CYP46A1, the rate-limiting enzyme for cholesterol degradation, is neuroprotective in Huntington's disease

被引:129
作者
Boussicault, Lydie [1 ]
Alves, Sandro [2 ,3 ]
Lamaziere, Antonin [4 ]
Planques, Anabelle [1 ,5 ]
Heck, Nicolas [1 ]
Moumne, Lara [1 ]
Despres, Gaetan [4 ]
Bolte, Susanne [6 ]
Hu, Amelie [1 ,7 ]
Pages, Christiane [1 ]
Galvan, Laurie [8 ]
Piguet, Francoise [9 ]
Aubourg, Patrick [2 ,3 ]
Cartier, Nathalie [2 ,3 ]
Caboche, Jocelyne [1 ]
Betuing, Sandrine [1 ]
机构
[1] Univ Paris 06, Sorbonne Univ,CNRS UMR 8246, Neuronal Signaling & Gene Regulat,UMR S 1130, Neurosci Paris Seine,Inst Biol Paris Seine,INSERM, F-75005 Paris, France
[2] MIRCEN CEA, INSERM, U1169, F-91400 Orsay, France
[3] Univ Paris Saclay, Univ Paris Sud, F-91400 Orsay, France
[4] Univ Paris 06, Sorbonne Univ, CNRS UMR LBM 7203, Lab Mass Spectrometry,INSERM ERL 1157,CHU St Anto, F-75012 Paris, France
[5] Coll France, INSERM CNRS 7141, Ctr Interdisciplinary Res Biol, Dev & Neuropharmacol, F-75231 Paris, France
[6] Univ Paris 06, Sorbonne Univ, Inst Biol Paris Seine CNRS FR, Cellular Imaging Facil, Paris, France
[7] Univ Libre Bruxelles, Lab Expt Neurol, Brussels, Belgium
[8] Univ Calif Los Angeles, Semel Inst, Los Angeles, CA USA
[9] IGBMC, Dept Translat Med & Neurogenet, INSERM U964, UMR CNRS UdS 7104, BP 10142, F-67404 Illkirch Graffenstaden, France
来源
BRAIN | 2016年 / 139卷
关键词
CYP46A1; cholesterol; striatum; Huntington's disease; neuroprotection; PLASMA; 24S-HYDROXYCHOLESTEROL; BIOSYNTHESIS PATHWAY; PROTEIN AGGREGATION; BRAIN CHOLESTEROL; MOUSE MODEL; CELL-DEATH; IN-VITRO; GENE; METABOLISM; DYSFUNCTION;
D O I
10.1093/brain/awv384
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
Dysregulation of cholesterol synthesis is implicated in Huntington's disease. Boussicault et al. show that expression of CYP46A1, the rate-limiting enzyme in cholesterol degradation, is reduced in patients and a mouse model. Restoration of CYP46A1 re-establishes normal cholesterol levels and is neuroprotective, suggesting that targeting cholesterol degradation may have therapeutic potential.Dysregulation of cholesterol synthesis is implicated in Huntington's disease. Boussicault et al. show that expression of CYP46A1, the rate-limiting enzyme in cholesterol degradation, is reduced in patients and a mouse model. Restoration of CYP46A1 re-establishes normal cholesterol levels and is neuroprotective, suggesting that targeting cholesterol degradation may have therapeutic potential.Huntington's disease is an autosomal dominant neurodegenerative disease caused by abnormal polyglutamine expansion in huntingtin (Exp-HTT) leading to degeneration of striatal neurons. Altered brain cholesterol homeostasis has been implicated in Huntington's disease, with increased accumulation of cholesterol in striatal neurons yet reduced levels of cholesterol metabolic precursors. To elucidate these two seemingly opposing dysregulations, we investigated the expression of cholesterol 24-hydroxylase (CYP46A1), the neuronal-specific and rate-limiting enzyme for cholesterol conversion to 24S-hydroxycholesterol (24S-OHC). CYP46A1 protein levels were decreased in the putamen, but not cerebral cortex samples, of post-mortem Huntington's disease patients when compared to controls. Cyp46A1 mRNA and CYP46A1 protein levels were also decreased in the striatum of the R6/2 Huntington's disease mouse model and in SThdhQ111 cell lines. In vivo, in a wild-type context, knocking down CYP46A1 expression in the striatum, via an adeno-associated virus-mediated delivery of selective shCYP46A1, reproduced the Huntington's disease phenotype, with spontaneous striatal neuron degeneration and motor deficits, as assessed by rotarod. In vitro, CYP46A1 restoration protected SThdhQ111 and Exp-HTT-expressing striatal neurons in culture from cell death. In the R6/2 Huntington's disease mouse model, adeno-associated virus-mediated delivery of CYP46A1 into the striatum decreased neuronal atrophy, decreased the number, intensity level and size of Exp-HTT aggregates and improved motor deficits, as assessed by rotarod and clasping behavioural tests. Adeno-associated virus-CYP46A1 infection in R6/2 mice also restored levels of cholesterol and lanosterol and increased levels of desmosterol. In vitro, lanosterol and desmosterol were found to protect striatal neurons expressing Exp-HTT from death. We conclude that restoring CYP46A1 activity in the striatum promises a new therapeutic approach in Huntington's disease.
引用
收藏
页码:953 / 970
页数:18
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