Cerebrospinal fluid matrix metalloproteinases are elevated in cerebral adrenoleukodystrophy and correlate with MRI severity and neurologic dysfunction.

[x-linked adrenoleukodystrophy]

X-linked adrenoleukodystrophy results from mutations in the ABCD 1 gene disrupting the metabolism of very -long -chain fatty acids . The most serious form of ALD , cerebral adrenoleukodystrophy (cALD ), causes neuroinflammation and demyelination . Neuroimaging in cALD shows inflammatory changes and indicates blood -brain -barrier (BBB ) disruption . We hypothesize that disruption may occur through the degradation of the extracellular matrix defining the BBB by matrix metalloproteinases (MMPs ). MMPs have not been evaluated in the setting of cALD .We used a multiplex assay to correlate the concentration of MMPs in cerebrospinal fluid and plasma to the severity of brain inflammation as determined by the ALD MRI (Loes ) score and the neurologic function score . There were significant elevations of MMP 2 , MMP 9 , MMP 10 , TIMP 1 , and total protein in the CSF of boys with cALD compared to controls . Levels of MMP 10 , TIMP 1 , and total protein in CSF showed significant correlation [p <0 .05 for each with pre-transplant MRI Loes Loes scores (R (2 ) = 0 .34 , 0 .20 , 0 .55 respectively ). Levels of TIMP 1 and total protein in CSF significantly correlated with pre-transplant neurologic functional scores (R (2 ) = 0 .22 and 0 .48 respectively ), and levels of MMP 10 and total protein in CSF significantly correlated with one -year post-transplant functional scores (R (2 ) = 0 .38 and 0 .69 ). There was a significant elevation of MMP 9 levels in plasma compared to control , but did not correlate with the MRI or neurologic function scores .M MPs were found to be elevated in the CSF of boys with cALD and may mechanistically contribute to the breakdown of the blood -brain -barrier . MMP concentrations directly correlate to radiographic and clinical neurologic severity . Interestingly , increased total protein levels showed superior correlation to MRI score and neurologic function score before and at one year after transplant .