
10.1371/journal.pone.0045381
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Microtubule-disturbing drugs inhibit lysosomal trafficking and induce lysosomal membrane permeabilization followed by cathepsin-dependent cell death. To identify specific trafficking-related proteins that control cell survival and lysosomal stability, we screened a molecular motor siRNA library in human MCF7 breast cancer cells. SiRNAs targeting four kinesins (KIF11/Eg5, KIF20A, KIF21A, KIF25), myosin 1G (MYO1G), myosin heavy chain 1 (MYH1) and tropomyosin 2 (TPM2) were identified as effective inducers of non- apoptotic cell death. The cell death induced by KIF11, KIF21A, KIF25, MYH1 or TPM2 siRNAs was preceded by lysosomal membrane permeabilization, and all identified siRNAs induced several changes in the endo-lysosomal compartment, i.e. increased lysosomal volume (KIF11, KIF20A, KIF25, MYO1G, MYH1), increased cysteine cathepsin activity (KIF20A, KIF25), altered lysosomal localization (KIF25, MYH1, TPM2), increased dextran accumulation (KIF20A), or reduced autophagic flux (MYO1G, MYH1). Importantly, all seven siRNAs also killed human cervix cancer (HeLa) and osteosarcoma (U-2-OS) cells and sensitized cancer cells to other lysosome-destabilizing treatments, i.e. photo-oxidation, siramesine, etoposide or cisplatin. Similarly to KIF11 siRNA, the KIF11 inhibitor monastrol induced lysosomal membrane permeabilization and sensitized several cancer cell lines to siramesine. While KIF11 inhibitors are under clinical development as mitotic blockers, our data reveal a new function for KIF11 in controlling lysosomal stability and introduce six other molecular motors as putative cancer drug targets.
引用
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页数:11
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