Loss of AMP-activated protein kinase in X-linked adrenoleukodystrophy patient-derived fibroblasts and lymphocytes.

[adrenomyeloneuropathy]

X-Adrenoleukodystrophy (X-ALD ) is a peroxisomal disorder characterized by accumulation of very -long -chain (VLC ) fatty acids , which induces inflammatory disease and alterations in cellular redox , both of which are reported to play a role in the pathogenesis of the severe form of the disease (childhood cerebral ALD ). While the mutation defect in ABCD 1 gene is common to all forms of X-ALD it fails to account for the spectrum of phenotypic variability seen in X-ALD patients , strongly suggesting a role for as yet unidentified modifier gene (s ). Here we report , for the first time , loss of AMP -activated protein kinase alpha 1 (AMPKÎ±1 ) in patient-derived fibroblasts and lymphocytes of the severe cerebral form of X-ALD (ALD ), and not in the milder adrenomyeloneuropathy (AMN ) form . Decrease in AMPK was observed at both protein and mRNA levels . AMPK loss in ALD patient-derived fibroblasts was associated with increased ubiquitination . Using the Seahorse Bioscience XF (e )96 Flux Analyzer for measuring the mitochondrial oxygen consumption and extracellular acidification rate we show that ALD patient-derived fibroblasts have a significantly lower "metabolic state " than AMN fibroblasts . Unstimulated ALD patient-derived lymphocytes had significantly higher proinflammatory gene expression . Selective AMPK loss represents a novel physiopathogenic factor in X-ALD disease mechanism . Strategies aimed at upregulating /recovering AMPK levels might have beneficial therapeutic effects in X-ALD .

Diseases
Validation

Diseases presenting "yet unidentified modifier gene" symptom

adrenomyeloneuropathy

x-linked adrenoleukodystrophy

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