Impaired very long-chain acyl-CoA β-oxidation in human X-linked adrenoleukodystrophy fibroblasts is a direct consequence of ABCD1 transporter dysfunction.

[zellweger syndrome]

X-linked adrenoleukodystrophy (X-ALD ), an inherited peroxisomal disorder , is caused by mutations in the ABCD 1 gene encoding the peroxisomal ATP-binding cassette (ABC ) transporter ABCD 1 (adrenoleukodystrophy protein , ALDP ). Biochemically , X-ALD is characterized by an accumulation of very long -chain fatty acids and partially impaired peroxisomal β-oxidation . In this study , we used primary human fibroblasts from X-ALD and Zellweger syndrome patients to investigate the peroxisomal β-oxidation defect . Our results show that the degradation of C 2 6 :0 -CoA esters is as severely impaired as degradation of unesterified very long -chain fatty acids in X-ALD and is abolished in Zellweger syndrome . Interestingly , the β-oxidation rates for both C 2 6 :0 -CoA and C 2 2 :0 -CoA were similarly affected , although C 2 2 :0 does not accumulate in patient fibroblasts . Furthermore , we show that the β-oxidation defect in X-ALD is directly caused by ABCD 1 dysfunction as blocking ABCD 1 function with a specific antibody reduced β-oxidation to levels observed in X-ALD fibroblasts . By quantification of mRNA and protein levels of the peroxisomal ABC transporters and by blocking with specific antibodies , we found that residual β-oxidation activity toward C 2 6 :0 -CoA in X-ALD fibroblasts is mediated by ABCD 3 , although the efficacy of ABCD 3 appeared to be much lower than that of ABCD 1 . Finally , using isolated peroxisomes , we show that β-oxidation of C 2 6 :0 -CoA is independent of additional CoA but requires a cytosolic factor of >10 -kDa molecular mass that is resistant to N-ethylmaleimide and heat inactivation . In conclusion , our findings in human cells suggest that , in contrast to yeast cells , very long -chain acyl-CoA esters are transported into peroxisomes by ABCD 1 independently of additional synthetase activity .