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T. Macarulla, A. Cervantes, E. Elez, E. Rodriguez-Braun, J. Baselga, S. Roselló, G. Sala, I. Blasco, H. Danaee, Y. Lee, J. Ecsedy, V. Shinde, A. Chakravarty, D. Bowman, H. Liu, O. Eton, H. Fingert and J. Tabernero, “Phase I Study of the Selective Aurora A Kinase Inhibitor MLN- 8054 in Patients with Advanced Solid Tumors: Safety, Pharmacokinetics, and Pharmacodynamics,” Molecular Cancer Therapeutics, Vol. 9, No. 10, 2010, pp. 2844- 2852. doi:10.1158/1535-7163.MCT-10-0299
has been cited by the following article:
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TITLE:
Evaluation of the Aurora Kinase Inhibitor, ZM447439, in Canine Malignant Lymphoid Cells in Vitro
AUTHORS:
Keijiro Shiomitsu, Xueqing Xia, Kyle Waite, Inder Sehgal, Shulin Li
KEYWORDS:
Aurora Kinase Inhibitor; Canine Malignant Lymphoid Cells; Cell Cycle; Apoptosis; ZM447439
JOURNAL NAME:
Open Journal of Veterinary Medicine,
Vol.3 No.1,
March
21,
2013
ABSTRACT:
Aurora kinases play an important role in the cell cycle. These enzymes help establish mitotic spindles by directing centrosome duplication and separation and by regulating the spindle assembly checkpoint thereby helping control cytokinesis. An over-expression of aurora kinases has been reported in a variety of human tumors. In this study, we identified the expression of aurora-A and aurora-B kinases in canine malignant lymphoid cells. We also evaluated the effects of the aurora kinase inhibitor (ZM447439), and found that this inhibitor decreases cell viability, increases DNA content change, and leads to apoptosis in canine B- and T-cell lymphoid cell lines. The lymphotoxicity induced by ZM447439 in these canine lymphoid cell lines suggests that further in vivo evaluation of aurora kinase inhibitors as a potential treatment for canine malignant lymphoid tumors is warranted.
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