Cells (Nov 2022)

Further Extension of Lifespan by <i>Unc-43/CaMKII</i> and <i>Egl-8/PLCβ</i> Mutations in Germline-Deficient <i>Caenorhabditis elegans</i>

  • Hildegard I. D. Mack,
  • Laura G. Buck,
  • Sonja Skalet,
  • Jennifer Kremer,
  • Hao Li,
  • Elisabeth K. M. Mack

DOI
https://doi.org/10.3390/cells11223527
Journal volume & issue
Vol. 11, no. 22
p. 3527

Abstract

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Reduction of insulin/insulin-like growth factor 1 (IGF1) signaling (IIS) promotes longevity across species. In the nematode Caenorhabditis elegans, ablation of germline stem cells (GSCs) and activity changes of the conserved signaling mediators unc-43/CaMKII (calcium/calmodulin-dependent kinase type II) and egl-8/PLCβ (phospholipase Cβ) also increase lifespan. Like IIS, these pathways depend on the conserved transcription factor daf-16/FOXO for lifespan extension, but how they functionally interact is unknown. Here, we show that altered unc-43/egl-8 activity further increases the lifespan of long-lived GSC-deficient worms, but not of worms that are long-lived due to a strong reduction-of-function mutation in the insulin/IGF1-like receptor daf-2. Additionally, we provide evidence for unc-43 and, to a lesser extent, egl-8 modulating the expression of certain collagen genes, which were reported to be dispensable for longevity of these particular daf-2 mutant worms, but not for other forms of longevity. Together, these results provide new insights into the conditions and potential mechanisms by which CaMKII- and PLCβ-signals modulate C. elegans lifespan.

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