Phenotype-genotype relationships in PEX10-deficient peroxisome biogenesis disorder patients.

[neonatal adrenoleukodystrophy]

The peroxisome biogenesis disorders (PBD ) are characterized by neural , hepatic , and renal deficiencies , severe mental retardation , and are often lethal . These disorders are genetically and phenotypically heterogeneous and are caused by defective peroxisomal protein import and decreased peroxisomal metabolic function . Mutations in PEX 10 have been identified in patients from complementation group 7 (CG 7 ) of the PBDs and we report here an analysis of the genotypes and phenotypes of PEX 10 -deficient patients . All four PEX 10 -deficient Zellweger Syndrome (ZS ) patients were found to have nonsense , frameshift , or splice site mutations that remove large portions of the PEX 10 coding region . In contrast , a more mildly affected PEX 10 -deficient neonatal adrenoleukodystrophy patient expressed a PEX 10 allele with a missense mutation , H 290 Q , affecting the C-terminal zinc-binding domain of the PEX 10 product . These results support the hypothesis that severe , loss -of-function mutations in PEX genes cause more severe clinical phenotypes , whereas mildly affected PBD patients have PEX gene mutations that retain residual function . To quantitate the effects of the PEX 10 mutations identified here and elsewhere we employed a functional complementation assay . Surprisingly , we observed that nonsense and frameshift mutations predicted to delete the C-terminal 2 /3 (R 125 X ) or 1 /3 (c .704 insA ) of the protein displayed nearly normal PEX 10 activity . Even more surprising , we found that the unexpectedly high PEX 10 activity displayed by these cDNAs could be eliminated by removing or mutating segments of the PEX 10 cDNA downstream of the mutations . Although these results demonstrate serious flaws in the PEX 10 functional complementation assay , they do suggest that the C-terminal zinc-binding domain is critical for PEX 10 function .