Current Biology

Current Biology

Volume 28, Issue 5, 5 March 2018, Pages 817-823.e3
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Drosophila Full-Length Amyloid Precursor Protein Is Required for Visual Working Memory and Prevents Age-Related Memory Impairment

https://doi.org/10.1016/j.cub.2018.01.077Get rights and content
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Highlights

  • Visual working memory is particularly sensitive to age-related memory impairment (AMI)

  • Reducing secretase-mediated processing of the Drosophila APP protein ameliorates AMI

  • Levels of unprocessed full-length Drosophila APP protein are decreased in old flies

  • Full-length Drosophila APP inhibits signaling by the neuronal-adhesion molecule FASII

Summary

The β-amyloid precursor protein (APP) plays a central role in the etiology of Alzheimer’s disease (AD). However, its normal physiological functions are still unclear. APP is cleaved by various secretases whereby sequential processing by the β- and γ-secretases produces the β-amyloid peptide that is accumulating in plaques that typify AD. In addition, this produces secreted N-terminal sAPPβ fragments and the APP intracellular domain (AICD). Alternative cleavage by α-secretase results in slightly longer secreted sAPPα fragments and the identical AICD. Whereas the AICD has been connected with transcriptional regulation, sAPPα fragments have been suggested to have a neurotrophic and neuroprotective role [1]. Moreover, expression of sAPPα in APP-deficient mice could rescue their deficits in learning, spatial memory, and long-term potentiation [2]. Loss of the Drosophila APP-like (APPL) protein impairs associative olfactory memory formation and middle-term memory that can be rescued with a secreted APPL fragment [3]. We now show that APPL is also essential for visual working memory. Interestingly, this short-term memory declines rapidly with age, and this is accompanied by enhanced processing of APPL in aged flies. Furthermore, reducing secretase-mediated proteolytic processing of APPL can prevent the age-related memory loss, whereas overexpression of the secretases aggravates the aging effect. Rescue experiments confirmed that this memory requires signaling of full-length APPL and that APPL negatively regulates the neuronal-adhesion molecule Fasciclin 2. Overexpression of APPL or one of its secreted N termini results in a dominant-negative interaction with the FASII receptor. Therefore, our results show that specific memory processes require distinct APPL products.

Keywords

age-related memory impairment
Drosophila
working memory
Amyloid Precursor Protein
Fasciclin 2
visual orientation
central complex

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3

Present address: Department of Oncology, University of Alberta, Katz Group Centre, 114th Street and 87th Avenue, Edmonton, AB T6G 2E1, Canada

4

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