Kinetochore life histories reveal an Aurora-B-dependent error correction mechanism in anaphase

Sen, Onur; Harrison, Jonathan U.; Burroughs, Nigel John; McAinsh, Andrew D.

doi:10.1016/j.devcel.2021.10.007

Cited by 28 publications

(17 citation statements)

References 75 publications

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“…2A, B ). 3D kinetochore tracking 28 , and measurement of EGFP-HURP intensity along the associated K-fibre showed that as metaphase sister kinetochores oscillated back-and-forth, HURP was exclusively present on depolymerising K-fibres (associated to the leading kinetochore sister), and never on the growing K-fibre (associated to the trailing kinetochore sister) (Fig. 2C, D ).…”

Section: Resultsmentioning

confidence: 98%

Evidence for a HURP/EB free mixed-nucleotide zone in kinetochore-microtubules

et al. 2022

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Current models infer that the microtubule-based mitotic spindle is built from GDP-tubulin with small GTP caps at microtubule plus-ends, including those that attach to kinetochores, forming the kinetochore-fibres. Here we reveal that kinetochore-fibres additionally contain a dynamic mixed-nucleotide zone that reaches several microns in length. This zone becomes visible in cells expressing fluorescently labelled end-binding proteins, a known marker for GTP-tubulin, and endogenously-labelled HURP - a protein which we show to preferentially bind the GDP microtubule lattice in vitro and in vivo. We find that in mitotic cells HURP accumulates on the kinetochore-proximal region of depolymerising kinetochore-fibres, whilst avoiding recruitment to nascent polymerising K-fibres, giving rise to a growing “HURP-gap”. The absence of end-binding proteins in the HURP-gaps leads us to postulate that they reflect a mixed-nucleotide zone. We generate a minimal quantitative model based on the preferential binding of HURP to GDP-tubulin to show that such a mixed-nucleotide zone is sufficient to recapitulate the observed in vivo dynamics of HURP-gaps.

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Section: Resultsmentioning

confidence: 98%

Evidence for a HURP/EB free mixed-nucleotide zone in kinetochore-microtubules

et al. 2022

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“…In a set of recent studies, it was reported that the Aurora B midzone gradient mediates phosphorylation of outer kinetochore proteins even during anaphase [201], at similar sites as in pre-anaphase cells [158]. Thus, it seems that error correction mediated by Aurora B has an additional layer operating in early anaphase [194,202] (Figure 7, route 2), which could explain previous observations that the proportion of lagging chromosomes during anaphase is by an order of magnitude higher than the proportion of cells with aneuploidy in the same population [203]. Furthermore, this led to a redefinition of lagging kinetochores by introducing a new term of 'lazy' kinetochores, transiently lagging kinetochores that are quickly and efficiently corrected during the early anaphase by the Aurora B-dependent mechanism [194] (Figure 7, route 2).…”

Section: Different Ways To Mis-segregation Through Polar Chromosomesmentioning

confidence: 99%

“…A recent study presented an intriguing model in which difficulties associated with the inability of unaligned chromosomes to congress are not necessarily caused by defects related to MTs, SAC, or motors but rather due to the presence of a complex system of organelle remnants behind the spindle poles, termed endomembranes, which could ensheat polar chromosomes and prevent their efficient capture by MTs, resulting in aneuploidy [189]. However, for definitive conclusions about the mechanisms underlying unaligned chromosome mis-segregation in unperturbed cells, one would need to track the origin and fate of mis-segregations through whole mitosis, similar to what was done recently from metaphase to telophase in human cells [194].…”

Section: Different Ways To Mis-segregation Through Polar Chromosomesmentioning

confidence: 99%

“…Thus, it seems that error correction mediated by Aurora B has an additional layer operating in early anaphase [194,202] (Figure 7, route 2), which could explain previous observations that the proportion of lagging chromosomes during anaphase is by an order of magnitude higher than the proportion of cells with aneuploidy in the same population [203]. Furthermore, this led to a redefinition of lagging kinetochores by introducing a new term of 'lazy' kinetochores, transiently lagging kinetochores that are quickly and efficiently corrected during the early anaphase by the Aurora B-dependent mechanism [194] (Figure 7, route 2). However, in certain situations, even moderate alignment defects can induce malfunctioning nuclear morphologies and micronuclei [204], calling for long-term tracking of chromosome fates during mitosis.…”

Section: Different Ways To Mis-segregation Through Polar Chromosomesmentioning

confidence: 99%

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Polar Chromosomes—Challenges of a Risky Path

Vukušić

Tolić

2022

Cells

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The process of chromosome congression and alignment is at the core of mitotic fidelity. In this review, we discuss distinct spatial routes that the chromosomes take to align during prometaphase, which are characterized by distinct biomolecular requirements. Peripheral polar chromosomes are an intriguing case as their alignment depends on the activity of kinetochore motors, polar ejection forces, and a transition from lateral to end-on attachments to microtubules, all of which can result in the delayed alignment of these chromosomes. Due to their undesirable position close to and often behind the spindle pole, these chromosomes may be particularly prone to the formation of erroneous kinetochore-microtubule interactions, such as merotelic attachments. To prevent such errors, the cell employs intricate mechanisms to preposition the spindle poles with respect to chromosomes, ensure the formation of end-on attachments in restricted spindle regions, repair faulty attachments by error correction mechanisms, and delay segregation by the spindle assembly checkpoint. Despite this protective machinery, there are several ways in which polar chromosomes can fail in alignment, mis-segregate, and lead to aneuploidy. In agreement with this, polar chromosomes are present in certain tumors and may even be involved in the process of tumorigenesis.

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“…Previously, the rate of lagging chromosomes in human cells was estimated at 5%; however, imaging limitations and data relying on fixed samples provide an incomplete picture. Using lattice light-sheet imaging and computational analysis of 3D kinetochore trajectory tracking, Andrew McAinsh, Nigel Borroughs and colleagues 1 propose that the risk of mis-segregation in human mitotic cells is higher than previously assumed. They quantify metaphase sister chromatid behaviour as a predictor for lagging chromosomes in anaphase and collect evidence for the existence of an early anaphase correction mechanism orchestrated by the kinase Aurora B.…”

mentioning

confidence: 99%

Oh lazy sister, where art thou?

Breuer¹

2021

Commun Biol

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Mitotic divisions achieve equal re-partition of chromosomes into daughter cells. In their recent work in Developmental Cell , Sen, Harrison et al. propose that the risk of mis-segregation in human mitotic cells is higher than previously thought and identify the existence of an early-anaphase correction mechanism. The study documents kinetochore dynamics in unprecedented detail, providing a detailed look at the events preceding loss of correct chromosomal numericity and genomic stability.

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Kinetochore life histories reveal an Aurora-B-dependent error correction mechanism in anaphase

Cited by 28 publications

References 75 publications

Evidence for a HURP/EB free mixed-nucleotide zone in kinetochore-microtubules

Evidence for a HURP/EB free mixed-nucleotide zone in kinetochore-microtubules

Polar Chromosomes—Challenges of a Risky Path

Oh lazy sister, where art thou?

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