Spindle Checkpoint Maintenance Requires Ame1 and Okp1

Overview

Journal Cell Cycle

Specialty Cell Biology

Date 2005 Sep 24

PMID 16177574

Citations 18

Authors

Isabelle Pot

James Knockleby

Victoria Aneliunas

Thao Nguyen

Sonia Ah-Kye

Gregory Liszt

Michael Snyder

Philip Hieter

Jackie Vogel

Affiliations

Soon will be listed here.

Abstract

Kinetochore proteins are required for high fidelity chromosome segregation and as a platform for checkpoint signaling. Ame1 is an essential component of the COMA (Ctf19, Okp1, Mcm21, Ame1) sub-complex of the central kinetochore of budding yeast. In this study, we describe the isolation and characterization of an Ame1 conditional mutant, ame1-4. ame1-4 cells exhibit chromosome segregation defects and Mad2-dependent cell cycle delay similar to okp1-5 cells. However, the viability of ame1-4 cells is markedly reduced relative to wild type and okp1-5 cells after three hours at restrictive temperature. To determine if ame1-4 cells enter anaphase with mis-segregated chromosomes, we monitored the localization of Bub3:VFP as a marker for anaphase onset. ame1-4 cells containing mis-segregated sister chromatids initially accumulate Bub3:VFP at kinetochores, indicating checkpoint activation and a metaphase arrest. Subsequently, Bub3:VFP de-localizes and cells reinitiate DNA duplication and budding without cytokinesis in the presence of un-segregated chromosomes. Overexpression of OKP1 in ame1-4 cells restores ame1-4 protein localization and a stable arrest. Based on our results, we propose that Ame1 and Okp1 are required for a sustained checkpoint arrest in the presence of mis-segregated chromosomes. Our results suggest that checkpoint response might be controlled not only at the level of activation but also via signals that ensure maintenance of the response.

Citing Articles

Recognition of centromere-specific histone Cse4 by the inner kinetochore Okp1-Ame1 complex.

Deng S, Cai J, Harrison S, Zhou H, Hinshaw S EMBO Rep. 2023; 24(12):e57702.

PMID: 37983946 PMC: 10702835. DOI: 10.15252/embr.202357702.

A role for β-1,6- and β-1,3-glucans in kinetochore function in Saccharomyces cerevisiae.

Kshirsagar R, Munhoven A, Tran Nguyen T, Ehrenhofer-Murray A Genetics. 2023; 226(2).

PMID: 37950911 PMC: 11221361. DOI: 10.1093/genetics/iyad195.

Reconstitution reveals two paths of force transmission through the kinetochore.

Hamilton G, Helgeson L, Noland C, Asbury C, Dimitrova Y, Davis T Elife. 2020; 9.

PMID: 32406818 PMC: 7367685. DOI: 10.7554/eLife.56582.

AI-Assisted Forward Modeling of Biological Structures.

Lawrimore J, Doshi A, Walker B, Bloom K Front Cell Dev Biol. 2019; 7:279.

PMID: 31799251 PMC: 6868055. DOI: 10.3389/fcell.2019.00279.

Where is the right path heading from the centromere to spindle microtubules?.

Hara M, Fukagawa T Cell Cycle. 2019; 18(11):1199-1211.

PMID: 31075048 PMC: 6592241. DOI: 10.1080/15384101.2019.1617008.