Immunoproteasome deficiency alters microglial cytokine response and improves cognitive deficits in Alzheimer’s disease-like APPPS1 mice

被引:0
作者
Lisa K. Wagner
Kate E. Gilling
Eileen Schormann
Peter M. Kloetzel
Frank L. Heppner
Elke Krüger
Stefan Prokop
机构
[1] Charité – Universitätsmedizin Berlin,Department of Neuropathology
[2] Brigham and Women’s Hospital,Present Address: Department of Neurology
[3] Harvard Medical School,Institute of Biochemistry
[4] Charité – Universitätsmedizin Berlin,Present Address: Institute of Medical Biochemistry and Molecular Biology
[5] Cluster of Excellence,Present Address: Department of Pathology and Laboratory Medicine
[6] NeuroCure,undefined
[7] Berlin Institute of Health (BIH),undefined
[8] University Medicine Greifswald,undefined
[9] Hospital of the University of Pennsylvania,undefined
来源
Acta Neuropathologica Communications | / 5卷
关键词
Proteasome; Immunoproteasome; Microglia; Inflammation; Alzheimer’s disease;
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摘要
The immunoproteasome (iP) represents a specialized type of proteasomes, which plays an important role in the clearance of oxidant-damaged proteins under inflammatory and pathological conditions determining the outcome of various diseases. In Alzheimer’s disease (AD)-like APPPS1 mice Aβ-deposition is paralleled by iP upregulation, most likely mediated through type I interferon induction. To define the impact of increased iP expression we crossed APPPS1 mice with mice deficient in the iP subunit LMP7 resulting in impaired iP function. While LMP7 deficient APPPS1 mice showed no major change in cerebral Aβ-pathology, we observed an altered cytokine response in microglia isolated from LMP7 deficient APPPS1 mice compared to LMP7 expressing APPPS1 control mice. The altered microglial cytokine profile upon iP deficiency in the presence of extracellular Aβ-pathology was associated with an improvement of Aβ-associated cognitive deficits typically present in APPPS1 mice. Our findings suggest a role for iP in the regulation of the innate immune response towards extracellular Aβ-pathology and indicate that inhibition of iP function can modulate the cognitive phenotype upon overexpression of Aβ.
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