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  4. Functional analysis and regulation of nuclear import of dorsal during the immune response in Drosophila
 
research article

Functional analysis and regulation of nuclear import of dorsal during the immune response in Drosophila

Lemaitre, B.  
•
Meister, M.
•
Govind, S.
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1995
The EMBO journal

In addition to its function in embryonic development, the NF-kappa B/rel-related gene dorsal (dl) of Drosophila is expressed in larval and adult fat body where its RNA expression is enhanced upon injury. Injury also leads to a rapid nuclear translocation of dl from the cytoplasm in fat body cells. Here we present data which strongly suggest that the nuclear localization of dl during the immune response is controlled by the Toll signaling pathway, comprising gene products that participate in the intracellular part of the embryonic dorsoventral pathway. We also report that in mutants such as Toll or cactus, which exhibit melanotic tumor phenotypes, dl is constitutively nuclear. Together, these results point to a potential link between the Toll signaling pathway and melanotic tumor induction. Although dl has been shown previously to bind to kappa B-related motifs within the promoter of the antibacterial peptide coding gene diptericin, we find that injury-induced expression of diptericin can occur in the absence of dl. Furthermore, the melanotic tumor phenotype of Toll and cactus is not dl dependent. These data underline the complexity of the Drosophila immune response. Finally, we observed that like other rel proteins, dl can control the level of its own transcription.

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Type
research article
DOI
10.1002/j.1460-2075.1995.tb07029.x
Web of Science ID

WOS:A1995QF71800013

PubMed ID

7859742

Author(s)
Lemaitre, B.  
Meister, M.
Govind, S.
Georgel, P.
Steward, R.
Reichhart, J. M.
Hoffmann, J. A.
Date Issued

1995

Publisher

Nature Publishing Group

Published in
The EMBO journal
Volume

14

Issue

3

Start page

536

End page

45

Subjects

Antimicrobial Cationic Peptides

•

Drosophila Proteins

•

Insect Proteins

•

Receptors

•

Cell Surface

•

Transcription Factors

Editorial or Peer reviewed

REVIEWED

Written at

OTHER

EPFL units
UPLEM  
Available on Infoscience
September 17, 2010
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/53787
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