Dilp8 and its candidate receptor, Drl, are involved in the transdetermination of the Drosophila imaginal disc

Author:

Nemoto Kazuya1,Masuko Keita12,Fuse Naoyuki1,Kurata Shoichiro1ORCID

Affiliation:

1. Graduate School of Pharmaceutical Sciences Tohoku University Sendai Japan

2. Department of Biology The University of North Carolina at Chapel Hill Chapel Hill North Carolina USA

Abstract

AbstractDrosophila imaginal disc cells can change their identity under stress conditions through transdetermination (TD). Research on TD can help elucidate the in vivo process of cell fate conversion. We previously showed that the overexpression of winged eye (wge) induces eye‐to‐wing TD in the eye disc and that an insulin‐like peptide, Dilp8, is then highly expressed in the disc. Although Dilp8 is known to mediate systemic developmental delay via the Lgr3 receptor, its role in TD remains unknown. This study showed that Dilp8 is expressed in specific cells that do not express eye or wing fate markers during Wge‐mediated TD and that the loss of Dilp8 impairs the process of eye‐to‐wing transition. Thus, Dilp8 plays a pivotal role in the cell fate conversion under wge overexpression. Furthermore, we found that instead of Lgr3, another candidate receptor, Drl, is involved in Wge‐mediated TD and acts locally in the eye disc cells. We propose a model in which Dilp8–Drl signaling organizes cell fate conversion in the imaginal disc during TD.

Funder

Japan Science Society

Mitsubishi Foundation

Publisher

Wiley

Subject

Cell Biology,Genetics

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