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Reference - PMID:25669599 - Fitness profiling links topoisomerase II regulation of centromeric integrity to doxorubicin resistance in fission yeast.

Reference summary

PubMed ID
PMID:25669599
Title
Fitness profiling links topoisomerase II regulation of centromeric integrity to doxorubicin resistance in fission yeast.
Authors
Nguyen TT, Lim JS, Tang RM, Zhang L, Chen ES
Citation
Sci Rep 2015 Feb 11;5:8400
Publication year
2015
Abstract
Doxorubicin, a chemotherapeutic agent, inhibits the religation step of topoisomerase II (Top2). However, the downstream ramifications of this action are unknown. Here we performed epistasis analyses of top2 with 63 genes representing doxorubicin resistance (DXR) genes in fission yeast and revealed a subset that synergistically collaborate with Top2 to confer DXR. Our findings show that the chromatin-regulating RSC and SAGA complexes act with Top2 in a cluster that is functionally distinct from the Ino80 complex. In various DXR mutants, doxorubicin hypersensitivity was unexpectedly suppressed by a concomitant top2 mutation. Several DXR proteins showed centromeric localization, and their disruption resulted in centromeric defects and chromosome missegregation. An additional top2 mutation could restore centromeric chromatin integrity, suggesting a counterbalance between Top2 and these DXR factors in conferring doxorubicin resistance. Overall, this molecular basis for mitotic catastrophe associated with doxorubicin treatment will help to facilitate drug combinatorial usage in doxorubicin-related chemotherapeutic regimens.

Annotation

Multi-locus phenotype

FYPO:0003559 - sensitive to doxorubicin

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Single locus phenotype

FYPO:0003165 - cut with abnormal chromosome segregation

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FYPO:0001407 - decreased cell population growth on glucose carbon source

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FYPO:0000284 - large and small daughter nuclei, with unequal mitotic sister chromatid segregation

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FYPO:0001387 - loss of viability at high temperature

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FYPO:0005228 - normal growth on doxorubicin

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FYPO:0003559 - sensitive to doxorubicin

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