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Cell-Nonautonomous Effects of dFOXO/DAF-16 in Aging

Nazif Alic, Jennifer M. A. Tullet, Teresa Niccoli, Susan Broughton, Matthew P. Hoddinott, Cathy Slack, David Gems, Linda Partridge

Cell Reports · 2014 · ▲ 60 citations

Abstract

Drosophila melanogaster and Caenorhabditis elegans each carry a single representative of the Forkhead box O (FoxO) family of transcription factors, dFOXO and DAF-16, respectively. Both are required for lifespan extension by reduced insulin/Igf signaling, and their activation in key tissues can extend lifespan. Aging of these tissues may limit lifespan. Alternatively, FoxOs may promote longevity cell nonautonomously by signaling to themselves (FoxO to FoxO) or other factors (FoxO to other) in distal tissues. Here, we show that activation of dFOXO and DAF-16 in the gut/fat body does not require dfoxo/daf-16 elsewhere to extend lifespan. Rather, in Drosophila, activation of dFOXO in the gut/fat body or in neuroendocrine cells acts on other organs to promote healthy aging by signaling to other, as-yet-unidentified factors. Whereas FoxO-to-FoxO signaling appears to be required for metabolic homeostasis, our results pinpoint FoxO-to-other signaling as an important mechanism through which localized FoxO activity ameliorates aging.

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Provenance

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OpenAlex
DOI
10.1016/j.celrep.2014.01.015
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2026-06-30 MST

Cite this

APA
Alic, N., Tullet, J.M.A., Niccoli, T., Broughton, S., Hoddinott, M.P., Slack, C., Gems, D., &amp; Partridge, L. (2014). Cell-Nonautonomous Effects of dFOXO/DAF-16 in Aging. <em>Cell Reports</em>. https://doi.org/10.1016/j.celrep.2014.01.015
Vancouver
Alic N, Tullet JMA, Niccoli T, Broughton S, Hoddinott MP, Slack C, et al. Cell-Nonautonomous Effects of dFOXO/DAF-16 in Aging. Cell Reports. 2014. doi:10.1016/j.celrep.2014.01.015.
BibTeX
@article{nazif2014CellNo, title = {Cell-Nonautonomous Effects of dFOXO/DAF-16 in Aging}, author = {Nazif Alic and Jennifer M. A. Tullet and Teresa Niccoli and Susan Broughton and Matthew P. Hoddinott and Cathy Slack and David Gems and Linda Partridge}, journal = {Cell Reports}, year = {2014}, doi = {10.1016/j.celrep.2014.01.015}, }

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