The peroxin Pex6p gene is impaired in peroxisomal biogenesis disorders of complementation group 6

N. Matsumoto; S. Tamura; A. Moser; H. W. Moser; N. Braverman; Y. Suzuki; N. Shimozawa; N. Kondo; Y. Fujiki

doi:10.1007/s100380170078

The peroxin Pex6p gene is impaired in peroxisomal biogenesis disorders of complementation group 6

N. Matsumoto, S. Tamura, A. Moser, H. W. Moser, N. Braverman, Y. Suzuki, N. Shimozawa, N. Kondo, Y. Fujiki

Division for Experimental Natural Science

Research output: Contribution to journal › Article › peer-review

32 Citations (Scopus)

Abstract

Human genetic peroxisomal biogenesis disorders (PBDs), such as Zellweger syndrome, comprise 13 different complementation groups (CGs). Eleven peroxin genes, termed PEXs, responsible for PBDs have been identified, whereas pathogenic genes for PBDs of 2CGs, CG-A (the same CG as CG8 in the United States and Europe) and CG6, remained unidentified. We herein provide several lines of novel evidence indicating that PEX6, the pathogenic gene for CG4, is impaired in PBD of CG6. Expression of PEX6 restored peroxisome assembly in fibroblasts from a CG6 PBD patient. This patient was a compound heterozygote for PEX6 gene alleles. Accordingly, by merging CG6 with CG4, human PBDs are now classified into 12 CGs.

Original language	English
Pages (from-to)	273-277
Number of pages	5
Journal	Journal of Human Genetics
Volume	46
Issue number	5
DOIs	https://doi.org/10.1007/s100380170078
Publication status	Published - 2001

All Science Journal Classification (ASJC) codes

Genetics
Genetics(clinical)

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title = "The peroxin Pex6p gene is impaired in peroxisomal biogenesis disorders of complementation group 6",

abstract = "Human genetic peroxisomal biogenesis disorders (PBDs), such as Zellweger syndrome, comprise 13 different complementation groups (CGs). Eleven peroxin genes, termed PEXs, responsible for PBDs have been identified, whereas pathogenic genes for PBDs of 2CGs, CG-A (the same CG as CG8 in the United States and Europe) and CG6, remained unidentified. We herein provide several lines of novel evidence indicating that PEX6, the pathogenic gene for CG4, is impaired in PBD of CG6. Expression of PEX6 restored peroxisome assembly in fibroblasts from a CG6 PBD patient. This patient was a compound heterozygote for PEX6 gene alleles. Accordingly, by merging CG6 with CG4, human PBDs are now classified into 12 CGs.",

author = "N. Matsumoto and S. Tamura and A. Moser and Moser, {H. W.} and N. Braverman and Y. Suzuki and N. Shimozawa and N. Kondo and Y. Fujiki",

year = "2001",

doi = "10.1007/s100380170078",

language = "English",

volume = "46",

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journal = "Jinrui idengaku zasshi. The Japanese journal of human genetics",

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T1 - The peroxin Pex6p gene is impaired in peroxisomal biogenesis disorders of complementation group 6

AU - Matsumoto, N.

AU - Tamura, S.

AU - Moser, A.

AU - Moser, H. W.

AU - Braverman, N.

AU - Suzuki, Y.

AU - Shimozawa, N.

AU - Kondo, N.

AU - Fujiki, Y.

PY - 2001

Y1 - 2001

N2 - Human genetic peroxisomal biogenesis disorders (PBDs), such as Zellweger syndrome, comprise 13 different complementation groups (CGs). Eleven peroxin genes, termed PEXs, responsible for PBDs have been identified, whereas pathogenic genes for PBDs of 2CGs, CG-A (the same CG as CG8 in the United States and Europe) and CG6, remained unidentified. We herein provide several lines of novel evidence indicating that PEX6, the pathogenic gene for CG4, is impaired in PBD of CG6. Expression of PEX6 restored peroxisome assembly in fibroblasts from a CG6 PBD patient. This patient was a compound heterozygote for PEX6 gene alleles. Accordingly, by merging CG6 with CG4, human PBDs are now classified into 12 CGs.

AB - Human genetic peroxisomal biogenesis disorders (PBDs), such as Zellweger syndrome, comprise 13 different complementation groups (CGs). Eleven peroxin genes, termed PEXs, responsible for PBDs have been identified, whereas pathogenic genes for PBDs of 2CGs, CG-A (the same CG as CG8 in the United States and Europe) and CG6, remained unidentified. We herein provide several lines of novel evidence indicating that PEX6, the pathogenic gene for CG4, is impaired in PBD of CG6. Expression of PEX6 restored peroxisome assembly in fibroblasts from a CG6 PBD patient. This patient was a compound heterozygote for PEX6 gene alleles. Accordingly, by merging CG6 with CG4, human PBDs are now classified into 12 CGs.

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The peroxin Pex6p gene is impaired in peroxisomal biogenesis disorders of complementation group 6

Abstract

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