Brain injury induces cholesterol 24-hydroxylase (Cyp46) expression in glial cells in a time-dependent manner

Smiljanić, Kosara; Lavrnja, Irena; Djordjevic, Aleksandra Mladenovic; Ruždijić, Sabera; Stojiljković, Mirjana; Peković, Sanja; Kanazir, Selma

doi:10.1007/s00418-010-0718-6

Cited by 25 publications

(24 citation statements)

References 54 publications

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“…CYP46A1 expression would be an adaptive response of the retina to changes in cholesterol levels. Similar activation of CYP46A1 in microglia was already reported in the brain in response to injury (Smiljanic et al, 2010).…”

Section: Cholesterol-24s-hydroxylase 24s-hydroxycholesterol and Neursupporting

confidence: 84%

Cholesterol and ocular pathologies: focus on the role of cholesterol-24S-hydroxylase in cholesterol homeostasis

Fourgeux

Martine

Gambert-Nicot

et al. 2015

OCL

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-The retina is responsible for coding the light stimulus into a nervous signal that is transferred to the brain via the optic nerve. The retina is formed by the association of the neurosensory retina and the retinal pigment epithelium that is supported by Bruch's membrane. Both the physical and metabolic associations between these partners are crucial for the functioning of the retina, by means of nutrient intake and removal of the cell and metabolic debris from the retina. Dysequilibrium are involved in the aging processes and pathologies such as age-related macular degeneration, the leading cause of visual loss after the age of 50 years in Western countries. The retina is composed of several populations of cells including glia that is involved in cholesterol biosynthesis. Cholesterol is the main sterol in the retina. It is present as free form in cells and as esters in Bruch's membrane. Accumulation of cholesteryl esters has been associated with aging of the retina and impairment of the retinal function. Under dietary influence and in situ synthesized, the metabolism of cholesterol is regulated by cell interactions, including neurons and glia via cholesterol-24S-hydroxylase. Several pathophysiological associations with cholesterol and its metabolism can be suggested, especially in relation to glaucoma and age-related macular degeneration.Keywords: Retina / lipid / cholesterol / glaucoma / age-related macular degeneration / aging Résumé -Cholestérol et pathologies oculaires : focus sur le rôle de la cholestérol-24S-hydroxylase dans l'homéostasie du cholestérol. La rétine est le tissu neurosensoriel de l'oeil qui assure la transduction visuelle, c'est-à-dire le codage de l'information lumineuse en influx nerveux. Le terme de rétine regroupe l'association de la rétine neurale et de l'épithélium pigmentaire rétinien qui repose sur la membrane de Bruch. L'association physique de ces deux partenaires et leurs interactions métaboliques sont des éléments indispensables au bon fonctionnement de la rétine, à la fois en termes d'apport en nutriments et de maintien de l'homéostasie. Des dérèglements de ces équilibres sont associés au vieillissement et à des pathologies comme la dégénérescence maculaire liée à l'âge, première cause de malvoyance après 50 ans dans les populations occidentales. La rétine neurale est composée de plusieurs types cellulaires, incluant la glie dont le rôle est crucial pour la biosynthèse du cholestérol dans la rétine. Le cholestérol est le principal stérol de la rétine. Il y est présent dans la cellule essentiellement en tant que cholestérol libre et d'esters de cholestérol au niveau extracellulaire dans la membrane de Bruch. L'accumulation de ces esters de cholestérol à ce niveau est un marqueur du vieillissement de la rétine et de la diminution de sa fonction. Sous influence alimentaire et synthétisé localement, le cholestérol est également régulé via les interactions entre populations cellulaires de la rétine, comme entre neurones et glie, via la cholestérol-24S-hydroxylase. Plusieur...

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Section: Cholesterol-24s-hydroxylase 24s-hydroxycholesterol and Neursupporting

confidence: 84%

Cholesterol and ocular pathologies: focus on the role of cholesterol-24S-hydroxylase in cholesterol homeostasis

Fourgeux

Martine

Gambert-Nicot

et al. 2015

OCL

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“…Previously, we and others have shown that activated macrophages/microglia express CYP46A1 in traumatic brain injury 26, 46 . Additionally, it was suggested that infiltrating macrophages express CYP46A1 during EAE 45 .…”

Section: Discussionmentioning

confidence: 80%

“…CYP46A1 expression was found in many types of neurons, where a majority of CYP46A1 expression was exclusively associated to neuronal somata, with lower levels found in dendrites 23, 26, 44, 56 . This study also revealed a strong CYP46A1 immunoreactivity in the neuronal somata in the grey matter at the onset and the end of EAE, which was lowered at the peak of disease probably due to neuronal degeneration.…”

Section: Discussionmentioning

confidence: 99%

“…Similarly, CYP46A1 positive astrocytes, surrounding the lesion site were detected after the hippocampal kainate injury 25 . In our previous study 26 , we have reported that traumatic brain injury induces the long-lasting upregulation of CYP46A1 protein expression at the lesion site, which was attributed to microglia and astrocytes in a time-dependent manner.…”

Section: Introductionmentioning

confidence: 91%

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Expression profiles of cholesterol metabolism-related genes are altered during development of experimental autoimmune encephalomyelitis in the rat spinal cord

Lavrnja

Smiljanić

Savić

et al. 2017

Sci Rep

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Increased evidence suggests that dysregulation of cholesterol metabolism may be a key event contributing to progression of multiple sclerosis (MS). Using an experimental autoimmune encephalomyelitis (EAE) model of MS we revealed specific changes in the mRNA and protein expression of key molecules involved in the maintaining of cholesterol homeostasis in the rat spinal cord: 3-hydroxy-3-methylglutaryl-coenzyme-A reductase (HMGCR), apolipoprotein E (ApoE) and cholesterol 24-hydroxylase (CYP46A1) during the course of disease. The presence of myelin lipid debris was seen only at the peak of EAE in demyelination loci being efficiently removed during the recovery period. Since CYP46A1 is responsible for removal of cholesterol excess, we performed a detailed profiling of CYP46A1 expression and revealed regional and temporal specificities in its distribution. Double immunofluorescence staining demonstrated CYP46A1 localization with neurons, infiltrated macrophages, microglia and astrocytes in the areas of demyelination, suggesting that these cells play a role in cholesterol turnover in EAE. We propose that alterations in the regulation of cholesterol metabolism at the onset and peak of EAE may add to the progression of disease, while during the recovery period may have beneficial effects contributing to the regeneration of myelin sheath and restoration of neuronal function.

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“…As so far only few studies demonstrated atypical Cyp46 expression in astrocytes under certain circumstances [e.g. human frontal cortex- (Brown et al 2004), and advanced Alzheimer disease- (Bogdanovic et al 2001)], Smiljanic et al (2010) were interested to study cellular and temporal pattern of Cyp46 expression in the context of traumatic brain injury (TBI), a widespread cause of death and major source of adult disability. Employing a rat TBI model the authors found longlasting neuronal and glial Cyp46 expression at the lesion site, indicating that TBI-induced production of damaged cell membranes elicits wide-spead Cyp46 expression to re-establish brain cholesterol homeostasis required for a glial scar formation.…”

Section: Central Nervous Systemmentioning

confidence: 99%

Histochemistry and cell biology: the annual review 2010

Hübner

Efthymiadis

2011

Histochem Cell Biol

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This review summarizes recent advances in histochemistry and cell biology which complement and extend our knowledge regarding various aspects of protein functions, cell and tissue biology, employing appropriate in vivo model systems in conjunction with established and novel approaches. In this context several non-expected results and discoveries were obtained which paved the way of research into new directions. Once the reader embarks on reading this review, it quickly becomes quite obvious that the studies contribute not only to a better understanding of fundamental biological processes but also provide use-oriented aspects that can be derived therefrom.

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Brain injury induces cholesterol 24-hydroxylase (Cyp46) expression in glial cells in a time-dependent manner

Cited by 25 publications

References 54 publications

Cholesterol and ocular pathologies: focus on the role of cholesterol-24S-hydroxylase in cholesterol homeostasis

Cholesterol and ocular pathologies: focus on the role of cholesterol-24S-hydroxylase in cholesterol homeostasis

Expression profiles of cholesterol metabolism-related genes are altered during development of experimental autoimmune encephalomyelitis in the rat spinal cord

Histochemistry and cell biology: the annual review 2010

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