A Cyclin A—Myb-MuvB—Aurora B network regulates the choice between mitotic cycles and polyploid endoreplication cycles

Rotelli, Michael D.; Policastro, Robert A.; Bolling, Anna M.; Killion, Andrew W.; Weinberg, Abraham J.; Dixon, Michael J.; Zentner, Gabriel E.; Walczak, Claire; Lilly, Mary A.; Calvi, Brian R.

doi:10.1371/journal.pgen.1008253

Cited by 33 publications

(26 citation statements)

References 107 publications

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“…It is known that the Lin52 protein is required for the Myb subunit to associate with the core of the MMB transcription factor complex (Andrejka et al 2011; Guiley et al 2015; Guiley et al 2018). This lin-52 phenotype is, therefore, consistent with our previous finding that knockdown of Myb switches wing and other cells to endoreplication (Rotelli et al 2019). Similar to Myb knockdown, it is likely that knockdown of lin-52 impairs the induction of mitotic gene expression by the MMB and promotes a switch to endoreplication cycles that skip mitosis (Rotelli et al 2019).…”

Section: Resultssupporting

confidence: 92%

“…This lin-52 phenotype is, therefore, consistent with our previous finding that knockdown of Myb switches wing and other cells to endoreplication (Rotelli et al 2019). Similar to Myb knockdown, it is likely that knockdown of lin-52 impairs the induction of mitotic gene expression by the MMB and promotes a switch to endoreplication cycles that skip mitosis (Rotelli et al 2019). Knockdown of βNACtes6 or lin-52 also reduced the area of the L3-L4 intervein region in adult wings, suggesting that tissue growth through an increase in cell size did not fully compensate for growth by cell proliferation (Figure 2F, K, Table 2).…”

Section: Resultssupporting

confidence: 92%

“…The MMB induces the periodic cell cycle expression of genes that are important for M phase and cytokinesis (Georlette et al 2007; Schmit et al 2007; Wen et al 2008; Debruhl et al 2013; Fischer et al 2016). We had found previously that knockdown of the Myb subunit of the MMB in the wing impairs expression of mitotic genes and results in a switch to a polyploid growth program, which, similar to lin-52 knockdown, resulted in longer wing hairs and reduced tissue mass in the adult wing (Rotelli et al 2019). The similar phenotype of Myb and lin-52 knockdown makes sense in the context of recent structure-function studies that indicate that Lin52 is required for the activating Myb subunit to associate with the MuvB core (Andrejka et al 2011; Guiley et al 2018).…”

Section: Resultsmentioning

confidence: 94%

“…We recently conducted a candidate shRNA screen of 240 genes, which RNA-Seq had shown are expressed at lower levels in endoreplicating cells in culture. This candidate screen showed that knockdown of genes in a CycA – Myb – Aurora B pathway induces cells in the wing and other tissues to switch to an alternative endoreplication growth program (Rotelli et al 2019). Here, we report the results of a random screen of 5,260 additional shRNA strains, which has identified 18 genes whose knockdown impairs wing growth.…”

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confidence: 99%

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An RNAi Screen for Genes Required for Growth ofDrosophilaWing Tissue

Rotelli

Bolling

Killion

et al. 2019

G3 Genes|Genomes|Genetics

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Cell division and tissue growth must be coordinated with development. Defects in these processes are the basis for a number of diseases, including developmental malformations and cancer. We have conducted an unbiased RNAi screen for genes that are required for growth in the Drosophila wing, using GAL4-inducible short hairpin RNA (shRNA) fly strains made by the Drosophila RNAi Screening Center. shRNA expression down the center of the larval wing disc using dpp-GAL4, and the central region of the adult wing was then scored for tissue growth and wing hair morphology. Out of 4,753 shRNA crosses that survived to adulthood, 18 had impaired wing growth. FlyBase and the new Alliance of Genome Resources knowledgebases were used to determine the known or predicted functions of these genes and the association of their human orthologs with disease. The function of eight of the genes identified has not been previously defined in Drosophila. The genes identified included those with known or predicted functions in cell cycle, chromosome segregation, morphogenesis, metabolism, steroid processing, transcription, and translation. All but one of the genes are similar to those in humans, and many are associated with disease. Knockdown of lin-52, a subunit of the Myb-MuvB transcription factor, or βNACtes6, a gene involved in protein folding and trafficking, resulted in a switch from cell proliferation to an endoreplication growth program through which wing tissue grew by an increase in cell size (hypertrophy). It is anticipated that further analysis of the genes that we have identified will reveal new mechanisms that regulate tissue growth during development.

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Section: Resultssupporting

confidence: 92%

Section: Resultssupporting

confidence: 92%

Section: Resultsmentioning

confidence: 94%

mentioning

confidence: 99%

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An RNAi Screen for Genes Required for Growth ofDrosophilaWing Tissue

Rotelli

Bolling

Killion

et al. 2019

G3 Genes|Genomes|Genetics

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“…Follicle cells undergo three endocycles, resulting in a ploidy of 16C. Previous work has shown that there are distinct changes in genome regulation during the endocycle, including a global decrease in transcription, decrease in E2F1 target gene expression, and acquisition of endocycle-specific ORC binding sites (Maqbool et al 2010;Sher et al 2012;Hua et al 2018;Rotelli et al 2019). Therefore, we hypothesized that follicle cell RT may be influenced by this developmentally regulated cell cycle transition.…”

Section: Cell Lineage Is a Major Driver Of Dna Rtmentioning

confidence: 99%

Rif1 Functions in a Tissue-Specific Manner To Control Replication Timing Through Its PP1-Binding Motif

et al. 2020

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Replication initiation in eukaryotic cells occurs asynchronously throughout S phase, yielding early- and late-replicating regions of the genome, a process known as replication timing (RT). RT changes during development to ensure accurate genome duplication and maintain genome stability. To understand the relative contributions that cell lineage, cell cycle, and replication initiation regulators have on RT, we utilized the powerful developmental systems available in Drosophila melanogaster. We generated and compared RT profiles from mitotic cells of different tissues and from mitotic and endocycling cells of the same tissue. Our results demonstrate that cell lineage has the largest effect on RT, whereas switching from a mitotic to an endoreplicative cell cycle has little to no effect on RT. Additionally, we demonstrate that the RT differences we observed in all cases are largely independent of transcriptional differences. We also employed a genetic approach in these same cell types to understand the relative contribution the eukaryotic RT control factor, Rif1, has on RT control. Our results demonstrate that Rif1 can function in a tissue-specific manner to control RT. Importantly, the Protein Phosphatase 1 (PP1) binding motif of Rif1 is essential for Rif1 to regulate RT. Together, our data support a model in which the RT program is primarily driven by cell lineage and is further refined by Rif1/PP1 to ultimately generate tissue-specific RT programs.

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YY2/BUB3 Axis promotes SAC Hyperactivation and Inhibits Colorectal Cancer Progression via Regulating Chromosomal Instability

Hosea,

Duan,

Meliala

et al. 2024

Advanced Science

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Spindle assembly checkpoint (SAC) is a crucial safeguard mechanism of mitosis fidelity that ensures equal division of duplicated chromosomes to the two progeny cells. Impaired SAC can lead to chromosomal instability (CIN), a well‐recognized hallmark of cancer that facilitates tumor progression; paradoxically, high CIN levels are associated with better therapeutic response and prognosis. However, the mechanism by which CIN determines tumor cell survival and therapeutic response remains poorly understood. Here, using a cross‐omics approach, YY2 is identified as a mitotic regulator that promotes SAC activity by activating the transcription of budding uninhibited by benzimidazole 3 (BUB3), a component of SAC. While both conditions induce CIN, a defect in YY2/SAC activity enhances mitosis and tumor growth. Meanwhile, hyperactivation of SAC mediated by YY2/BUB3 triggers a delay in mitosis and suppresses growth. Furthermore, it is revealed that YY2/BUB3‐mediated excessive CIN causes higher cell death rates and drug sensitivity, whereas residual tumor cells that survived DNA damage‐based therapy have moderate CIN and increased drug resistance. These results provide insights into the role of SAC activity and CIN levels in influencing tumor cell survival and drug response, as well as suggest a novel anti‐tumor therapeutic strategy that combines SAC activity modulators and DNA‐damage agents.

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A Cyclin A—Myb-MuvB—Aurora B network regulates the choice between mitotic cycles and polyploid endoreplication cycles

Cited by 33 publications

References 107 publications

An RNAi Screen for Genes Required for Growth ofDrosophilaWing Tissue

An RNAi Screen for Genes Required for Growth ofDrosophilaWing Tissue

Rif1 Functions in a Tissue-Specific Manner To Control Replication Timing Through Its PP1-Binding Motif

YY2/BUB3 Axis promotes SAC Hyperactivation and Inhibits Colorectal Cancer Progression via Regulating Chromosomal Instability

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