Flavopiridol enhances the effect of docetaxel in Vitro and in Vivo in human gastric cancer cells Journal Article

  


Authors: Motwani, M.; Rizzo, C.; Sirotnak, F.; She, Y.; Schwartz, G. K.
Article Title: Flavopiridol enhances the effect of docetaxel in Vitro and in Vivo in human gastric cancer cells
Abstract: Gastric cancer is one of the leading causes of cancer death throughout the world. It is a disease in desperate need of new therapeutic approaches. Docetaxel, a semisynthetic taxane, has shown potent activity against a broad range of solid tumors. However, in gastric cancer, response rates to docetaxel remain only ∼20%. In these studies we show that flavopiridol, a cyclin-dependent kinase inhibitor, potentiates docetaxel-induced apoptosis 3-fold in MKN-74 human gastric cells. This effect is sequence dependent, such that flavopiridol must follow docetaxel to induce this effect. Docetaxel induces transient arrest in the M phase of the cell cycle. Cells exit mitosis in a specific time window without cytokinesis with a decrease in cyclin B1/cdc-2 kinase activity and MPM-2 labeling. Flavopiridol treatment of docetaxel-treated cells enhances the exit from mitosis with a more rapid decrease in mitotic markers including MPM-2 labeling and cyclin B1/cdc2 kinase activity. In contrast, pretreatment with flavopiridol prevents cells from entering mitosis by inhibiting cyclin B1/cdc-2 kinase activity, thus antagonizing the docetaxel effect. The testing of this combination against MKN-74 xenografts confirms the sequence dependency. Treatment of MKN-74 tumor-bearing xenografts with docetaxel at a dose of 10 mg/kg followed 3-7 h later by flavopiridol at a dose of 2.5 mg/kg resulted in a 1-18% decrease in tumor volume. In contrast, treatment with docetaxel alone at this same dose resulted in a 394% increase in tumor volume. When flavopiridol was given immediately after docetaxel, the effect was not statistically different from that of docetaxel alone. The reverse combination of flavopiridol followed 7 h later by docetaxel was similar to treatment with docetaxel alone. Flavopiridol alone had no effect in this tumor model. Thus, flavopiridol, when combined with docetaxel in a sequence-specific manner, may provide a completely new therapeutic approach in the treatment of gastric cancer. © 2003 American Association for Cancer Research.
Keywords: drug potentiation; antineoplastic agents; flow cytometry; antineoplastic agent; mitosis; metabolism; cell cycle; apoptosis; antineoplastic agents, phytogenic; in vitro study; enzyme inhibitor; cell line, tumor; time; time factors; docetaxel; drug synergism; drug antagonism; enzyme inhibitors; tumor cell line; immunoblotting; flavonoid; flavonoids; flavopiridol; piperidines; taxoids; cyclin b1; neoplasm transplantation; cyclin b; retinoblastoma protein; stomach neoplasms; stomach tumor; taxoid; cyclin dependent kinase 1; cancer transplantation; propidium iodide; piperidine derivative; cdc2 protein kinase; humans; human; article; propidium
Journal Title: Molecular Cancer Therapeutics
Volume: 2
Issue: 6
ISSN: 1535-7163
Publisher: American Association for Cancer Research  
Date Published: 2003-06-01
Start Page: 549
End Page: 555
Language: English
PUBMED: 12813134
PROVIDER: scopus
DOI/URL:

http://www.scopus.com/inward/record.url?eid=2-s2.0-0348075994&partnerID=40&md5=fdeda7f91dfef77bdc87b94c5da47a18
Notes: Export Date: 12 September 2014 -- Source: Scopus
Citation Impact
What is Dimensions Citation Badge?
MSK Authors
  1. Gary Schwartz
    385 Schwartz
  2. Monica V Motwani
    36 Motwani
  3. Yuhong She
    31 She
  4. Francis M Sirotnak
    184 Sirotnak
  5. Carina Rizzo
    1 Rizzo
Related MSK Work