Peroxisome biogenesis disorders with prolonged survival: phenotypic expression in a cohort of 31 patients.

[neonatal adrenoleukodystrophy]

The peroxisome biogenesis disorders (PBDs ) with generalized peroxisomal dysfunction include Zellweger syndrome (ZS ), neonatal adrenoleukodystrophy (NALD ), and infantile Refsum disease (IRD ). There is clinical , biochemical , and genetic overlap among the three phenotypes , also known as Zellweger spectrum disorders . Clinical distinctions between the phenotypes are not sharply defined . Only limited sources are available to serve as a background for prognosis in PBD , especially in case of prolonged survival . We delineated the natural history of 31 PBD patients (age 1 .2 -24 years ) through systematic clinical and biochemical investigations . We excluded classical ZS from our study , and included all patients with a biochemically confirmed generalized peroxisomal disorder over 1 year of age , irrespective of the previously diagnosed phenotype . The initial clinical suspicion , age at diagnosis , growth , development , neurological symptoms , organ involvements , and survival are summarized . Common to all patients were cognitive and motor dysfunction , retinopathy , sensorineural hearing impairment , and hepatic involvement . Many patients showed postnatal growth failure , 10 patients displayed hyperoxaluria of whom 4 had renal stones . Motor skills ranged from sitting with support to normal gait . Speech development ranged from non-verbal expression to grammatical speech and comprehensive reading . The neurodevelopmental course was variable with stable course , rapid decline with leukodystrophy , spinocerebellar syndrome , and slow decline over a wide range of faculties as outcome profiles . At the molecular level , 21 patients had mutations in the PEX 1 gene . The two most common PEX 1 mutations were the G 8 43 D (c .2528 G-->A ) missense and the c .2097 insT frameshift mutation . Patients having the G 8 43 D /G 8 43 D or the G 8 43 D /c .2097 insT genotypes were compared . Patients homozygous for G 8 43 D generally had a better developmental outcome . However , one patient who was homozygous for the "mild " G 8 43 D mutation had an early lethal disease , whereas two other patients had a phenotype overlapping with the G 8 43 D /c .2097 insT group . This indicates that next to the PEX 1 genotype other yet unknown factors determine the ultimate phenotype .