Histone deacetylase inhibitor upregulates peroxisomal fatty acid oxidation and inhibits apoptotic cell death in abcd1-deficient glial cells.

[x-linked adrenoleukodystrophy]

In X-ALD , mutation /deletion of ALD gene (ABCD 1 ) and the resultant very long chain fatty acid (VLCFA ) derangement has dramatically opposing effects in astrocytes and oligodendrocytes . While loss of Abcd 1 in astrocytes produces a robust inflammatory response , the oligodendrocytes undergo cell death leading to demyelination in X-linked adrenoleukodystrophy (X-ALD ). The mechanisms of these distinct pathways in the two cell types are not well understood . Here , we investigated the effects of Abcd 1 -knockdown and the subsequent alteration in VLCFA metabolism in human U 87 astrocytes and rat B 12 oligodendrocytes . Loss of Abcd 1 inhibited peroxisomal β-oxidation activity and increased expression of VLCFA synthesizing enzymes , elongase of very long chain fatty acids (ELOVLs ) (1 and 3 ) in both cell types . However , higher induction of ELOVL 's in Abcd 1 -deficient B 12 oligodendrocytes than astrocytes suggests that ELOVL pathway may play a prominent role in oligodendrocytes in X-ALD . While astrocytes are able to maintain the cellular homeostasis of anti-apoptotic proteins , Abcd 1 -deletion in B 12 oligodendrocytes downregulated the anti-apototic (Bcl-2 and Bcl-x L ) and cell survival (phospho-Erk 1 /2 ) proteins , and upregulated the pro-apoptotic proteins (Bad , Bim , Bax and Bid ) leading to cell loss . These observations provide insights into different cellular signaling mechanisms in response to Abcd 1 -deletion in two different cell types of CNS . The apoptotic responses were accompanied by activation of caspase-3 and caspase-9 suggesting the involvement of mitochondrial -caspase-9 -dependent mechanism in Abcd 1 -deficient oligodendrocytes . Treatment with histone deacetylase (HDAC ) inhibitor suberoylanilide hydroxamic acid (SAHA ) corrected the VLCFA derangement both in vitro and in vivo , and inhibited the oligodendrocytes loss . These observations provide a proof-of principle that HDAC inhibitor SAHA may have a therapeutic potential for X-ALD .