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• W2735833462 endingPage "e1006910" @default.
• W2735833462 startingPage "e1006910" @default.
• W2735833462 abstract "Hox transcription factors specify distinct cell types along the anterior-posterior axis of metazoans by regulating target genes that modulate signaling pathways. A well-established example is the induction of Epidermal Growth Factor (EGF) signaling by an Abdominal-A (Abd-A) Hox complex during the specification of Drosophila hepatocyte-like cells (oenocytes). Previous studies revealed that Abd-A is non-cell autonomously required to promote oenocyte fate by directly activating a gene (rhomboid) that triggers EGF secretion from sensory organ precursor (SOP) cells. Neighboring cells that receive the EGF signal initiate a largely unknown pathway to promote oenocyte fate. Here, we show that Abd-A also plays a cell autonomous role in inducing oenocyte fate by activating the expression of the Pointed-P1 (PntP1) ETS transcription factor downstream of EGF signaling. Genetic studies demonstrate that both PntP1 and PntP2 are required for oenocyte specification. Moreover, we found that PntP1 contains a conserved enhancer (PntP1OE) that is activated in oenocyte precursor cells by EGF signaling via direct regulation by the Pnt transcription factors as well as a transcription factor complex consisting of Abd-A, Extradenticle, and Homothorax. Our findings demonstrate that the same Abd-A Hox complex required for sending the EGF signal from SOP cells, enhances the competency of receiving cells to select oenocyte cell fate by up-regulating PntP1. Since PntP1 is a downstream effector of EGF signaling, these findings provide insight into how a Hox factor can both trigger and potentiate the EGF signal to promote an essential cell fate along the body plan." @default.
• W2735833462 created "2017-07-21" @default.
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• W2735833462 date "2017-07-17" @default.
• W2735833462 modified "2023-10-10" @default.
• W2735833462 title "A Hox complex activates and potentiates the Epidermal Growth Factor signaling pathway to specify Drosophila oenocytes" @default.
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• W2735833462 doi "https://doi.org/10.1371/journal.pgen.1006910" @default.
• W2735833462 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/5536354" @default.
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• W2735833462 hasPublicationYear "2017" @default.
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