Single cell tracking reveals that Msh2 is a key component of an early-acting DNA damage-activated G2 checkpoint

Márquez, Nuria Ponce; Chappell, Sally Claire; Sansom, Owen J.; Clarke, Alan R.; Court, Jacquelyn; Errington, Rachel J.; Smith, Paul J.

doi:10.1038/sj.onc.1206876

Cited by 27 publications

(27 citation statements)

References 27 publications

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“…CHO-K1 and CHO-K1 MT-1 2.20 cultures were established in multiwell dishes and transferred to a time-lapse instrument (28,29) designed to capture transmission-phase images from multiwell plates. The Axiovert 100 microscope (Carl Zeiss, Welwyn Garden City, UK) was fitted with an incubator to maintain 37°C/5% CO2 (Solent Scientific, Portsmouth, UK), and images were captured using an ORCA-ER charge-coupled device camera (Hamamatsu, Reading, UK).…”

Section: Methodsmentioning

confidence: 99%

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Impact of overexpression of metallothionein-1 on cell cycle progression and zinc toxicity

Smith

Wiltshire²,

Furon³

et al. 2008

American Journal of Physiology-Cell Physiology

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Metallothioneins (MTs) have an important role in zinc homeostasis and may counteract the impact of oversupply. Both intracellular zinc and MT expression have been implicated in proliferation control and resistance to cellular stress, although the interdependency is unclear. The study addresses the consequences of a steady-state overexpression of MT-1 for intracellular zinc levels, cell cycle progression, and protection from zinc toxicity using a panel of cell lines with differential expression of MT-1. The panel comprised parental Chinese hamster ovary-K1 cells with low endogenous expression of MT and transfectants with enhanced expression of mouse MT-1 on an autonomously replicating expression vector with a noninducible promoter. Cell cycle progression, determined by flow cytometry and time-lapse microscopy, revealed that enhanced cytoplasmic expression of MT-1 does not impact on normal cell cycle operation, suggesting that basal levels of MT-1 expression are not limiting for background levels of oxidative stress. MT-1 overexpression correlated with a steady-state increase in cytoplasmic free Zn(2+), assessed using the fluorescent zinc-sensor Zinquin, particularly at high levels of overexpression, further suggesting that zinc availability is normally not limiting for cell cycle progression. Enhanced MT-1 expression, over a 10-fold range, had a clear impact on resistance to Cd(2+) and Zn(2+) toxicity. In the case of Zn(2+), the degree of protection afforded was less, indicating that MT-1 has a limited range and saturable capacity for effecting resistance. The results have implications for the use of cellular stress responses to exogenously supplied zinc and zinc-based systemic therapies.

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Section: Methodsmentioning

confidence: 99%

“…Each cell in the field was tracked, and the time to event and duration recorded. The time-lapse event curves were processed and analyzed as previously described (28,29) for rodent cells.…”

Section: Methodsmentioning

confidence: 99%

Impact of overexpression of metallothionein-1 on cell cycle progression and zinc toxicity

Smith

Wiltshire²,

Furon³

et al. 2008

American Journal of Physiology-Cell Physiology

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“…Traditionally tracking studies have been done using time-lapse microscope imaging techniques to visualize the process of cell dynamics. However this is a time intensive method and so limits analysis to a few hundred cells at most [4,5]. The heterogeneity of cell populations is such that statistics dictate that these studies must be scaled up to measurements on several thousands of cells if realistic models of cell behavior are to be obtained.…”

Section: Introductionmentioning

confidence: 99%

Cell-population tracking using quantum dots in flow cytometry

et al. 2008

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We have used flow-cytometry together with computational modeling of quantum dot portioning during cell division to identify population distributions of proliferating cells. The objective has been to develop a robust assay of integrated cellular fluorescence which reports the extent of cellular bifurcation within a complex population and potentially provides profiles of drug resistance, cell clonality and levels of aneuploidy in tumour cells. The implementation of a data analysis program based on genetic algorithms provides a complete description of the proliferation dynamics and gives values for the inter-mitotic time, the partitioning ratio of quantum dots between daughter cells and their associated deviations.

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“…The multitag time-lapse event curves were processed appropriately and visualized in graphical plots as previously described. 25,26 Time-laspe microscopy: tracking eGFP-cyclin B1 profiles. The principles have been described previously.…”

Section: Methodsmentioning

confidence: 99%

“…Both increased and reduced levels o�� parental cell �� contents are apparent in clones arising ��rom �CR�� e�posed cultures. (C) �imelapse imaging (C) �imelapse imaging �imelapse imaging 25 o�� changes in cyclin B��e��P reporter e�pression during cell cycle progression to mitosis in control cells (upper sequence) or into mitotic �ypass (up to 70% events; lower sequence) in the presence o�� 2 mg/ml �CR��. �o evidence o�� a commitment to mitosis �e��ore cyclin B� switch�o�� (lower sequence).…”

Section: Routing To Icrf-193-induced Tetraploidy Avoids the Mitotic Smentioning

confidence: 99%

Mitotic Bypass Via An Occult Cell Cycle Phase Following DNA Topoisomerase II Inhibition In p53 Functional Human Tumor Cells

Smith¹,

Márquez²,

Wiltshire³

et al. 2007

Cell Cycle

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Single cell tracking reveals that Msh2 is a key component of an early-acting DNA damage-activated G2 checkpoint

Cited by 27 publications

References 27 publications

Impact of overexpression of metallothionein-1 on cell cycle progression and zinc toxicity

Impact of overexpression of metallothionein-1 on cell cycle progression and zinc toxicity

Cell-population tracking using quantum dots in flow cytometry

Mitotic Bypass Via An Occult Cell Cycle Phase Following DNA Topoisomerase II Inhibition In p53 Functional Human Tumor Cells

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