Abstract
Autophagy is a conserved pathway that plays a key role in cell homeostasis in normal settings, as well as abnormal and stress conditions. Autophagy dysfunction is found in various neurodegenerative diseases, although it remains unclear whether autophagy impairment is a contributor or consequence of neurodegeneration. Axonal injury is an acute neuronal stress that triggers autophagic responses in an age-dependent manner. In this study, we investigate the injury-triggered autophagy response in a C. elegans model of tauopathy. We found that transgenic expression of pro-aggregant Tau, but not the anti-aggregant Tau, abolished axon injury-induced autophagy activation, resulting in a reduced axon regeneration capacity. Furthermore, axonal trafficking of autophagic vesicles were significantly reduced in the animals expressing pro-aggregant F3ΔK280 Tau, indicating that Tau aggregation impairs autophagy regulation. Importantly, the reduced number of total or trafficking autophagic vesicles in the tauopathy model was not restored by the autophagy activator rapamycin. Loss of PTL-1, the sole Tau homologue in C. elegans, also led to impaired injury-induced autophagy activation, but with an increased basal level of autophagic vesicles. Therefore, we have demonstrated that Tau aggregation as well as Tau depletion both lead to disruption of injury-induced autophagy responses, suggesting that aberrant protein aggregation or microtubule dysfunction can modulate autophagy regulation in neurons after injury.
Highlights
Autophagy is a lysosome-mediated intracellular catabolic process that is a central component in stress response [1]
We have recently reported that axon injury activates autophagy, which is required for effective axon regeneration through limiting Notch signaling [30]
To test whether injury-induced autophagy is affected by protein aggregation, we investigated autophagy dynamics in a transgenic Tau aggregation model that expresses chromosomally integrated versions of the amyloidogenic F3DK280 fragment of human Tau derived from the repeat domain of TauDK280 [31,33,34]
Summary
Autophagy is a lysosome-mediated intracellular catabolic process that is a central component in stress response [1]. It plays a conserved role in maintaining cellular homeostasis by degrading dysfunctional proteins, lipids, and organelles through an autophagosome-lysosome pathway [2]. In response to increased energy demands of cells, autophagy provides metabolic substrates, making autophagy a cytoprotective mechanism [3]. Autophagy is initiated with the formation of a double membrane structure around cellular substances, followed by the formation of autophagosome that fuses with a lysosome. The engulfed substances are degraded and recycled back to the cell as amino and fatty acids [5]
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