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Drep-2 is a novel synaptic protein important for learning and memory
ISSN
2050-084X
Date Issued
2014
Author(s)
Andlauer, Till F. M.
Scholz-Kornehl, Sabrina
Tian, Rui
Kirchner, Marieluise
Babikir, Husam A.
Depner, Harald
Loll, Bernhard
Quentin, Christine
Gupta, Varun K.
Dipt, Shubham
Cressy, Michael
Selbach, Matthias
Schwaerzel, Martin
Sigrist, Stephan J.
DOI
10.7554/eLife.03895
Abstract
CIDE-N domains mediate interactions between the DNase Dff40/CAD and its inhibitor Dff45/ICAD. In this study, we report that the CIDE-N protein Drep-2 is a novel synaptic protein important for learning and behavioral adaptation. Drep-2 was found at synapses throughout the Drosophila brain and was strongly enriched at mushroom body input synapses. It was required within Kenyon cells for normal olfactory short-and intermediate-term memory. Drep-2 colocalized with metabotropic glutamate receptors (mGluRs). Chronic pharmacological stimulation of mGluRs compensated for drep-2 learning deficits, and drep-2 and mGluR learning phenotypes behaved non-additively, suggesting that Drep 2 might be involved in effective mGluR signaling. In fact, Drosophila fragile X protein mutants, shown to benefit from attenuation of mGluR signaling, profited from the elimination of drep-2. Thus, Drep-2 is a novel regulatory synaptic factor, probably intersecting with metabotropic signaling and translational regulation.
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