Wingless, decapentaplegic and EGF receptor signaling pathways interact to specify dorso-ventral pattern in the adult abdomen of Drosophila

Adult abdominal segments of Drosophila are subdivided along the dorso-ventral axis into a dorsal tergite, a ventral sternite and ventro-lateral pleural cuticle. We report that this pattern is largely specified during the pupal stage by Wingless (Wg), Decapentaplegic (Dpp) and Drosophila EGF Receptor (DER) signaling. Expression of wg and dpp is activated at the posterior edge of the anterior compartment by Hedgehog signaling. Within this region, wg and dpp are expressed in domains that are mutually exclusive along the dorso-ventral axis: wg is expressed in the sternite and medio-lateral tergite, whereas dpp expression is confined to the pleura and the dorsal midline. Neither gene is expressed in the lateral tergite. Shirras and Couso (1996, Dev. Biol. 175, 24–36) have shown that tergite and sternite cell fates are specified by Wg signaling. We find that DER acts synergistically with Wg to promote tergite and sternite identities, and that Wg and DER activities are opposed by Dpp signaling, which promotes pleural identity. Wg and Dpp interact antagonistically at two levels. First, their expression is confined to complementary domains by mutual transcriptional repression. Second, Wg and Dpp compete directly with one another by exerting opposite effects on cell fate. DER signaling does not affect the expression of wg or dpp, indicating that it interacts with Wg and Dpp at the level of cell fate determination. Within the tergite, the requirements for Wg and DER function are roughly complementary: Wg is required mainly in the medial region, whereas DER is most important laterally. Finally, we show that Dpp signaling at the dorsal midline controls dorso-ventral patterning within the tergite by promoting pigmentation in the medial region.

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Requirements of high levels of Hedgehog signaling activity for medial-region cell fate determination in Drosophila legs: identification of pxb, a putative Hedgehog signaling attenuator gene repressed along the anterior–posterior compartment boundary

Mechanisms of Development ◽

10.1016/s0925-4773(02)00119-3 ◽

2002 ◽

Vol 116 (1-2) ◽

pp. 3-18 ◽

Cited By ~ 10

Author(s):

Mikiko Inaki ◽

Tetsuya Kojima ◽

Ryu Ueda ◽

Kaoru Saigo

Keyword(s):

Cell Fate ◽

Hedgehog Signaling ◽

Cell Fate Determination ◽

Posterior Compartment ◽

Medial Region ◽

Fate Determination ◽

Compartment Boundary ◽

Signaling Activity ◽

Anterior Posterior

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Differential effects of EGF receptor signalling on neuroblast lineages along the dorsoventral axis of the Drosophila CNS

Development ◽

10.1242/dev.125.17.3291 ◽

1998 ◽

Vol 125 (17) ◽

pp. 3291-3299 ◽

Cited By ~ 3

Author(s):

G. Udolph ◽

J. Urban ◽

G. Rusing ◽

K. Luer ◽

G.M. Technau

Keyword(s):

Cell Fate ◽

Egf Receptor ◽

Cell Lineage ◽

Dorsoventral Patterning ◽

Cell Fates ◽

Regulatory Pathways ◽

Differential Effects ◽

Receptor Signalling ◽

Cns Midline ◽

Lineage Analysis

The Drosophila ventral nerve cord derives from a stereotype population of about 30 neural stem cells, the neuroblasts, per hemineuromere. Previous experiments provided indications for inductive signals at ventral sites of the neuroectoderm that confer neuroblast identities. Using cell lineage analysis, molecular markers and cell transplantation, we show here that EGF receptor signalling plays an instructive role in CNS patterning and exerts differential effects on dorsoventral subpopulations of neuroblasts. The Drosophila EGF receptor (DER) is capable of cell autonomously specifiying medial and intermediate neuroblast cell fates. DER signalling appears to be most critical for proper development of intermediate neuroblasts and less important for medial neuroblasts. It is not required for lateral neuroblast lineages or for cells to adopt CNS midline cell fate. Thus, dorsoventral patterning of the CNS involves both DER-dependent and -independent regulatory pathways. Furthermore, we discuss the possibility that different phases of DER activation exist during neuroectodermal patterning with an early phase independent of midline-derived signals.

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EGF receptor attenuates Dpp signaling and helps to distinguish the wing and leg cell fates in Drosophila

Development ◽

10.1242/dev.127.17.3769 ◽

2000 ◽

Vol 127 (17) ◽

pp. 3769-3776 ◽

Cited By ~ 1

Author(s):

K. Kubota ◽

S. Goto ◽

K. Eto ◽

S. Hayashi

Keyword(s):

Spatial Distribution ◽

Cell Fate ◽

Receptor Tyrosine Kinase ◽

Egf Receptor ◽

Homeobox Gene ◽

Cell Fate Decision ◽

Cell Fates ◽

Dorsoventral Axis ◽

Fate Decision ◽

Number Of Cells

Wing and leg precursors of Drosophila are recruited from a common pool of ectodermal cells expressing the homeobox gene Dll. Induction by Dpp promotes this cell fate decision toward the wing and proximal leg. We report here that the receptor tyrosine kinase EGFR antagonizes the wing-promoting function of Dpp and allows recruitment of leg precursor cells from uncommitted ectodermal cells. By monitoring the spatial distribution of cells responding to Dpp and EGFR, we show that nuclear transduction of the two signals peaks at different position along the dorsoventral axis when the fates of wing and leg discs are specified and that the balance of the two signals assessed within the nucleus determines the number of cells recruited to the wing. Differential activation of the two signals and the cross talk between them critically affect this cell fate choice.

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spalt-dependent switching between two cell fates that are induced by the Drosophila EGF receptor

Development ◽

10.1242/dev.128.5.723 ◽

2001 ◽

Vol 128 (5) ◽

pp. 723-732 ◽

Cited By ~ 2

Author(s):

P.R. Elstob ◽

V. Brodu ◽

A.P. Gould

Keyword(s):

Cell Fate ◽

Animal Species ◽

Egf Receptor ◽

Zinc Finger Protein ◽

Cell Types ◽

Chordotonal Organ ◽

Egfr Signaling ◽

Cell Fates ◽

Finger Protein ◽

Distinct Cell

Signaling from the EGF receptor (EGFR) can trigger the differentiation of a wide variety of cell types in many animal species. We have explored the mechanisms that generate this diversity using the Drosophila peripheral nervous system. In this context, Spitz (SPI) ligand can induce two alternative cell fates from the dorsolateral ectoderm: chordotonal sensory organs and non-neural oenocytes. We show that the overall number of both cell types that are induced is controlled by the degree of EGFR signaling. In addition, the spalt (sal) gene is identified as a critical component of the oenocyte/chordotonal fate switch. Genetic and expression analyses indicate that the SAL zinc-finger protein promotes oenocyte formation and supresses chordotonal organ induction by acting both downstream and in parallel to the EGFR. To explain these findings, we propose a prime-and-respond model. Here, sal functions prior to signaling as a necessary but not sufficient component of the oenocyte prepattern that also serves to raise the apparent threshold for induction by SPI. Subsequently, sal-dependent SAL upregulation is triggered as part of the oenocyte-specific EGFR response. Thus, a combination of SAL in the responding nucleus and increased SPI ligand production sets the binary cell-fate switch in favour of oenocytes. Together, these studies help to explain how one generic signaling pathway can trigger the differentiation of two distinct cell types.

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The Role of Hedgehog Signaling in Adult Lung Regeneration and Maintenance

Journal of Developmental Biology ◽

10.3390/jdb7030014 ◽

2019 ◽

Vol 7 (3) ◽

pp. 14 ◽

Cited By ~ 3

Author(s):

Chaoqun Wang ◽

Monica Cassandras ◽

Tien Peng

Keyword(s):

Cell Fate ◽

Hedgehog Signaling ◽

Structural Integrity ◽

Current Knowledge ◽

Cell Fates ◽

Adult Lung ◽

Hh Signaling ◽

Key Aspects ◽

And Behavior ◽

Lung Regeneration

As a secreted morphogen, Sonic Hedgehog (SHH) determines differential cell fates, behaviors, and functions by forming a gradient of Hedgehog (Hh) activation along an axis of Hh-receptive cells during development. Despite clearly delineated roles for Hh during organ morphogenesis, whether Hh continues to regulate cell fate and behavior in the same fashion in adult organs is less understood. Adult organs, particularly barrier organs interfacing with the ambient environment, are exposed to insults that require renewal of cellular populations to maintain structural integrity. Understanding key aspects of Hh’s ability to generate an organ could translate into conceptual understanding of Hh’s ability to maintain organ homeostasis and stimulate regeneration. In this review, we will summarize the current knowledge about Hh signaling in regulating adult lung regeneration and maintenance, and discuss how alteration of Hh signaling contributes to adult lung diseases.

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Drosophila Notch receptor activity suppresses Hairless function during adult external sensory organ development.

Genetics ◽

10.1093/genetics/141.4.1491 ◽

1995 ◽

Vol 141 (4) ◽

pp. 1491-1505

Author(s):

D F Lyman ◽

B Yedvobnick

Keyword(s):

Cell Fate ◽

Daughter Cell ◽

Notch Receptor ◽

Sensory Organ ◽

Cell Fates ◽

Gain Of Function ◽

Over Expression ◽

Cell Fate Decisions ◽

Synergistic Enhancement ◽

Conditional Expression

Abstract The neurogenic Notch locus of Drosophila encodes a receptor necessary for cell fate decisions within equivalence groups, such as proneural clusters. Specification of alternate fates within clusters results from inhibitory communication among cells having comparable neural fate potential. Genetically, Hairless (H) acts as an antagonist of most neurogenic genes and may insulate neural precursor cells from inhibition. H function is required for commitment to the bristle sensory organ precursor (SOP) cell fate and for daughter cell fates. Using Notch gain-of-function alleles and conditional expression of an activated Notch transgene, we show that enhanced signaling produces H-like loss-of-function phenotypes by suppressing bristle SOP cell specification or by causing an H-like transformation of sensillum daughter cell fates. Furthermore, adults carrying Notch gain of function and H alleles exhibit synergistic enhancement of mutant phenotypes. Over-expression of an H+ transgene product suppressed virtually all phenotypes generated by Notch gain-of-function genotypes. Phenotypes resulting from over-expression of the H+ transgene were blocked by the Notch gain-of-function products, indicating a balance between Notch and H activity. The results suggest that H insulates SOP cells from inhibition and indicate that H activity is suppressed by Notch signaling.

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Histone Acetyltransferases and Stem Cell Identity

Cancers ◽

10.3390/cancers13102407 ◽

2021 ◽

Vol 13 (10) ◽

pp. 2407

Author(s):

Ruicen He ◽

Arthur Dantas ◽

Karl Riabowol

Keyword(s):

Stem Cells ◽

Stem Cell ◽

Cell Fate ◽

Epigenetic Modification ◽

Cell Types ◽

Histone Acetyltransferases ◽

Specific Cell ◽

Cell Fates ◽

Cell Identity ◽

Hematopoietic Stem

Acetylation of histones is a key epigenetic modification involved in transcriptional regulation. The addition of acetyl groups to histone tails generally reduces histone-DNA interactions in the nucleosome leading to increased accessibility for transcription factors and core transcriptional machinery to bind their target sequences. There are approximately 30 histone acetyltransferases and their corresponding complexes, each of which affect the expression of a subset of genes. Because cell identity is determined by gene expression profile, it is unsurprising that the HATs responsible for inducing expression of these genes play a crucial role in determining cell fate. Here, we explore the role of HATs in the maintenance and differentiation of various stem cell types. Several HAT complexes have been characterized to play an important role in activating genes that allow stem cells to self-renew. Knockdown or loss of their activity leads to reduced expression and or differentiation while particular HATs drive differentiation towards specific cell fates. In this study we review functions of the HAT complexes active in pluripotent stem cells, hematopoietic stem cells, muscle satellite cells, mesenchymal stem cells, neural stem cells, and cancer stem cells.

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Notch signaling coordinates ommatidial rotation in the Drosophila eye via transcriptional regulation of the EGF-Receptor ligand Argos

Scientific Reports ◽

10.1038/s41598-019-55203-w ◽

2019 ◽

Vol 9 (1) ◽

Author(s):

Yildiz Koca ◽

Benjamin E. Housden ◽

William J. Gault ◽

Sarah J. Bray ◽

Marek Mlodzik

Keyword(s):

Notch Signaling ◽

Cell Fate ◽

Planar Cell Polarity ◽

Egf Receptor ◽

Control Cell ◽

Loss Of Function ◽

Egfr Signaling ◽

Specific Expression ◽

Egfr Signaling Pathway ◽

Ommatidial Rotation

AbstractIn all metazoans, a small number of evolutionarily conserved signaling pathways are reiteratively used during development to orchestrate critical patterning and morphogenetic processes. Among these, Notch (N) signaling is essential for most aspects of tissue patterning where it mediates the communication between adjacent cells to control cell fate specification. In Drosophila, Notch signaling is required for several features of eye development, including the R3/R4 cell fate choice and R7 specification. Here we show that hypomorphic alleles of Notch, belonging to the Nfacet class, reveal a novel phenotype: while photoreceptor specification in the mutant ommatidia is largely normal, defects are observed in ommatidial rotation (OR), a planar cell polarity (PCP)-mediated cell motility process. We demonstrate that during OR Notch signaling is specifically required in the R4 photoreceptor to upregulate the transcription of argos (aos), an inhibitory ligand to the epidermal growth factor receptor (EGFR), to fine-tune the activity of EGFR signaling. Consistently, the loss-of-function defects of Nfacet alleles and EGFR-signaling pathway mutants are largely indistinguishable. A Notch-regulated aos enhancer confers R4 specific expression arguing that aos is directly regulated by Notch signaling in this context via Su(H)-Mam-dependent transcription.

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Curcumin regulates cell fate and metabolism by inhibiting hedgehog signaling in hepatic stellate cells

Laboratory Investigation ◽

10.1038/labinvest.2015.59 ◽

2015 ◽

Vol 95 (7) ◽

pp. 790-803 ◽

Cited By ~ 28

Author(s):

Naqi Lian ◽

Yuanyuan Jiang ◽

Feng Zhang ◽

Huanhuan Jin ◽

Chunfeng Lu ◽

...

Keyword(s):

Cell Fate ◽

Hepatic Stellate Cells ◽

Hedgehog Signaling ◽

Stellate Cells

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Context-dependent roles of YAP/TAZ in stem cell fates and cancer

Cellular and Molecular Life Sciences ◽

10.1007/s00018-021-03781-2 ◽

2021 ◽

Author(s):

Lucy LeBlanc ◽

Nereida Ramirez ◽

Jonghwan Kim

Keyword(s):

Stem Cell ◽

Cell Fate ◽

Control Cell ◽

Substantial Portion ◽

Cell Fates ◽

Cell Fate Decisions ◽

Cell Death Pathways ◽

Multiple Context ◽

Cancer Cell Survival ◽

Context Dependent

AbstractHippo effectors YAP and TAZ control cell fate and survival through various mechanisms, including transcriptional regulation of key genes. However, much of this research has been marked by conflicting results, as well as controversy over whether YAP and TAZ are redundant. A substantial portion of the discordance stems from their contradictory roles in stem cell self-renewal vs. differentiation and cancer cell survival vs. apoptosis. In this review, we present an overview of the multiple context-dependent functions of YAP and TAZ in regulating cell fate decisions in stem cells and organoids, as well as their mechanisms of controlling programmed cell death pathways in cancer.

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