A Retinoblastoma Orthologue Is a Major Regulator of S-Phase, Mitotic, and Developmental Gene Expression in Dictyostelium

Strasser, Kimchi; Bloomfield, Gareth; MacWilliams, Asa; Ceccarelli, Adriano; MacWilliams, Harry K.; Tsang, Adrian

doi:10.1371/journal.pone.0039914

Cited by 11 publications

(18 citation statements)

References 63 publications

(93 reference statements)

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“…Accordingly, we predict that immediately following cell division cells will enter S-phase. Consistent with this and previous reports (Araki et al, 1994;MacWilliams et al, 2006;Strasser et al, 2012), we observe increased numbers of BrdU-stained cells immediately following cell division between 3 and 4 hours after Ax2 and adprt2 2 cells were stained with antibodies that recognise phosphorylated H2AX (cH2AX). In parallel, cells were left untreated and incubated in 100 mM BrdU for 30 minutes and subsequently subjected to immunofluorescence using antibodies against BrdU.…”

Section: Resultssupporting

confidence: 92%

“…The cell synchronisation protocol was adapted from previously described methods (Araki et al, 1994;Strasser et al, 2012). Briefly, exponentially growing cells were seeded at between 0.75 and 1610 6 cells/ml and incubated in shaking suspension (220 rpm) at 9.5˚C for 16 hours to induce cell cycle arrest in G2.…”

Section: Methodsmentioning

confidence: 99%

“…One interpretation of these data are that in the absence of Adprt2, MMS-induced DNA damage is specifically recognised by components of the NHEJ machinery. However, given that ARTs have been implicated promoting HR at stalled and/or collapsed replication forks (Bryant et al, 2009;Sugimura et al, 2008;Yang et al, 2004), an alternative possibility is that this observation reflects a defect in the HR pathway in adprt2 2 cells, as opposed to an inherent bias towards NHEJ. However, compared to untreated control cultures, FLAG-Rad51 is enriched in chromatin fractions prepared from Ax2 and adprt2 2 cells exposed to the DSB-inducing agent phleomycin ( Fig.…”

Section: Adprt1a Signals Mms-induced Dna Lesions In the Absence Of Admentioning

confidence: 99%

“…It is important to note that vertebrate ARTs have been implicated in promoting HR, particularly at DSBs generated at stalled replication forks (Bryant et al, 2009;Sugimura et al, 2008;Yang et al, 2004). Given that Adprt2 is acting in a manner analogous to PARP1, at least as regards signalling base damage and DNA SSBs, an important consideration is that the absence of FLAG-Rad51 recruitment to MMS-induced DNA lesions in adprt2 2 cells reflects an inherent defect in HR, as opposed to a preferential engagement of the NHEJ machinery.…”

Section: Loss Of Ssb-responsive Arts Promote Nhej 3457mentioning

confidence: 99%

“…DNA DSBs can be repaired by homologous recombination (HR) or nonhomologous end-joining (NHEJ) (Branzei and Foiani, 2008). PARP1 has been implicated in HR-mediated repair of DSBs at stalled and/or damaged replication forks (Bryant et al, 2009;Sugimura et al, 2008;Yang et al, 2004), in addition to alternative NHEJ (A-NHEJ), an end-joining pathway that is activated in the absence of core NHEJ factors such as DNAPKCs and Ku (Audebert et al, 2004;Brown et al, 2002;Robert et al, 2009;Wang et al, 2006). However, its role in classic NHEJ is less clear.…”

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confidence: 99%

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Nonhomologous end-joining promotes resistance to DNA damage in the absence of an ADP-ribosyltransferase that signals DNA single strand breaks

Couto

Hsu

Teo

et al. 2013

Journal of Cell Science

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Summary ADP-ribosylation of proteins at DNA lesions by ADP-ribosyltransferases (ARTs) is an early response to DNA damage. The best defined role of ADP-ribosylation in the DNA damage response is in repair of single strand breaks (SSBs). Recently, we initiated a study of how ADP-ribosylation regulates DNA repair in Dictyostelium and found that two ARTs (Adprt1b and Adprt2) are required for tolerance of cells to SSBs, and a third ART (Adprt1a) promotes nonhomologous end-joining (NHEJ). Here we report that disruption of adprt2 results in accumulation of DNA damage throughout the cell cycle following exposure to agents that induce base damage and DNA SSBs. Although ADP-ribosylation is evident in adprt2 -cells exposed to methylmethanesulfonate (MMS), disruption of adprt1a and adprt2 in combination abolishes this response and further sensitises cells to this agent, indicating that in the absence of Adprt2, Adprt1a signals MMS-induced DNA lesions to promote resistance of cells to DNA damage. As a consequence of defective signalling of SSBs by Adprt2, Adprt1a is required to assemble NHEJ factors in chromatin, and disruption of the NHEJ pathway in combination with adprt2 increases sensitivity of cells to MMS. Taken together, these data indicate overlapping functions of different ARTs in signalling DNA damage, and illustrate a critical requirement for NHEJ in maintaining cell viability in the absence of an effective SSB response.

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Section: Resultssupporting

confidence: 92%

Section: Methodsmentioning

confidence: 99%

Section: Adprt1a Signals Mms-induced Dna Lesions In the Absence Of Admentioning

confidence: 99%

Section: Loss Of Ssb-responsive Arts Promote Nhej 3457mentioning

confidence: 99%

mentioning

confidence: 99%

See 3 more Smart Citations

Nonhomologous end-joining promotes resistance to DNA damage in the absence of an ADP-ribosyltransferase that signals DNA single strand breaks

Couto

Hsu

Teo

et al. 2013

Journal of Cell Science

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Microfluidic single-cell measurements of oxidative stress as a function of cell cycle position

Allcroft,

Duong,

Skardal

et al. 2023

Anal Bioanal Chem

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Cell Cycle Heterogeneity Can Generate Robust Cell Type Proportioning

et al. 2018

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SummaryCell-cell heterogeneity can facilitate lineage choice during embryonic development because it primes cells to respond to differentiation cues. However, remarkably little is known about the origin of heterogeneity or whether intrinsic and extrinsic variation can be controlled to generate reproducible cell type proportioning seen in vivo. Here, we use experimentation and modeling in D. discoideum to demonstrate that population-level cell cycle heterogeneity can be optimized to generate robust cell fate proportioning. First, cell cycle position is quantitatively linked to responsiveness to differentiation-inducing signals. Second, intrinsic variation in cell cycle length ensures cells are randomly distributed throughout the cell cycle at the onset of multicellular development. Finally, extrinsic perturbation of optimal cell cycle heterogeneity is buffered by compensatory changes in global signal responsiveness. These studies thus illustrate key regulatory principles underlying cell-cell heterogeneity optimization and the generation of robust and reproducible fate choice in development.

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A Retinoblastoma Orthologue Is a Major Regulator of S-Phase, Mitotic, and Developmental Gene Expression in Dictyostelium

Cited by 11 publications

References 63 publications

Nonhomologous end-joining promotes resistance to DNA damage in the absence of an ADP-ribosyltransferase that signals DNA single strand breaks

Nonhomologous end-joining promotes resistance to DNA damage in the absence of an ADP-ribosyltransferase that signals DNA single strand breaks

Microfluidic single-cell measurements of oxidative stress as a function of cell cycle position

Cell Cycle Heterogeneity Can Generate Robust Cell Type Proportioning

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