Neurotoxic Microglial Activation via IFNγ-Induced Nrf2 Reduction Exacerbating Alzheimer's Disease

Microglial neuroinflammation appears to be neuroprotective in the early pathological stage, yet neurotoxic, which often precedes neurodegeneration in Alzheimer's disease (AD). However, it remains unclear how the microglial activities transit to the neurotoxic state during AD progression, due to complex neuron-glia interactions. Here, the mechanism of detrimental microgliosis in AD by employing 3D human AD mini-brains, brain tissues of AD patients, and 5XFAD mice is explored. In the human and animal AD models, amyloid-beta (A beta)-overexpressing neurons and reactive astrocytes produce interferon-gamma (IFN gamma) and excessive oxidative stress. IFN gamma results in the downregulation of mitogen-activated protein kinase (MAPK) and the upregulation of Kelch-like ECH-associated Protein 1 (Keap1) in microglia, which inactivate nuclear factor erythroid-2-related factor 2 (Nrf2) and sensitize microglia to the oxidative stress and induces a proinflammatory microglia via nuclear factor kappa B (NF kappa B)-axis. The proinflammatory microglia in turn produce neurotoxic nitric oxide and proinflammatory mediators exacerbating synaptic impairment, phosphorylated-tau accumulation, and discernable neuronal loss. Interestingly, recovering Nrf2 in the microglia prevents the activation of proinflammatory microglia and significantly blocks the tauopathy in AD minibrains. Taken together, it is envisioned that IFN gamma-driven Nrf2 downregulation in microglia as a key target to ameliorate AD pathology. Mechanisms of detrimental microgliosis in Alzheimer's disease are explored. Interferon-gamma (IFN gamma) upregulates Kelch-like ECH-associated Protein 1 (Keap1) in microglia, which inactivates nuclear factor erythroid-2-related factor 2 (Nrf2) and sensitizes microglia to the oxidative stress, resulting in the transition of proinflammatory microglia via nuclear factor kappa B (NF kappa B)-axis. The proinflammatory microglia in tern exacerbate synaptic impairment, phosphorylated-tau accumulation, and decernable neuronal loss at the end. image