Rae1 is an essential mitotic checkpoint regulator that cooperates with Bub3 to prevent chromosome missegregation
JR Babu, KB Jeganathan, DJ Baker, X Wu… - Journal of Cell …, 2003 - rupress.org
JR Babu, KB Jeganathan, DJ Baker, X Wu, N Kang-Decker, JM Van Deursen
Journal of Cell Biology, 2003•rupress.orgT cells from these mice did not have a detectable defect in nuclear export of mRNA. Unlike
null mice, compound haplo-insufficient Rae1/Bub3 mice are viable. However, cells from
these mice exhibit much greater rates of premature sister chromatid separation and
chromosome missegregation than single haplo-insufficient cells. Finally, we show that mice
with mitotic checkpoint defects are more susceptible to dimethylbenzanthrene-induced
tumorigenesis than wild-type mice. Thus, our data demonstrate a novel function for Rae1 …
null mice, compound haplo-insufficient Rae1/Bub3 mice are viable. However, cells from
these mice exhibit much greater rates of premature sister chromatid separation and
chromosome missegregation than single haplo-insufficient cells. Finally, we show that mice
with mitotic checkpoint defects are more susceptible to dimethylbenzanthrene-induced
tumorigenesis than wild-type mice. Thus, our data demonstrate a novel function for Rae1 …
T cells from these mice did not have a detectable defect in nuclear export of mRNA. Unlike null mice, compound haplo-insufficient Rae1/Bub3 mice are viable. However, cells from these mice exhibit much greater rates of premature sister chromatid separation and chromosome missegregation than single haplo-insufficient cells. Finally, we show that mice with mitotic checkpoint defects are more susceptible to dimethylbenzanthrene-induced tumorigenesis than wild-type mice. Thus, our data demonstrate a novel function for Rae1 and characterize Rae1 and Bub3 as related proteins with essential, overlapping, and cooperating roles in the mitotic checkpoint.
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