期刊
MOLECULAR BIOLOGY OF THE CELL
卷 20, 期 17, 页码 3818-3827出版社
AMER SOC CELL BIOLOGY
DOI: 10.1091/mbc.E09-04-0330
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资金
- National Institute of General Medical Sciences [T32 GM07270]
- National Institutes of Health [GM064386]
- Canadian Institutes of Health Research [FRN 57913, MSH 63646]
Accurate chromosome segregation depends on sister kinetochores making bioriented attachments to microtubules from opposite poles. An essential regulator of biorientation is the Ipl1/Aurora B protein kinase that destabilizes improper microtubule-kinetochore attachments. To identify additional biorientation pathways, we performed a systematic genetic analysis between the ipl1-321 allele and all nonessential budding yeast genes. One of the mutants, mcm21 Delta, precociously separates pericentromeres and this is associated with a defect in the binding of the Scc2 cohesin-loading factor at the centromere. Strikingly, Mcm21 becomes essential for biorientation when Ipl1 function is reduced, and this appears to be related to its role in pericentromeric cohesion. When pericentromeres are artificially tethered, Mcm21 is no longer needed for biorientation despite decreased Ipl1 activity. Taken together, these data reveal a specific role for pericentromeric linkage in ensuring kinetochore biorientation.
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