Abstract
The peroxisome biogenesis disorders (PBDs) are currently difficult-to-treat multiple-organ dysfunction disorders that result from the defective biogenesis of peroxisomes. Genes encoding Peroxins, which are required for peroxisome biogenesis or functions, are known causative genes of PBDs. The human peroxin genes PEX3 or PEX16 are required for peroxisomal membrane protein targeting, and their mutations cause Zellweger syndrome, a class of PBDs. Lack of understanding about the pathogenesis of Zellweger syndrome has hindered the development of effective treatments. Here, we developed potential Drosophila models for Zellweger syndrome, in which the Drosophila pex3 or pex16 gene was disrupted. As found in Zellweger syndrome patients, peroxisomes were not observed in the homozygous Drosophila pex3 mutant, which was larval lethal. However, the pex16 homozygote lacking its maternal contribution was viable and still maintained a small number of peroxisome-like granules, even though PEX16 is essential for the biosynthesis of peroxisomes in humans. These results suggest that the requirements for pex3 and pex16 in peroxisome biosynthesis in Drosophila are different, and the role of PEX16 orthologs may have diverged between mammals and Drosophila. The phenotypes of our Zellweger syndrome model flies, such as larval lethality in pex3, and reduced size, shortened longevity, locomotion defects, and abnormal lipid metabolisms in pex16, were reminiscent of symptoms of this disorder, although the Drosophila pex16 mutant does not recapitulate the infant death of Zellweger syndrome. Furthermore, pex16 mutants showed male-specific sterility that resulted from the arrest of spermatocyte maturation. pex16 expressed in somatic cyst cells but not germline cells had an essential role in the maturation of male germline cells, suggesting that peroxisome-dependent signals in somatic cyst cells could contribute to the progression of male germ-cell maturation. These potential Drosophila models for Zellweger syndrome should contribute to our understanding of its pathology.
Highlights
The peroxisome biogenesis disorders (PBDs) are human recessive hereditary diseases that arise from mutations in PEX genes, which encode the Peroxins, essential proteins for the biogenesis of peroxisomes [1]
Taken together with our finding that the number of peroxisomes is severely reduced in the pex161 homozygotes, these results suggest that the pex161 mutant can serve as a potential Drosophila model of Zellweger syndrome, it does not recapitulate the infant death associated with this syndrome
We developed Drosophila models of PBDs, in which Drosophila pex3 or pex16 genes were disrupted
Summary
The peroxisome biogenesis disorders (PBDs) are human recessive hereditary diseases that arise from mutations in PEX genes, which encode the Peroxins, essential proteins for the biogenesis of peroxisomes [1]. The analysis of these mutants revealed that the import of some peroxisomal matrix proteins is required for spermatogenesis and the metabolism of VLCFAs [24] These mutants do not show other phenotypes reminiscent of PBD symptoms, such as defects in neuronal development and function [24]. In contrast to the pex and pex mutants, which show developmental defects only in spermatogenesis [24], the pex mutant was larval lethal, and the pex mutant showed a reduced lifespan and various defects in development and neural function We conclude that these mutants reflect broad symptoms of PBDs, and can be viewed as Drosophila models of these diseases, especially of Zellweger syndrome, the Drosophila pex mutant does not recapitulate the infant death seen in Zellweger syndrome patients
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