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Publication : Adiponectin alleviated Alzheimer-like pathologies via autophagy-lysosomal activation.

First Author  He K Year  2021
Journal  Aging Cell Volume  20
Issue  12 Pages  e13514
PubMed ID  34775673 Mgi Jnum  J:336625
Mgi Id  MGI:6841041 Doi  10.1111/acel.13514
Citation  He K, et al. (2021) Adiponectin alleviated Alzheimer-like pathologies via autophagy-lysosomal activation. Aging Cell 20(12):e13514
abstractText  Adiponectin (APN) deficiency has also been associated with Alzheimer-like pathologies. Recent studies have illuminated the importance of APN signaling in reducing Abeta accumulation, and the Abeta elimination mechanism remains rudimentary. Therefore, we aimed to elucidate the APN role in reducing Abeta accumulation and its associated abnormalities by targeting autophagy and lysosomal protein changes. To assess, we performed a combined pharmacological and genetic approach while using preclinical models and human samples. Our results demonstrated that the APN level significantly diminished in the plasma of patients with dementia and 5xFAD mice (6 months old), which positively correlated with Mini-Mental State Examination (MMSE), and negatively correlated with Clinical Dementia Rating (CDR), respectively. APN deficiency accelerated cognitive impairment, Abeta deposition, and neuroinflammation in 5xFAD mice (5xFAD*APN KO), which was significantly rescued by AdipoRon (AR) treatment. Furthermore, AR treatment also markedly reduced Abeta deposition and attenuated neuroinflammation in APP/PS1 mice without altering APP expression and processing. Interestingly, AR treatment triggered autophagy by mediating AMPK-mTOR pathway signaling. Most importantly, APN deficiency dysregulated lysosomal enzymes level, which was recovered by AR administration. We further validated these changes by proteomic analysis. These findings reveal that APN is the negative regulator of Abeta deposition and its associated pathophysiologies. To eliminate Abeta both extra- and intracellular deposition, APN contributes via the autophagic/lysosomal pathway. It presents a therapeutic avenue for AD therapy by targeting autophagic and lysosomal signaling.
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