Differential Expression of Cholesterol Hydroxylases in Alzheimer's Disease

Brown, James A.; Theisler, Catherine; Silberman, Simone; Magnuson, Debra J.; Gottardi-Littell, Numa; Lee, John M.; Yager, Debra; Crowley, Janet; Sambamurti, Kumar; Rahman, Mahbubur; Reiss, Allison B.; Eckman, Christopher B.; Wolozin, Benjamin

doi:10.1074/jbc.m402324200

Cited by 240 publications

(212 citation statements)

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“…There appears to be a link between CYP46A1 and AD; the CYP46A1 expression pattern in the brain and levels of 24OH-CH in the serum and cerebrospinal f luid are different in healthy people and those affected by AD (13)(14)(15)(16)(17). The association between polymorphisms in the CYP46A1 gene and susceptibility to AD was also demonstrated in a number of studies (www.alzforum.org).…”

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confidence: 90%

“…Evidence has also been obtained in cultured cells and mice that supports a role for side-chain oxysterols, including 24OH-CH, as endogenous ligands for liver X receptors, that regulate the expression of genes involved in fatty acid and cholesterol metabolism (7). 24OH-CH was also shown to inhibit the formation of amyloid ␤-peptides, a hallmark of AD, in cell cultures (14,18). Additionally, 24OH-CH is thought to induce apolipoprotein E-mediated cholesterol eff lux from astrocytes and thus to affect the progression of neurodegenerative diseases, including AD (19).…”

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confidence: 99%

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Crystal structures of substrate-bound and substrate-free cytochrome P450 46A1, the principal cholesterol hydroxylase in the brain

Mast

White²,

Björkhem

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

108

132

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By converting cholesterol to 24S-hydroxycholesterol, cytochrome P450 46A1 (CYP46A1) initiates the major pathway for cholesterol removal from the brain. Two crystal structures of CYP46A1 were determined. First is the 1.9-Å structure of CYP46A1 complexed with a high-affinity substrate cholesterol 3-sulfate (CH-3S). The second structure is that of the substrate-free CYP46A1 at 2.4-Å resolution. CH-3S is bound in the productive orientation and occupies the entire length of the banana-shaped hydrophobic active-site cavity. A unique helix B -C loop insertion (residues 116 -120) contributes to positioning cholesterol for oxygenation catalyzed by CYP46A1. A comparison with the substrate-free structure reveals substantial substrate-induced conformational changes in CYP46A1 and suggests that structurally distinct compounds could bind in the enzyme active site. In vitro assays were performed to characterize the effect of different therapeutic agents on cholesterol hydroxylase activity of purified full-length recombinant CYP46A1, and several strong inhibitors and modest coactivators of CYP46A1 were identified. Structural and biochemical data provide evidence that CYP46A1 activity could be altered by exposure to some therapeutic drugs and potentially other xenobiotics.cholesterol metabolism ͉ monooxygenase ͉ drug interactions ͉ cholesterol 3-sulfate A ccumulating evidence indicates that neurodegeneration and development of neurological disorders such as Alzheimer's disease (AD) are associated with disturbances in cholesterol homeostasis in the brain (1-5). It is also becoming increasingly clear that the conversion of cholesterol to 24S-hydroxycholesterol (24OH-CH) is an important mechanism that controls cholesterol turnover in the central nervous system (6-8). Cholesterol 24-hydroxylation is carried out by cytochrome P450 46A1 (CYP46A1) and represents the first step in the major pathway for cholesterol elimination from the brain (9-11). Unlike cholesterol, 24OH-CH can cross the blood-brain barrier and be delivered to the liver for further degradation to bile acids.Studies of CYP46A1-knockout mice indicate that the continued synthesis and turnover of cerebral cholesterol via 24-hydroxylation are necessary for memory and learning (12). There appears to be a link between CYP46A1 and AD; the CYP46A1 expression pattern in the brain and levels of 24OH-CH in the serum and cerebrospinal f luid are different in healthy people and those affected by AD (13-17). The association between polymorphisms in the CYP46A1 gene and susceptibility to AD was also demonstrated in a number of studies (www.alzforum.org). However, this association has not yet been unambiguously proven and is still under investigation. Evidence has also been obtained in cultured cells and mice that supports a role for side-chain oxysterols, including 24OH-CH, as endogenous ligands for liver X receptors, that regulate the expression of genes involved in fatty acid and cholesterol metabolism (7). 24OH-CH was also shown to inhibit the formation of amyloid ␤-peptides, a ha...

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confidence: 90%

mentioning

confidence: 99%

Crystal structures of substrate-bound and substrate-free cytochrome P450 46A1, the principal cholesterol hydroxylase in the brain

Mast

White²,

Björkhem

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

108

132

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“…In intact cells and in vitro, 24SOH can down-regulate sterol synthesis (15,16). When provided to neurons, 24SOH decreases the secretion of Aβ (17). 24SOH levels were decreased in brain samples from patients with AD (18).…”

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confidence: 99%

ACAT1 gene ablation increases 24(S)-hydroxycholesterol content in the brain and ameliorates amyloid pathology in mice with AD

Bryleva

Rogers

Chang

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

175

180

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Cholesterol metabolism has been implicated in the pathogenesis of several neurodegenerative diseases, including the abnormal accumulation of amyloid-β, one of the pathological hallmarks of Alzheimer disease (AD). Acyl-CoA:cholesterol acyltransferases (ACAT1 and ACAT2) are two enzymes that convert free cholesterol to cholesteryl esters. ACAT inhibitors have recently emerged as promising drug candidates for AD therapy. However, how ACAT inhibitors act in the brain has so far remained unclear. Here we show that ACAT1 is the major functional isoenzyme in the mouse brain. ACAT1 gene ablation (A1−) in triple transgenic (i.e., 3XTg-AD) mice leads to more than 60% reduction in full-length human APPswe as well as its proteolytic fragments, and ameliorates cognitive deficits. At 4 months of age, A1− causes a 32% content increase in 24-hydroxycholesterol (24SOH), the major oxysterol in the brain. It also causes a 65% protein content decrease in HMG-CoA reductase (HMGR) and a 28% decrease in sterol synthesis rate in AD mouse brains. In hippocampal neurons, A1− causes an increase in the 24SOH synthesis rate; treating hippocampal neuronal cells with 24SOH causes rapid declines in hAPP and in HMGR protein levels. A model is provided to explain our findings: in neurons, A1− causes increases in cholesterol and 24SOH contents in the endoplasmic reticulum, which cause reductions in hAPP and HMGR protein contents and lead to amelioration of amyloid pathology. Our study supports the potential of ACAT1 as a therapeutic target for treating certain forms of AD.Alzheimer disease | cholesterol esterification | lipid metabolism | oxysterols

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“…Various oxysterols, including 24SOH, can downregulate sterol synthesis in intact cells and in vitro (61,62), and can bind and activate the LXRs (52,63). When provided to neurons, 24SOH decreases the secretion of Abeta (64). 24SOH levels were decreased in brain samples from late stage AD patients (65), suggesting a relationship between 24SOH and AD.…”

Section: Alzheimer's Disease Amyloid Precursor Protein (App) and Chmentioning

confidence: 90%

Neuronal cholesterol esterification by ACAT1 in Alzheimer's disease

Chang

Bryleva

et al. 2010

IUBMB Life

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SummaryCholesterol has been implicated in various neurodegenerative diseases. Here we review the connection between cholesterol and Alzheimer's disease (AD), focusing on a recent study that links neuronal cholesterol esterification with biosynthesis of 24(S)-hydroxycholesterol and the fate of human amyloid precursor protein in a mouse model of AD. We also briefly evaluate the potential of ACAT1 as a drug target for AD.

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Differential Expression of Cholesterol Hydroxylases in Alzheimer's Disease

Cited by 240 publications

References 40 publications

Crystal structures of substrate-bound and substrate-free cytochrome P450 46A1, the principal cholesterol hydroxylase in the brain

Crystal structures of substrate-bound and substrate-free cytochrome P450 46A1, the principal cholesterol hydroxylase in the brain

ACAT1 gene ablation increases 24(S)-hydroxycholesterol content in the brain and ameliorates amyloid pathology in mice with AD

Neuronal cholesterol esterification by ACAT1 in Alzheimer's disease

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