Abstract
In autophagy long-lived proteins, protein aggregates or damaged organelles are engulfed by vesicles called autophagosomes prior to lysosomal degradation. Autophagy dysfunction is a hallmark of several neurodegenerative diseases in which misfolded proteins or dysfunctional mitochondria accumulate. Excessive autophagy can also exacerbate brain injury under certain conditions. In this review, we provide specific examples to illustrate the critical role played by autophagy in pathological conditions affecting the brain and discuss potential therapeutic implications. We show how a singular type of autophagy-dependent cell death termed autosis has attracted attention as a promising target for improving outcomes in perinatal asphyxia and hypoxic-ischaemic injury to the immature brain. We provide evidence that autophagy inhibition may be protective against radiotherapy-induced damage to the young brain. We describe a specialized form of macroautophagy of therapeutic relevance for motoneuron and neuromuscular diseases, known as chaperone-assisted selective autophagy, in which heat shock protein B8 is used to deliver aberrant proteins to autophagosomes. We summarize studies pinpointing mitophagy mediated by the serine/threonine kinase PINK1 and the ubiquitin-protein ligase Parkin as a mechanism potentially relevant to Parkinson's disease, despite debate over the physiological conditions in which it is activated in organisms. Finally, with the example of the autophagy-inducing agent rilmenidine and its discrepant effects in cell culture and mouse models of motor neuron disorders, we illustrate the importance of considering aspects such a disease stage and aggressiveness, type of insult and load of damaged or toxic cellular components, when choosing the appropriate drug, timepoint and duration of treatment.
Highlights
Given that both oxidative stress and excitotoxicity are documented to contribute to hypoxic-ischaemic injury (HI) (Khoshnam et al 2017), studies of the possible recruitment of autophagy to stroke were a logical extension of our work
Defective chaperone-assisted selective autophagy (CASA) has been linked to motor neuron disorders such as amyotrophic lateral sclerosis (ALS) and spinal bulbar and muscular atrophy (SBMA) and mitophagy is suspected to be impaired in specific forms of Parkinson’s disease, as well as in other neurodegenerative diseases, according to studies not discussed in this review (Wong & Holzbaur 2014, Cai & Jeong 2020)
From an assessment of the current state of knowledge, it is clear that we are still some distance from a holistic understanding of how autophagy is recruited in different brain diseases and in which cases it is merely associated with cell death rather than mediating or even causing cell death (Klionsky et al 2016)
Summary
MND, Motor neuron disease MDV, mitochondria-derived vesicles MiT/TFE, transcription factors of the microphtalmia/transcription factor E family Mfn, Mitofusin 2 NDs, neurodegenerative diseases NEF, nucleotide exchange factor NLRP3, nucleotide-binding domain-like receptor protein 3 OMM, outer mitochondrial membrane PCD, programmed cell death PD, Parkinson’s disease polyQ, elongated glutamine repeats SBMA, spinal bulbar and muscular atrophy siRNA, short interfering RNA SOD1, superoxide dismutase 1 TDP-43, TAR DNA binding protein of 43 kDa TFEB, transcription factor EB TOM, translocase of outer mitochondrial membrane UPRmt, mitochondrial unfolded protein response
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