Identification of three distinct peroxisomal protein import defects in patients with peroxisome biogenesis disorders.

[neonatal adrenoleukodystrophy]

Zellweger syndrome , neonatal adrenoleukodystrophy , infantile Refsum 's disease , and classical rhizomelic chondrodysplasia punctata are lethal genetic disorders caused by defects in peroxisome biogenesis . We report here a characterization of the peroxisomal matrix protein import capabilities of fibroblasts from 62 of these peroxisome biogenesis disorder patients representing all ten known complementation groups . Using an immunofluorescence microscopy assay , we identified three distinct peroxisomal protein import defects among these patients . Type -1 cells have a specific inability to import proteins containing the PTS 1 peroxisomal targeting signal , type -2 cells have a specific defect in import of proteins containing the PTS 2 signal , and type -3 cells exhibit a loss of , or reduction in , the import of both PTS 1 and PTS 2 proteins . Considering that the common cellular phenotype of Zellweger syndrome , neonatal adrenoleukodystrophy and infantile Refsum 's disease has been proposed to be a complete defect in peroxisomal matrix protein import , the observation that 85 % (40 /47 ) of the type -3 cell lines imported a low but detectable amount of both PTS 1 and PTS 2 proteins was surprising . Furthermore , different cell lines with the type -3 defect exhibited a broad spectrum of different phenotypes ; some showed a complete absence of matrix protein import while others contained 50 -100 matrix protein-containing peroxisomes per cell . We also noted certain relationships between the import phenotypes and clinical diagnoses : both type -1 cell lines were from neonatal adrenoleukodystrophy patients , all 13 type -2 cell lines were from classical rhizomelic chondrodysplasia punctata patients , and the type -3 import defect was found in the vast majority of Zellweger syndrome (22 /22 ), neonatal adrenoleukodytrophy (17 /19 ), and infantile Refsum 's disease (7 /7 ) patients . Our finding that all type -1 cell lines were from the second complementation group (CG 2 ), all 13 type -2 cell lines were from CG 11 , and that cells from the eight remaining complementation groups only exhibit the type -3 defect indicates that mutations in particular genes give rise to the different types of peroxisomal protein import defects . This hypothesis is further supported by correlations between certain complementation groups and particular type -3 subphenotypes : all patient cell lines belonging to CG 3 and CG 10 showed a complete absence of peroxisomal matrix protein import while those from CG 6 , CG 7 , and CG 8 imported some peroxisomal matrix proteins . However , the fact that cell lines from within particular complementation groups (CG 1 , CG 4 ) could have different matrix protein import characteristics suggests that allelic heterogeneity also plays an important role in generating different import phenotypes in certain patients .(ABSTRACT TRUNCATED AT 400 WORDS )