Prospero Acts as a Binary Switch between Self-Renewal and Differentiation in Drosophila Neural Stem Cells

Choksi, Semil P.; Southall, Tony D.; Bossing, Torsten; Edoff, Karin; Wit, Elzo de; Fischer, Bettina; Steensel, Bas van; Micklem, Gos; Brand, Andrea H.

doi:10.1016/j.devcel.2006.09.015

Cited by 368 publications

(491 citation statements)

References 71 publications

(84 reference statements)

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“…In one instance, Trbl suppresses a block in cell division caused by a dominant negative version of the Rho kinase Pebble (Gregory et al, 2007). As mentioned above, Trbl misexpression in male spermatagonia increases transit amplification of stem cells (Schulz et al, 2004); subsequently, it was shown that trbl RNA was down-regulated by the Prospero transcription factor, a negative regulator of spermatogonial stem cell proliferation (Choksi et al, 2006).…”

Section: -Present: Trbl Controls Cell Division During Tissue Pattmentioning

confidence: 96%

Developmental roles of tribbles protein family members

Dobens

Bouyain

2012

Developmental Dynamics

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The gene tribbles (trbl), identified 12 years ago in genetic screens for mutations that control both cell division and cell migration during embryonic Drosophila development, is the founding member of the Tribbles (Trib) family of kinase-like proteins that have diverse roles in cell signaling, tissue homeostasis, and cancer. Trib proteins share three motifs: (1) a divergent kinase region (Trib domain) with undetermined catalytic activity, (2) a COP1 site used to direct key target proteins to the proteosome for degradation, and (3) a MEK1 site that binds and modulates MAPKK kinase activity. The notion that Tribs act as scaffolding proteins to balance signaling levels in multiple pathways retains an attractive simplicity, but given recent data showing that divergent kinases act by means of novel catalytic mechanisms, the enzymatic activity of Tribs remains untested. Here, we focus on the role of Tribs during development. Developmental analysis of Drosophila trbl phenotypes reveals tissue-specific, sometimes contradictory roles. In mammals, multiple Trib isoforms exhibit overlapping and tissue-specific functions. Recent data indicate the mechanism of Trib activity is conserved and requires the Trib domain. Finally, we discuss the connections between Tribs in disease and cancer that have implications for their normal roles during organogenesis.

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Section: -Present: Trbl Controls Cell Division During Tissue Pattmentioning

confidence: 96%

Developmental roles of tribbles protein family members

Dobens

Bouyain

2012

Developmental Dynamics

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“…Once segregated to the GMC, Mira is degraded, thereby releasing Pros from the cortex (Ikeshima-Kataoka et al 1997;Shen et al 1997;Matsuzaki et al 1998). Pros can then enter the nucleus, where it has been thought to specify GMC identity by promoting the expression of GMC-specific genes and repressing the expression of neuroblast-specific genes (but see Choksi et al 2006).…”

Section: Neurogenesis In Drosophila (A) Neuroblast Formation: Notch Smentioning

confidence: 99%

“…In pins lgl double mutants, DaPKC is delocalized and inherited by both daughter cells, and thus neuroblasts undergo continuous symmetric self-renewing divisions (adapted from Lee et al 2006a). expression of Prospero in brat mutant clones rescues the brat phenotype (Bello et al 2006). Recently it has been shown, by whole genome mapping of the genes regulated by Prospero, that Prospero acts as a binary switch between stem cell self-renewal and differentiation, and that GMCs are transformed into neuroblasts in prospero mutant embryos (Choksi et al 2006). Brat is involved in the control of cell growth, possibly to maintain the size of neuroblasts as they undergo self-renewal.…”

Section: Neurogenesis In Drosophila (A) Neuroblast Formation: Notch Smentioning

confidence: 99%

Insights into neural stem cell biology from flies

Egger

Chell

Brand

2007

Phil. Trans. R. Soc. B

134

126

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Drosophila neuroblasts are similar to mammalian neural stem cells in their ability to self-renew and to produce many different types of neurons and glial cells. In the past two decades, great advances have been made in understanding the molecular mechanisms underlying embryonic neuroblast formation, the establishment of cell polarity and the temporal regulation of cell fate. It is now a challenge to connect, at the molecular level, the different cell biological events underlying the transition from neural stem cell maintenance to differentiation. Progress has also been made in understanding the later stages of development, when neuroblasts become mitotically inactive, or quiescent, and are then reactivated postembryonically to generate the neurons that make up the adult nervous system. The ability to manipulate the steps leading from quiescence to proliferation and from proliferation to differentiation will have a major impact on the treatment of neurological injury and neurodegenerative disease.

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“…4). Notably, mutations in genes that result in defects in function or asymmetric localization of cell fate determinants such as mutations in Pros, Numb, Brat or in their adaptors Mira and Pon result in massive tumorous overproliferation in the brain due to the production of supernumerary self-renewing daughters at the expense of differentiated cells (Bello et al, 2006;Betschinger et al, 2006;Choksi et al, 2006;Wang et al, 2006a). Neural tumors also result from mutation of other genes involved in asymmetric cell division such as discs large (dlg), lethal giant larva (lgl), and scribble (scrib) or the genes encoding the Aur-A and Polo kinases !…”

Section: ! 6!mentioning

confidence: 99%

Control of neural stem cell self-renewal and differentiation in Drosophila

Kang

Reichert

2014

Cell Tissue Res

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The neural stem cells of Drosophila, called neuroblasts, have the ability to self-renew and at the same time produce many different types of neurons and glial cells. In the central brain and ventral ganglia, neuroblasts are specified and delaminate from the neuroectoderm during embryonic development under the control of proneural and neurogenic genes. In contrast, in the optic lobes, neuroepithelial cells are

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Prospero Acts as a Binary Switch between Self-Renewal and Differentiation in Drosophila Neural Stem Cells

Cited by 368 publications

References 71 publications

Developmental roles of tribbles protein family members

Developmental roles of tribbles protein family members

Insights into neural stem cell biology from flies

Control of neural stem cell self-renewal and differentiation in Drosophila

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