Aurora B Overexpression Causes Aneuploidy and p21Cip1 Repression during Tumor Development |
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| Authors: | Alejandra González-Loyola Gonzalo Fernández-Miranda Marianna Trakala David Partida Kumiko Samejima Hiromi Ogawa Marta Ca?amero Alba de Martino ángel Martínez-Ramírez Guillermo de Cárcer Ignacio Pérez de Castro William C Earnshaw Marcos Malumbres |
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| Institution: | aCell Division and Cancer Group, Spanish National Cancer Research Center, Madrid, Spain;bWellcome Trust Centre for Cell Biology, University of Edinburgh, Edinburgh, United Kingdom;cHistopathology Unit, Spanish National Cancer Research Center, Madrid, Spain;dCytogenetics Unit, M. D. Anderson Hospital, Madrid, Spain |
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| Abstract: | Aurora kinase B, one of the three members of the mammalian Aurora kinase family, is the catalytic component of the chromosomal passenger complex, an essential regulator of chromosome segregation in mitosis. Aurora B is overexpressed in human tumors although whether this kinase may function as an oncogene in vivo is not established. Here, we report a new mouse model in which expression of the endogenous Aurkb locus can be induced in vitro and in vivo. Overexpression of Aurora B in cultured cells induces defective chromosome segregation and aneuploidy. Long-term overexpression of Aurora B in vivo results in aneuploidy and the development of multiple spontaneous tumors in adult mice, including a high incidence of lymphomas. Overexpression of Aurora B also results in a reduced DNA damage response and decreased levels of the p53 target p21Cip1
in vitro and in vivo, in line with an inverse correlation between Aurora B and p21Cip1 expression in human leukemias. Thus, overexpression of Aurora B may contribute to tumor formation not only by inducing chromosomal instability but also by suppressing the function of the cell cycle inhibitor p21Cip1. |
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