The key genes, phosphoproteins, processes, and pathways affected by efavirenz‐activated CYP46A1 in the amyloid‐decreasing paradigm of efavirenz treatment

The key genes, phosphoproteins, processes, and pathways affected by efavirenz‐activated CYP46A1 in the amyloid‐decreasing paradigm of efavirenz treatment

ABSTRACT Efavirenz (EFV) is an anti‐HIV drug, and cytochrome P450 46A1 (CYP46A1) is the major brain cholesterol hydroxylase. Previously, we discovered that EFV activates CYP46A1 and improves behavioral performance in 5XFAD mice, an Alzheimer's disease model. Herein, the unbiased omics and other...

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Veröffentlicht in:The FASEB journal 2019-08, Vol.33 (8), p.8782-8798
Hauptverfasser: Petrov, Alexey M., Mast, Natalia, Li, Yong, Pikuleva, Irina A.
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Sprache:eng
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24‐hydroxycholesterol
5XFAD mice
Alkynes
Alzheimer disease
Animals
Benzoxazines - pharmacology
Brain - drug effects
Brain - metabolism
Cholesterol 24-Hydroxylase - metabolism
Cyclopropanes
Cytochrome P-450 Enzyme Inducers - pharmacology
Metabolic Networks and Pathways
Mice
Mice, Inbred C57BL
Signal Transduction
Transcriptome
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container_issue 8
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container_title The FASEB journal
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creator Petrov, Alexey M.
Mast, Natalia
Li, Yong
Pikuleva, Irina A.
description ABSTRACT Efavirenz (EFV) is an anti‐HIV drug, and cytochrome P450 46A1 (CYP46A1) is the major brain cholesterol hydroxylase. Previously, we discovered that EFV activates CYP46A1 and improves behavioral performance in 5XFAD mice, an Alzheimer's disease model. Herein, the unbiased omics and other approaches were used to study 5XFAD mice in the amyloid‐decreasing paradigm of CYP46A1 activation by EFV. These approaches revealed increases in the brain levels of postsynaptic density protein 95, gephyrin, synaptophysin, synapsin, glial fibrillary acidic protein, and CYP46A1 and documented altered expression and phosphorylation of 66 genes and 77 proteins, respectively. The data obtained pointed to EFV effects at the synaptic level, plasmin‐depended amyloid clearance, inflammation and microglia phenotype, oxidative stress and cellular hypoxia, autophagy and ubiquitin‐proteasome systems as well as apoptosis. These effects could be realized in part via changes in the Ca2+‐, small GTPase, and catenin signaling. A model is proposed, in which CYP46A1‐dependent lipid raft rearrangement and subsequent decrease of protein phosphorylation are central in EFV effects and explain behavioral improvements in EFV‐treated 5XFAD mice.—Petrov, A. M., Mast, N., Li, Y., Pikuleva, I. A. The key genes, phosphoproteins, processes, and pathways affected by efavirenz‐activated CYP46A1 in the amyloid‐decreasing paradigm of efavirenz treatment. FASEB J. 33, 8782–8798 (2019). www.fasebj.org
doi_str_mv 10.1096/fj.201900092R
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Previously, we discovered that EFV activates CYP46A1 and improves behavioral performance in 5XFAD mice, an Alzheimer's disease model. Herein, the unbiased omics and other approaches were used to study 5XFAD mice in the amyloid‐decreasing paradigm of CYP46A1 activation by EFV. These approaches revealed increases in the brain levels of postsynaptic density protein 95, gephyrin, synaptophysin, synapsin, glial fibrillary acidic protein, and CYP46A1 and documented altered expression and phosphorylation of 66 genes and 77 proteins, respectively. The data obtained pointed to EFV effects at the synaptic level, plasmin‐depended amyloid clearance, inflammation and microglia phenotype, oxidative stress and cellular hypoxia, autophagy and ubiquitin‐proteasome systems as well as apoptosis. These effects could be realized in part via changes in the Ca2+‐, small GTPase, and catenin signaling. A model is proposed, in which CYP46A1‐dependent lipid raft rearrangement and subsequent decrease of protein phosphorylation are central in EFV effects and explain behavioral improvements in EFV‐treated 5XFAD mice.—Petrov, A. M., Mast, N., Li, Y., Pikuleva, I. A. The key genes, phosphoproteins, processes, and pathways affected by efavirenz‐activated CYP46A1 in the amyloid‐decreasing paradigm of efavirenz treatment. 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Previously, we discovered that EFV activates CYP46A1 and improves behavioral performance in 5XFAD mice, an Alzheimer's disease model. Herein, the unbiased omics and other approaches were used to study 5XFAD mice in the amyloid‐decreasing paradigm of CYP46A1 activation by EFV. These approaches revealed increases in the brain levels of postsynaptic density protein 95, gephyrin, synaptophysin, synapsin, glial fibrillary acidic protein, and CYP46A1 and documented altered expression and phosphorylation of 66 genes and 77 proteins, respectively. The data obtained pointed to EFV effects at the synaptic level, plasmin‐depended amyloid clearance, inflammation and microglia phenotype, oxidative stress and cellular hypoxia, autophagy and ubiquitin‐proteasome systems as well as apoptosis. These effects could be realized in part via changes in the Ca2+‐, small GTPase, and catenin signaling. A model is proposed, in which CYP46A1‐dependent lipid raft rearrangement and subsequent decrease of protein phosphorylation are central in EFV effects and explain behavioral improvements in EFV‐treated 5XFAD mice.—Petrov, A. M., Mast, N., Li, Y., Pikuleva, I. A. The key genes, phosphoproteins, processes, and pathways affected by efavirenz‐activated CYP46A1 in the amyloid‐decreasing paradigm of efavirenz treatment. 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Previously, we discovered that EFV activates CYP46A1 and improves behavioral performance in 5XFAD mice, an Alzheimer's disease model. Herein, the unbiased omics and other approaches were used to study 5XFAD mice in the amyloid‐decreasing paradigm of CYP46A1 activation by EFV. These approaches revealed increases in the brain levels of postsynaptic density protein 95, gephyrin, synaptophysin, synapsin, glial fibrillary acidic protein, and CYP46A1 and documented altered expression and phosphorylation of 66 genes and 77 proteins, respectively. The data obtained pointed to EFV effects at the synaptic level, plasmin‐depended amyloid clearance, inflammation and microglia phenotype, oxidative stress and cellular hypoxia, autophagy and ubiquitin‐proteasome systems as well as apoptosis. These effects could be realized in part via changes in the Ca2+‐, small GTPase, and catenin signaling. 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subjects 24‐hydroxycholesterol
5XFAD mice
Alkynes
Alzheimer disease
Animals
Benzoxazines - pharmacology
Brain - drug effects
Brain - metabolism
Cholesterol 24-Hydroxylase - metabolism
Cyclopropanes
Cytochrome P-450 Enzyme Inducers - pharmacology
Metabolic Networks and Pathways
Mice
Mice, Inbred C57BL
Signal Transduction
Transcriptome
title The key genes, phosphoproteins, processes, and pathways affected by efavirenz‐activated CYP46A1 in the amyloid‐decreasing paradigm of efavirenz treatment
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