Insulin signaling in the aging of healthy and proteotoxically stressed mechanosensory neurons

0 avis

Insulin signaling in the aging of healthy and proteotoxically stressed mechanosensory neurons

Archive ouverte

International audience. Insulin signaling is central to cellular metabolism and organismal aging. However, the role of insulin signaling in natural and proteotoxically stressed aging neurons has yet to be fully described. We studied aging of Caenorbaditis elegans mechanosensory neurons expressing a neurotoxic expanded polyglutamine transgene (polyQ128), or lacking this proteotoxicity stressor (polyQ0), under conditions in which the insulin signaling pathway was disrupted by RNA interference (RNAi). We describe specific changes in lifespan, mechanosensory neuronal morphologies, and mechansensory function following RNAi treatment targeting the insulin signaling pathway. Overall, we confirmed that transcription factor DAF-16 is neuroprotective in the proteotoxically stressed model, though not strikingly in the naturally aging model. Decreased insulin signaling through daf-2 RNAi improved mechanosensory function in both models and decreased protein aggregation load in polyQ128, yet showed opposing effects on accumulation of neuronal aberrations in both strains. Decreased daf-2 signaling slightly enhanced mechanosensation while greatly enhancing branching of the mechanosensory neuron axons and dendrites in polyQ0 animals, suggesting that branching is an adaptive response in natural aging. These effects in polyQ0 did not appear to involve DAF-16, suggesting the existence of a non-canonical DAF-2 pathway for the modulation of morphological adaptation. However, in polyQ128 animals, decreased daf-2 signaling significantly enhanced mechanosensation while decreasing neuronal aberrations. Unlike other interventions that reduce the strength of insulin signaling, daf-2 RNAi dramatically redistributed large polyQ128 aggregates to the cell body, away from neuronal processes. Our results suggest that insulin signaling strength can differentially affect specific neurons aging naturally or under proteotoxic stress

Langue: en

Consulter en ligne

Consulter le document

Suggestions

Du même auteur

Morphological remodeling of C. elegans neurons during aging is modified by compromised protein homeostasis

Archive ouverte | Vayndorf, Elena M. | CCSD

International audience. Understanding cellular outcomes, such as neuronal remodeling, that are common to both healthy and diseased aging brains is essential to the development of successful brain aging strategies. H...

C-elegans neurons jettison protein aggregates and mitochondria under neurotoxic stress

Archive ouverte | Melentijevic, Ilija | CCSD

International audience. The toxicity of misfolded proteins and mitochondrial dysfunction are pivotal factors that promote age-associated functional neuronal decline and neurodegenerative disease(1,2). Accordingly, n...

The Wnt Receptor Ryk Reduces Neuronal and Cell Survival Capacity by Repressing FOXO Activity During the Early Phases of Mutant Huntingtin Pathogenicity

Archive ouverte | Tourette, Cendrine | CCSD

International audience. The Wnt receptor Ryk is an evolutionary-conserved protein important during neuronal differentiation through several mechanisms, including c-secretase cleavage and nuclear translocation of its...

Chargement des enrichissements...