6533b7cefe1ef96bd1256d57

RESEARCH PRODUCT

Activités cytotoxiques et pro-oxydantes d'acides gras à très longue chaîne sur des oligodendrocytes murins sauvages et déficients en Abcd1 et Acox1 : application à la physiopathologie de l'X-ALD et de la P-NALD

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description

X-ALD and P-NALD are two rare, peroxisomal metabolic and neurodegenerative diseases. ABCD1 and ACOX1 are known to be responsible for X-ALD and P-NALD, respectively. The actively demyelinating lesions in CNS, exhibited signs of oxidative stress and cell death. The accumulation of VLCFA in plasma and tissue is the biochemical common hallmark to both diseases. First, we characterized a murine oligodendrocytes cell line 158N to use it as a model. This 158N cell line which has characteristics of mature oligodendrocytes (expression of myelin proteins MOG, MBP, PLP), has also functional peroxisomes with Abcd1 and Acox1 proteins. Then, we studied the cytotoxic and pro-oxidative effects of VLCFA (C24: 0 and C26: 0), and the effects of in vitro silencing of the Abcd1 and Acox1 genes by siRNA on the redox balance and cell death. Effects of VLCFA on the biophysical characteristics of cytoplasmic membrane were also evaluated. Moreover, markers of oxidative stress were researched on plasma of patients with different forms of X-ALD. In vitro, we showed that the accumulation of VLCFA on 158N cells induced overproduction of reactive oxygen and nitrogen species and a disruption of antioxidant defense systems (catalase, SOD, GSH). This was accompanied by lipid peroxidation, protein carbonylation and degradation of DNA. The extinction of Abcd1 and Acox1 by siRNA increased the production of radical species and potentialized the oxidative stress induced by VLCFA. On plasma of patients with different forms X-ALD, compared to healthy subjects, we showed an accumulation of lipid peroxidation products (7-hydroxycholesterol, HODEs). The rate of these two products is correlated with the severity of the disease: CCALD> AMN> Addison> ACALD. The VLCFA also induce cell death on 158N by a non-apoptotic process. This cell death is characterized by: a rapid increased of intracellular Ca2+ level, pH decrease, a loss of mitochondrial transmembrane potential associated with structural changes of mitochondria, a destabilization of lysosomes, and formation of autophagic vacuoles. The VLCFA also disrupt the membrane fluidity. Furthermore, VLCFA do not affect the expression of myelin major proteins PLP and MBP. This work highlighted a direct link between VLCFA accumulation, oxidative stress and induction of cell death involving lysosomes. Abcd1 and Acox1 deficiency promotes oxidative stress. In agreement with results obtained in vitro, the detection of markers of lipid peroxidation in the plasma of X-ALD patients favors the hypothesis of an involvement of oxidative stress in this pathology.