Journal
CELL CYCLE
Volume 8, Issue 8, Pages 1206-1216Publisher
TAYLOR & FRANCIS INC
DOI: 10.4161/cc.8.8.8205
Keywords
CDK5RAP2; primary microcephaly; spindle checkpoint; BUBR1; MAD2; drug resistance; paclitaxel; doxorubicin
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Funding
- CNU, NSFC funds [30570371, 90608014, 30711120570, 30700420]
- New Century Excellent Talents in University [06-0187]
- Beijing Natural Science Foundation Program and Scientific Research Key Program of Beijing Municipal Commission of Education [KZ200810028014]
- Academic Human Resources Development in Institutions of Higher Learning Under the Jurisdiction of Beijing Municipality
- National Institutes of Health [R01CA88873]
- Beijing Nova Program [2007B062]
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The combination of paclitaxel and doxorubicin is among the most successful chemotherapy regimens in cancer treatment. CDK5RAP2, when mutated, causes primary microcephaly. We show here that inhibition of CDK5RAP2 expression causes chromosome mis-segregation, fails to maintain the spindle checkpoint, and is associated with reduced expression of the spindle checkpoint proteins BUBR1 and MAD2 and an increase in chromatin-associated CDC20. CDK5RAP2 resides on the BUBR1 and MAD2 promoters and regulates their transcription. Furthermore, CDK5RAP2-knockdown cells have increased resistance to paclitaxel and doxorubicin, and this resistance is partially rescued upon restoration of CDK5RAP2 expression. Cancer cells cultured in the presence of paclitaxel or doxorubicin exhibit dramatically decreased CDK5RAP2 levels. These results suggest that CDK5RAP2 is required for spindle checkpoint function and is a common target in paclitaxel and doxorubicin resistance.
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