Peroxisome biogenesis disorders: molecular basis for impaired peroxisomal membrane assembly: in metabolic functions and biogenesis of peroxisomes in health and disease.

[zellweger syndrome]

Peroxisome is a single -membrane organelle in eukaryotes . The functional importance of peroxisomes in humans is highlighted by peroxisome-deficient peroxisome biogenesis disorders (PBDs ) such as Zellweger syndrome (ZS ). Gene defects of peroxins required for both membrane assembly and matrix protein import are identified : ten mammalian pathogenic peroxins for ten complementation groups of PBDs , are required for matrix protein import ; three , Pex 3 p , Pex 16 p and Pex 19 p , are shown to be essential for peroxisome membrane assembly and responsible for the most severe ZS in PBDs of three complementation groups 12 , 9 , and 14 , respectively . Patients with severe ZS with defects of PEX 3 , PEX 16 , and PEX 19 tend to carry severe mutation such as nonsense mutations , frameshifts and deletions . With respect to the function of these three peroxins in membrane biogenesis , two distinct pathways have been proposed for the import of peroxisomal membrane proteins in mammalian cells : a Pex 19 p - and Pex 3 p -dependent class I pathway and a Pex 19 p - and Pex 16 p -dependent class II pathway . In class II pathway , Pex 19 p also forms a soluble complex with newly synthesized Pex 3 p as the chaperone for Pex 3 p in the cytosol and directly translocates it to peroxisomes . Pex 16 p functions as the peroxisomal membrane receptor that is specific to the Pex 3 p -Pex 19 p complexes . A model for the import of peroxisomal membrane proteins is suggested , providing new insights into the molecular mechanisms underlying the biogenesis of peroxisomes and its regulation involving Pex 3 p , Pex 19 p , and Pex 16 p . Another model suggests that in Saccharomyces cerevisiae peroxisomes likely emerge from the endoplasmic reticulum .