Caffeic acid phenethyl ester induces adrenoleukodystrophy (Abcd2) gene in human X-ALD fibroblasts and inhibits the proinflammatory response in Abcd1/2 silenced mouse primary astrocytes.

[x-linked adrenoleukodystrophy]

X-linked adrenoleukodystrophy (X-ALD ) is a peroxisomal disorder caused by mutations in the ABCD 1 gene . Accumulation of very long chain fatty acids (VLCFA ) that have been attributed to reduced peroxisomal VLCFA β-oxidation activity are the hallmark of the disease . Overexpression of ABCD 2 gene , the closest homolog of ABCD 1 , has been shown to compensate for ABCD 1 , thus correcting the VLCFA derangement . The accumulation of VLCFA leads to a neuroinflammatory disease process associated with demyelination of the cerebral white matter . The present study underlines the importance of caffeic acid phenethyl ester (CAPE ) in inducing the expression of ABCD 2 (ALDRP ), and normalizing the peroxisomal β-oxidation as well as the levels of saturated and monounsaturated VLCFAs in cultured human skin fibroblasts of X-ALD patients . The expression of ELOVL 1 , the single elongase catalyzing the synthesis of both saturated VLCFA (C 2 6 :0 ) and mono-unsaturated VLCFA (C 2 6 :1 ), was also reduced by CAPE treatment . Importantly , CAPE upregulated Abcd 2 expression and peroxisomal β-oxidation and lowered the VLCFA levels in Abcd 1 -deficient U 87 astrocytes and B 12 oligodendrocytes . In addition , using Abcd 1 /Abcd 2 -silenced mouse primary astrocytes we examined the effects of CAPE in VLCFA-induced inflammatory response . CAPE treatment decreased the inflammatory response as the expression of inducible nitric oxide synthase , inflammatory cytokine , and activation of NF-κB in Abcd 1 /Abcd 2 -silenced mouse primary astrocytes was reduced . The observations indicate that CAPE corrects both the metabolic disease of VLCFA as well as secondary inflammatory disease ; therefore , it may be a potential drug candidate to be tested for X-ALD therapy in humans .