Literature DB >> 23325760

Notch cooperates with Lozenge/Runx to lock haemocytes into a differentiation programme.

Ana Terriente-Felix1, Jinghua Li, Stephanie Collins, Amy Mulligan, Ian Reekie, Fred Bernard, Alena Krejci, Sarah Bray.   

Abstract

The diverse functions of Notch signalling imply that it must elicit context-specific programmes of gene expression. With the aim of investigating how Notch drives cells to differentiate, we have used a genome-wide approach to identify direct Notch targets in Drosophila haemocytes (blood cells), where Notch promotes crystal cell differentiation. Many of the identified Notch-regulated enhancers contain Runx and GATA motifs, and we demonstrate that binding of the Runx protein Lozenge (Lz) is required for enhancers to be competent to respond to Notch. Functional studies of targets, such as klumpfuss (ERG/WT1 family) and pebbled/hindsight (RREB1 homologue), show that Notch acts both to prevent the cells adopting alternate cell fates and to promote morphological characteristics associated with crystal cell differentiation. Inappropriate activity of Klumpfuss perturbs the differentiation programme, resulting in melanotic tumours. Thus, by acting as a master regulator, Lz directs Notch to activate selectively a combination of target genes that correctly locks cells into the differentiation programme.

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Year:  2013        PMID: 23325760      PMCID: PMC3557782          DOI: 10.1242/dev.086785

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


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