Loss of spindle assembly checkpoint-mediated inhibition of Cdc20 promotes tumorigenesis in mice

doi:10.1083/jcb.200904020

A correction to this article has been published: Li et al., J. Cell Biol. 186 (1) 161
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doi:10.1083/jcb.200904020
The Journal of Cell Biology, Vol. 185, No. 6, 983-994
The Rockefeller University Press, 0021-9525 $30.00
© Li et al.

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Loss of spindle assembly checkpoint–mediated inhibition of Cdc20 promotes tumorigenesis in mice

Min Li¹, Xiao Fang¹, Zhubo Wei¹, J. Philippe York¹, and Pumin Zhang¹^,2

¹ Department of Molecular Physiology and Biophysics and ² Department of Biochemistry and Molecular Biology, Baylor College of Medicine, Houston, TX 77030

Correspondence to Pumin Zhang: pzhang{at}bcm.tmc.edu

Genomic instability is a hallmark of human cancers. Spindleassembly checkpoint (SAC) is a critical cellular mechanism thatprevents chromosome missegregation and therefore aneuploidyby blocking premature separation of sister chromatids. Thus,SAC, much like the DNA damage checkpoint, is essential for genomestability. In this study, we report the generation and analysisof mice carrying a Cdc20 allele in which three residues criticalfor the interaction with Mad2 were mutated to alanine. The mutantCdc20 protein (AAA-Cdc20) is no longer inhibited by Mad2 inresponse to SAC activation, leading to the dysfunction of SACand aneuploidy. The dysfunction could not be rescued by theadditional expression of another Cdc20 inhibitor, BubR1. Furthermore,we found that Cdc20^AAA/AAA mice died at late gestation, butCdc20^+/AAA mice were viable. Importantly, Cdc20^+/AAA mice developedspontaneous tumors at highly accelerated rates, indicating thatthe SAC-mediated inhibition of Cdc20 is an important tumor-suppressingmechanism.

Abbreviations used in this paper: APC/C, anaphase-promotingcomplex/cyclosome; CIN, chromosomal instability; ES, embryonicstem; iMEF, immortalized MEF; MCC, mitotic checkpoint complex;MEF, mouse embryonic fibroblast; SAC, spindle assembly checkpoint;SKY, spectrum karyotyping.

© 2009 Li et al.
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