Lobe and Serrate are required for cell survival during early eye development in Drosophila

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Organogenesis involves an initial surge of cell proliferation, leading to differentiation. This is followed by cell death in order to remove extra cells. During early development, there is little or no cell death. However, there is a lack of information concerning the genes required for survival during the early cell-proliferation phase. Here, we show that Lobe (L) and the Notch (N) ligand Serrate (Ser), which are both involved in ventral eye growth, are required for cell survival in the early eye disc. We observed that the loss-of-ventraleye phenotype in L or Ser mutants is due to the induction of cell death and the upregulation of secreted Wingless (Wg). This loss-of-ventral-eye phenotype can be rescued by (i) increasing the levels of cell death inhibitors, (ii) reducing the levels of Hid-Reaper-Grim complex, or (iii) reducing canonical Wg signaling components. Blocking Jun-N-terminal kinase (JNK) signaling, which can induce caspase-independent cell death, significantly rescued ventral eye loss in L or Ser mutants. However, blocking both caspase-dependent cell death and JNK signaling together showed stronger rescues of the L- or Ser-mutant eye at a 1.5-fold higher frequency. This suggests that L or Ser loss-of-function triggers both caspase-dependent and -independent cell death. Our studies thus identify a mechanism responsible for cell survival in the early eye.
Publisher
COMPANY OF BIOLOGISTS LTD
Issue Date
2006-12
Language
English
Article Type
Article
Keywords

JNK-DEPENDENT APOPTOSIS; MORPHOGENETIC FURROW; RETINAL DIFFERENTIATION; SIGNALING PATHWAYS; ALAGILLE-SYNDROME; HEAD INVOLUTION; CASPASE DRONC; IAP FUNCTION; WINGLESS; DEATH

Citation

DEVELOPMENT, v.133, no.23, pp.4771 - 4781

ISSN
0950-1991
DOI
10.1242/dev.02686
URI
http://hdl.handle.net/10203/90322
Appears in Collection
BS-Journal Papers(저널논문)
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