Evaluation of retinoids for induction of the redundant gene ABCD2 as an alternative treatment option in X-linked adrenoleukodystrophy.

[x-linked adrenoleukodystrophy]

X-linked adrenoleukodystrophy (X-ALD ), the most common peroxisomal disorder , is a clinically heterogeneous disease that can manifest as devastating inflammatory cerebral demyelination (CALD ) leading to death of affected males . Currently , the only curative treatment is allogeneic hematopoietic stem cell transplantation (HSCT ). However , HSCT is only effective when performed at an early stage because the inflammation may progress for eighteen months after HSCT . Thus , alternative treatment options able to immediately halt the progression are urgently needed . X-ALD is caused by mutations in the ABCD 1 gene , encoding the peroxisomal membrane protein ABCD 1 , resulting in impaired very long -chain fatty acid metabolism . The related ABCD 2 protein is able to functionally compensate for ABCD 1 -deficiency both in vitro and in vivo . Recently , we demonstrated that of the cell types derived from CD 34 + stem cells , predominantly monocytes but not lymphocytes are metabolically impaired in X-ALD . As ABCD 2 is virtually not expressed in these cells , we hypothesize that a pharmacological up-regulation of ABCD 2 should compensate metabolically and halt the inflammation in CALD . Retinoids are anti-inflammatory compounds known to act on ABCD 2 . Here , we investigated the capacity of selected retinoids for ABCD 2 induction in human monocytes /macrophages . In THP-1 cells , 13 -cis-retinoic acid reached the highest , fivefold , increase in ABCD 2 expression . To test the efficacy of retinoids in vivo , we analyzed ABCD 2 mRNA levels in blood cells isolated from acne patients receiving 13 -cis-retinoic acid therapy . In treated acne patients , ABCD 2 mRNA levels were comparable to pre-treatment levels in monocytes and lymphocytes . Nevertheless , when primary monocytes were in vitro differentiated into macrophages and treated with 13 -cis-retinoic acid , we observed a fourfold induction of ABCD 2 . However , the level of ABCD 2 induction obtained by retinoids alone is probably not of therapeutic relevance for X-ALD . In conclusion , our results suggest a change in promoter accessibility during macrophage differentiation allowing induction of ABCD 2 by retinoids .