An in vivo RNA interference screen identifies gene networks controlling Drosophila melanogaster blood cell homeostasis

<p>Abstract</p> <p>Background</p> <p>In metazoans, the hematopoietic system plays a key role both in normal development and in defense of the organism. In Drosophila, the cellular immune response involves three types of blood cells: plasmatocytes, crystal cells and lamellocytes. This last cell type is barely present in healthy larvae, but its production is strongly induced upon wasp parasitization or in mutant contexts affecting larval blood cell homeostasis. Notably, several zygotic mutations leading to melanotic mass (or "tumor") formation in larvae have been associated to the deregulated differentiation of lamellocytes. To gain further insights into the gene regulatory network and the mechanisms controlling larval blood cell homeostasis, we conducted a tissue-specific loss of function screen using hemocyte-specific Gal4 drivers and <it>UAS-dsRNA </it>transgenic lines.</p> <p>Results</p> <p>By targeting around 10% of the Drosophila genes, this <it>in vivo </it>RNA interference screen allowed us to recover 59 melanotic tumor suppressor genes. In line with previous studies, we show that melanotic tumor formation is associated with the precocious differentiation of stem-cell like blood progenitors in the larval hematopoietic organ (the lymph gland) and the spurious differentiation of lamellocytes. We also find that melanotic tumor formation can be elicited by defects either in the fat body, the embryo-derived hemocytes or the lymph gland. In addition, we provide a definitive confirmation that lymph gland is not the only source of lamellocytes as embryo-derived plasmatocytes can differentiate into lamellocytes either upon wasp infection or upon loss of function of the Friend of GATA cofactor U-shaped.</p> <p>Conclusions</p> <p>In this study, we identify 55 genes whose function had not been linked to blood cell development or function before in Drosophila. Moreover our analyses reveal an unanticipated plasticity of embryo-derived plasmatocytes, thereby shedding new light on blood cell lineage relationship, and pinpoint the Friend of GATA transcription cofactor U-shaped as a key regulator of the plasmatocyte to lamellocyte transformation.</p

LRCH Proteins: A Novel Family of Cytoskeletal Regulators

Background: Comparative genomics has revealed an unexpected level of conservation for gene products across the evolution of animal species. However, the molecular function of only a few proteins has been investigated experimentally, and the role of many animal proteins still remains unknown. Here we report the characterization of a novel family of evolutionary conserved proteins, which display specific features of cytoskeletal scaffolding proteins, referred to as LRCHs. Principal Findings: Taking advantage of the existence of a single LRCH gene in flies, dLRCH, we explored its function in cultured cells, and show that dLRCH act to stabilize the cell cortex during cell division. dLRCH depletion leads to ectopic cortical blebs and alters positioning of the mitotic spindle. We further examined the consequences of dLRCH deletion throughout development and adult life. Although dLRCH is not essential for cell division in vivo, flies lacking dLRCH display a reduced fertility and fitness, particularly when raised at extreme temperatures. Conclusion/Significance: These results support the idea that some cytoskeletal regulators are important to buffer environmental variations and ensure the proper execution of basic cellular processes, such as the control of cell shape

Caractérisation fonctionnelle du rôle du gène Dmoesine au cours de l'ovogénèse chez la drosophile

TOULOUSE3-BU Sciences (315552104) / SudocSudocFranceF

A mild cold stress that increases resistance to heat lowers FOXO translocation in Drosophila melanogaster.

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Hypergravity increases resistance to heat in dFOXO Drosophila melanogaster mutants and can lower FOXO translocation in wild-type males

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Les facteurs OvoL

Des avancées majeures révèlent l’hétérogénéité intra-tumorale des cancers d’origine épithéliale, incluant des cellules initiatrices de tumeurs qui ressemblent aux cellules souches adultes. Les cellules souches normales et tumorales partagent en effet leur plasticité entre phénotypes épithéliaux et mésenchymateux, progressant par une série d’états intermédiaires, réversibles. Si un cœur de régulateurs (Snail, Zeb, …) est bien connu pour déclencher la transition épithélio-mésenchymateuse (TEM), les facteurs OvoL/Shavenbaby sont récemment apparus comme des stabilisateurs épithéliaux. La balance entre facteurs pro-TEM et OvoL pourrait ainsi réguler la plasticité phénotypique et le potentiel métastatique des tumeurs. Nous abordons cette question chez la drosophile, un modèle pour disséquer in vivo la fonction de Shavenbaby. Nos travaux montrent que Shavenbaby est un régulateur clé de l’homéostasie des cellules souches adultes. Shavenbaby est indispensable à leur survie, agissant en interaction directe avec la voie Hippo pour protéger les cellules souches de la mort cellulaire programmée

Modeling Cancers in Drosophila

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The Hippo pathway regulates apical-domain size independently of its growth-control function

The Hippo pathway, identified in Drosophila and conserved in vertebrates, regulates tissue growth by promoting cell cycle exit and apoptosis. In addition to their well-characterised overproliferation phenotype, adult Drosophila epithelial cells mutant for the kinases Hippo and Warts have hypertrophic apical domains. Here we examine the molecular basis of this apical hypertrophy and its impact on cell proliferation. In the wing imaginal disc epithelium, we observe increased staining for members of the apical polarity complexes aPKC and Crumbs as well as adherens junction components when Hippo activity is compromised, while basolateral markers are not affected. This increase in apical proteins is correlated with a hypertrophy of the apical domain and adherens junctions. The cell surface localisation of the Notch receptor is also increased in mutant clones, opening the possibility that aberrant receptor signalling may participate in overgrowth of hpo-deficient tissue. Interestingly, however, although the polarity determinant Crumbs is required for the accumulation of apical proteins, this does not appear to significantly contribute to the overproliferation defect elicited by loss of Hippo signalling. Therefore, Hippo signalling controls growth and apical domain size by distinct mechanisms