The BTB-ZF transcription factor Tramtrack69 shapes neural cell lineages by coordinating cell proliferation and cell fate

AbstractCell diversity in multicellular organisms relies on coordination between cell proliferation and the acquisition of cell identity. The equilibrium between these two processes is essential to assure the correct number of determined cells at a given time at a given place. Here, we show that Tramtrack-69 (Ttk69, a BTB-ZF transcription factor ortholog of the human PLZF factor) plays an essential role in controlling this balance. In theDrosophilabristle cell lineage, producing the external sensory organs composed by a neuron and accessory cells, we show thatttk69loss of function leads to supplementary neural-type cells at the expense of accessory cells. Our data indicate that Ttk69 (1) promotes cell-cycle exit of newborn terminal cells by downregulatingcycE, the principal cyclin involved in S-phase entry and (2) regulates cell fate acquisition and terminal differentiation by downregulating the expression ofhamletand upregulating that ofSuppressor of Hairless, two transcription factors involved in neural-fate acquisition and accessory-cell differentiation, respectively. Thus, Ttk69 plays a central role in shaping neural cell lineages by integrating molecular mechanisms that regulate progenitor cell-cycle exit and cell-fate commitment.Summary statementTramtrack-69, a transcription factor orthologous to the human tumor-suppressor PLZF, plays a central role in precursor cell lineages by integrating molecular mechanisms that regulate progenitor cell-cycle exit and cell-fate determination.

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Shaping of Drosophila Neural Cell Lineages Through Coordination of Cell Proliferation and Cell Fate by the BTB-ZF Transcription Factor Tramtrack-69

Genetics ◽

10.1534/genetics.119.302234 ◽

2019 ◽

Vol 212 (3) ◽

pp. 773-788

Author(s):

Françoise Simon ◽

Anne Ramat ◽

Sophie Louvet-Vallée ◽

Jérôme Lacoste ◽

Angélique Burg ◽

...

Keyword(s):

Cell Cycle ◽

Cell Proliferation ◽

Transcription Factor ◽

Cell Fate ◽

Zinc Finger ◽

Molecular Mechanisms ◽

Neural Cell ◽

Cell Cycle Exit ◽

Cell Lineages ◽

Accessory Cells

Cell diversity in multicellular organisms relies on coordination between cell proliferation and the acquisition of cell identity. The equilibrium between these two processes is essential to assure the correct number of determined cells at a given time at a given place. Using genetic approaches and correlative microscopy, we show that Tramtrack-69 (Ttk69, a Broad-complex, Tramtrack and Bric-à-brac - Zinc Finger (BTB-ZF) transcription factor ortholog of the human promyelocytic leukemia zinc finger factor) plays an essential role in controlling this balance. In the Drosophila bristle cell lineage, which produces the external sensory organs composed by a neuron and accessory cells, we show that ttk69 loss-of-function leads to supplementary neural-type cells at the expense of accessory cells. Our data indicate that Ttk69 (1) promotes cell cycle exit of newborn terminal cells by downregulating CycE, the principal cyclin involved in S-phase entry, and (2) regulates cell-fate acquisition and terminal differentiation, by downregulating the expression of hamlet and upregulating that of Suppressor of Hairless, two transcription factors involved in neural-fate acquisition and accessory cell differentiation, respectively. Thus, Ttk69 plays a central role in shaping neural cell lineages by integrating molecular mechanisms that regulate progenitor cell cycle exit and cell-fate commitment.

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The WT1-like transcription factor Klumpfuss maintains lineage commitment of enterocyte progenitors in the Drosophila intestine

Nature Communications ◽

10.1038/s41467-019-12003-0 ◽

2019 ◽

Vol 10 (1) ◽

Cited By ~ 8

Author(s):

Jerome Korzelius ◽

Sina Azami ◽

Tal Ronnen-Oron ◽

Philipp Koch ◽

Maik Baldauf ◽

...

Keyword(s):

Transcription Factor ◽

Cell Differentiation ◽

Cell Fate ◽

Progenitor Cell ◽

Lineage Commitment ◽

Proneural Gene ◽

Cell Lineages ◽

Daughter Cells ◽

Mechanistic Insight ◽

Insight Into

Abstract In adult epithelial stem cell lineages, the precise differentiation of daughter cells is critical to maintain tissue homeostasis. Notch signaling controls the choice between absorptive and entero-endocrine cell differentiation in both the mammalian small intestine and the Drosophila midgut, yet how Notch promotes lineage restriction remains unclear. Here, we describe a role for the transcription factor Klumpfuss (Klu) in restricting the fate of enteroblasts (EBs) in the Drosophila intestine. Klu is induced in Notch-positive EBs and its activity restricts cell fate towards the enterocyte (EC) lineage. Transcriptomics and DamID profiling show that Klu suppresses enteroendocrine (EE) fate by repressing the action of the proneural gene Scute, which is essential for EE differentiation. Loss of Klu results in differentiation of EBs into EE cells. Our findings provide mechanistic insight into how lineage commitment in progenitor cell differentiation can be ensured downstream of initial specification cues.

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The transcription factor Zic4 acts as a transdifferentiation switch

10.1101/2021.12.22.473838 ◽

2021 ◽

Author(s):

Matthias Christian Vogg ◽

Jaroslav Ferenc ◽

Wanda Christa Buzgariu ◽

Chrystelle Perruchoud ◽

Panagiotis Papasaikas ◽

...

Keyword(s):

Cell Cycle ◽

Transcription Factor ◽

Gene Regulatory Network ◽

Cell Fate ◽

Regulatory Network ◽

Molecular Mechanisms ◽

Model System ◽

Cell Identity ◽

Transcriptional Switch ◽

Gene Regulatory

The molecular mechanisms that maintain cell identities and prevent transdifferentiation remain mysterious. Interestingly, both dedifferentiation and transdifferentiation are transiently reshuffled during regeneration. Therefore, organisms that regenerate readily offer a fruitful paradigm to investigate the regulation of cell fate stability. Here, we used Hydra as a model system and show that Zic4 silencing is sufficient to induce transdifferentiation of tentacle into foot cells. We identified a Wnt-controlled Gene Regulatory Network that controls a transcriptional switch of cell identity. Furthermore, we show that this switch also controls the re-entry into the cell cycle. Our data indicate that maintenance of cell fate by a Wnt-controlled GRN is a key mechanism during both homeostasis and regeneration.

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The Phox2b transcription factor coordinately regulates neuronal cell cycle exit and identity

Development ◽

10.1242/dev.127.23.5191 ◽

2000 ◽

Vol 127 (23) ◽

pp. 5191-5201 ◽

Cited By ~ 3

Author(s):

V. Dubreuil ◽

M. Hirsch ◽

A. Pattyn ◽

J. Brunet ◽

C. Goridis

Keyword(s):

Cell Cycle ◽

Transcription Factor ◽

Cell Fate ◽

Motor Neurons ◽

Ventricular Zone ◽

Ectopic Expression ◽

Neuronal Cell ◽

Cell Cycle Exit ◽

Neuronal Precursors ◽

Regulation Of Cell Cycle

In the vertebrate neural tube, cell cycle exit of neuronal progenitors is accompanied by the expression of transcription factors that define their generic and sub-type specific properties, but how the regulation of cell cycle withdrawal intersects with that of cell fate determination is poorly understood. Here we show by both loss- and gain-of-function experiments that the neuronal-subtype-specific homeodomain transcription factor Phox2b drives progenitor cells to become post-mitotic. In the absence of Phox2b, post-mitotic neuronal precursors are not generated in proper numbers. Conversely, forced expression of Phox2b in the embryonic chick spinal cord drives ventricular zone progenitors to become post-mitotic neurons and to relocate to the mantle layer. In the neurons thus generated, ectopic expression of Phox2b is sufficient to initiate a programme of motor neuronal differentiation characterised by expression of Islet1 and of the cholinergic transmitter phenotype, in line with our previous results showing that Phox2b is an essential determinant of cranial motor neurons. These results suggest that Phox2b coordinates quantitative and qualitative aspects of neurogenesis, thus ensuring that neurons of the correct phenotype are generated in proper numbers at the appropriate times and locations.

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Cell cycle and cell-fate determination in Drosophila neural cell lineages

Trends in Genetics ◽

10.1016/j.tig.2005.05.010 ◽

2005 ◽

Vol 21 (7) ◽

pp. 413-420 ◽

Cited By ~ 15

Author(s):

Pierre Fichelson ◽

Agnès Audibert ◽

Françoise Simon ◽

Michel Gho

Keyword(s):

Cell Cycle ◽

Cell Fate ◽

Neural Cell ◽

Cell Fate Determination ◽

Fate Determination ◽

Cell Lineages

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Homeodomain Transcription Factor Phox2a, via Cyclic AMP-Mediated Activation, Induces p27Kip1 Transcription, Coordinating Neural Progenitor Cell Cycle Exit and Differentiation

Molecular and Cellular Biology ◽

10.1128/mcb.00575-06 ◽

2006 ◽

Vol 26 (23) ◽

pp. 8826-8839 ◽

Cited By ~ 21

Author(s):

Maryline Paris ◽

Wen-Horng Wang ◽

Min-Hwa Shin ◽

David S. Franklin ◽

Ourania M. Andrisani

Keyword(s):

Cell Cycle ◽

Transcription Factor ◽

Cyclic Amp ◽

Neuronal Differentiation ◽

Progenitor Cell ◽

Neural Progenitor Cell ◽

Neural Progenitor ◽

Camp Signaling ◽

Cell Cycle Exit ◽

Homeodomain Transcription Factor

ABSTRACT Mechanisms coordinating neural progenitor cell cycle exit and differentiation are incompletely understood. The cyclin-dependent kinase inhibitor p27Kip1 is transcriptionally induced, switching specific neural progenitors from proliferation to differentiation. However, neuronal differentiation-specific transcription factors mediating p27Kip1 transcription have not been identified. We demonstrate the homeodomain transcription factor Phox2a, required for central nervous system (CNS)- and neural crest (NC)-derived noradrenergic neuron differentiation, coordinates cell cycle exit and differentiation by inducing p27Kip1 transcription. Phox2a transcription and activation in the CNS-derived CAD cell line and primary NC cells is mediated by combined cyclic AMP (cAMP) and bone morphogenetic protein 2 (BMP2) signaling. In the CAD cellular model, cAMP and BMP2 signaling initially induces proliferation of the undifferentiated precursors, followed by p27Kip1 transcription, G1 arrest, and neuronal differentiation. Small interfering RNA silencing of either Phox2a or p27Kip1 suppresses p27Kip1 transcription and neuronal differentiation, suggesting a causal link between p27Kip1 expression and differentiation. Conversely, ectopic Phox2a expression via the Tet-off expression system promotes accelerated CAD cell neuronal differentiation and p27Kip1 transcription only in the presence of cAMP signaling. Importantly, endogenous or ectopically expressed Phox2a activated by cAMP signaling binds homeodomain cis-acting elements of the p27Kip1 promoter in vivo and mediates p27Kip1-luciferase expression in CAD and NC cells. We conclude that developmental cues of cAMP signaling causally link Phox2a activation with p27Kip1 transcription, thereby coordinating neural progenitor cell cycle exit and differentiation.

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LMNB2 promotes the progression of colorectal cancer by silencing p21 expression

Cell Death and Disease ◽

10.1038/s41419-021-03602-1 ◽

2021 ◽

Vol 12 (4) ◽

Author(s):

Chen-Hua Dong ◽

Tao Jiang ◽

Hang Yin ◽

Hu Song ◽

Yi Zhang ◽

...

Keyword(s):

Colorectal Cancer ◽

Cell Cycle ◽

Cell Proliferation ◽

Cell Cycle Progression ◽

Molecular Mechanisms ◽

Gene Set Enrichment Analysis ◽

Molecular Therapy ◽

Cycle Progression ◽

Cancer Tissues

AbstractColorectal cancer is the second common cause of death worldwide. Lamin B2 (LMNB2) is involved in chromatin remodeling and the rupture and reorganization of nuclear membrane during mitosis, which is necessary for eukaryotic cell proliferation. However, the role of LMNB2 in colorectal cancer (CRC) is poorly understood. This study explored the biological functions of LMNB2 in the progression of colorectal cancer and explored the possible molecular mechanisms. We found that LMNB2 was significantly upregulated in primary colorectal cancer tissues and cell lines, compared with paired non-cancerous tissues and normal colorectal epithelium. The high expression of LMNB2 in colorectal cancer tissues is significantly related to the clinicopathological characteristics of the patients and the shorter overall and disease-free cumulative survival. Functional analysis, including CCK8 cell proliferation test, EdU proliferation test, colony formation analysis, nude mouse xenograft, cell cycle, and apoptosis analysis showed that LMNB2 significantly promotes cell proliferation by promoting cell cycle progression in vivo and in vitro. In addition, gene set enrichment analysis, luciferase report analysis, and CHIP analysis showed that LMNB2 promotes cell proliferation by regulating the p21 promoter, whereas LMNB2 has no effect on cell apoptosis. In summary, these findings not only indicate that LMNB2 promotes the proliferation of colorectal cancer by regulating p21-mediated cell cycle progression, but also suggest the potential value of LMNB2 as a clinical prognostic marker and molecular therapy target.

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The EGL-13 SOX Domain Transcription Factor Affects the Uterine Cell Lineages in Caenorhabditis elegans

Genetics ◽

10.1093/genetics/165.3.1623 ◽

2003 ◽

Vol 165 (3) ◽

pp. 1623-1628

Author(s):

Hediye Nese Cinar ◽

Keri L Richards ◽

Kavita S Oommen ◽

Anna P Newman

Keyword(s):

Transcription Factor ◽

Cell Division ◽

Caenorhabditis Elegans ◽

Cell Fate ◽

Cell Lineages

Abstract We isolated egl-13 mutants in which the cells of the Caenorhabditis elegans uterus initially appeared to develop normally but then underwent an extra round of cell division. The data suggest that egl-13 is required for maintenance of the cell fate.

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A Unilateral Negative Feedback Loop Between miR-200 microRNAs and Sox2/E2F3 Controls Neural Progenitor Cell-Cycle Exit and Differentiation

Journal of Neuroscience ◽

10.1523/jneurosci.2124-12.2012 ◽

2012 ◽

Vol 32 (38) ◽

pp. 13292-13308 ◽

Cited By ~ 71

Author(s):

C. Peng ◽

N. Li ◽

Y.-K. Ng ◽

J. Zhang ◽

F. Meier ◽

...

Keyword(s):

Cell Cycle ◽

Negative Feedback ◽

Progenitor Cell ◽

Feedback Loop ◽

Neural Progenitor Cell ◽

Neural Progenitor ◽

Negative Feedback Loop ◽

Cell Cycle Exit

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Histone chaperone HIRA regulates neural progenitor cell proliferation and neurogenesis via β-catenin

The Journal of Cell Biology ◽

10.1083/jcb.201610014 ◽

2017 ◽

Vol 216 (7) ◽

pp. 1975-1992 ◽

Cited By ~ 14

Author(s):

Yanxin Li ◽

Jianwei Jiao

Keyword(s):

Cell Cycle ◽

Cell Proliferation ◽

Progenitor Cell ◽

Neural Progenitor Cells ◽

Neural Progenitor Cell ◽

Neural Progenitor ◽

Histone Chaperone ◽

Epigenetic Mechanism ◽

Progenitor Cell Proliferation ◽

Early Neurogenesis

Histone cell cycle regulator (HIRA) is a histone chaperone and has been identified as an epigenetic regulator. Subsequent studies have provided evidence that HIRA plays key roles in embryonic development, but its function during early neurogenesis remains unknown. Here, we demonstrate that HIRA is enriched in neural progenitor cells, and HIRA knockdown reduces neural progenitor cell proliferation, increases terminal mitosis and cell cycle exit, and ultimately results in premature neuronal differentiation. Additionally, we demonstrate that HIRA enhances β-catenin expression by recruiting H3K4 trimethyltransferase Setd1A, which increases H3K4me3 levels and heightens the promoter activity of β-catenin. Significantly, overexpression of HIRA, HIRA N-terminal domain, or β-catenin can override neurogenesis abnormities caused by HIRA defects. Collectively, these data implicate that HIRA, cooperating with Setd1A, modulates β-catenin expression and then regulates neurogenesis. This finding represents a novel epigenetic mechanism underlying the histone code and has profound and lasting implications for diseases and neurobiology.

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