The pathogenic peroxin Pex26p recruits the Pex1p-Pex6p AAA ATPase complexes to peroxisomes.

[neonatal adrenoleukodystrophy]

Peroxisomes are ubiquitous organelles with a single membrane that contain over 50 different enzymes that catalyse various metabolic pathways , including beta -oxidation and lipid synthesis . Peroxisome biogenesis disorders (PBDs ), such as Zellweger syndrome and neonatal adrenoleukodystrophy , are fatal genetic diseases that are autosomal recessive . Among the PBDs of the 12 complementation groups (CGs ), 11 associated PEX genes have been isolated . Accordingly , only the PBD pathogenic gene for CG 8 (also called CG-A ) remains unidentified . Here we have isolated human PEX 26 encoding a type II peroxisomal membrane protein of relative molecular mass 34 ,000 (M (r ) 34 K ) by using ZP 1 67 cells , a Chinese hamster ovary (CHO ) mutant cell line . Expression of PEX 26 restores peroxisomal protein import in the fibroblasts of an individual with PBD of CG 8 . This individual possesses a homozygous , inactivating pathogenic point mutation , Arg 98 Trp , in Pex 26 . Pex 6 and Pex 1 of the AAA ATPase family co -immunoprecipitate with Pex 26 . Epitope-tagged Pex 6 and Pex 1 are discernible as puncta in normal CHO -K 1 cells , but not in PEX 26 -defective cells . PEX 26 expression in ZP 1 67 cells re -establishes colocalization of Pex 6 and Pex 1 with Pex 26 , in a Pex 6 -dependent manner . Thus , Pex 26 recruits Pex 6 -Pex 1 complexes to peroxisomes .