Isolation and characterization of peroxisome-deficient Chinese hamster ovary cell mutants representing human complementation group III

被引：37

作者：

Okumoto, K

Bogaki, A

Tateishi, K

Tsukamoto, T

Osumi, T

Shimozawa, N

Suzuki, Y

Orii, T

Fujiki, Y

机构：

[1] KYUSHU UNIV,FAC SCI,DEPT BIOL,FUKUOKA 81281,JAPAN

[2] HIMEJI INST TECHNOL,DEPT LIFE SCI,KAMIGORI,HYOGO 67812,JAPAN

[3] GIFU UNIV,DEPT PEDIAT,GIFU 500,JAPAN

来源：

EXPERIMENTAL CELL RESEARCH | 1997年 / 233卷 / 01期

关键词：

D O I：

10.1006/excr.1997.3552

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

We made use of the 9-(1'-pyrene)nonanol/ultraviolet (P9OH/UV) method and isolated peroxisome-deficient mutant cells. TKa cells, the wild-type Chinese hamster ovary (CHO) cells, CHO-K1, that had been stably transfected with cDNA encoding Pex2p (formerly peroxisome assembly factor-1, PAF-1) were used to avoid frequent isolation of the Z65-type, PEX2-defective mutants. P9OH/UV-resistant cell colonies were examined for the intracellular location of catalase, a peroxisomal matrix enzyme, by immunofluorescence microscopy and using anti-catalase antibody. As six mutant cell clones showed cytosolic catalase, there was likely to be a deficiency in peroxisome assembly. These mutants also showed the typical peroxisome assembly-defective phenotype, including significant decrease of dihydroxyacetonephosphate acyltransferase, the first step key enzyme in plasmalogen synthesis, and loss of resistance to 12-(1'-pyrene)dodecanoic acid/UV treatment. By transfection of Pex2p and Pex6p (formerly PAF-2) cDNAs and cell fusion analysis between the CHO cell mutants, two mutants, ZP104 and ZP109, were found to belong to a novel complementation group. Further complementation analysis using fibroblasts from patients with peroxisome biogenesis disorders revealed that the mutants belonged to human complementation group III. Taken together, ZP104 and ZP109 are in a newly identified fifth complementation group in CHO mutants reported to date and represent the human complementation group III. (C) 1997 Academic Press.

引用

页码：11 / 20

页数：10

共 35 条

[1]

AKAO T, 1994, BIOCHEM MOL BIOL INT, V34, P915

[2] GENETIC-HETEROGENEITY IN THE CEREBROHEPATORENAL (ZELLWEGER) SYNDROME AND OTHER INHERITED DISORDERS WITH A GENERALIZED IMPAIRMENT OF PEROXISOMAL FUNCTIONS - A STUDY USING COMPLEMENTATION ANALYSIS [J].

BRUL, S ;

WESTERVELD, A ;

STRIJLAND, A ;

WANDERS, RJA ;

SCHRAM, AW ;

HEYMANS, HSA ;

SCHUTGENS, RBH ;

VANDENBOSCH, H ;

TAGER, JM .

JOURNAL OF CLINICAL INVESTIGATION, 1988, 81 (06) :1710-1715

[3] HIGH-EFFICIENCY TRANSFORMATION OF MAMMALIAN-CELLS BY PLASMID DNA [J].

CHEN, C ;

OKAYAMA, H .

MOLECULAR AND CELLULAR BIOLOGY, 1987, 7 (08) :2745-2752

[4] Unified nomenclature for peroxisome biogenesis factors [J].

Distel, B ;

Erdmann, R ;

Gould, SJ ;

Blobel, G ;

Crane, DI ;

Cregg, JM ;

Dodt, G ;

Fujiki, Y ;

Goodman, JM ;

Just, WW ;

Kiel, JAKW ;

Kunau, WH ;

Lazarow, PB ;

Mannaerts, GP ;

Moser, HW ;

Osumi, T ;

Rachubinski, RA ;

Roscher, A ;

Subramani, S ;

Tabak, HF ;

Tsukamoto, T ;

Valle, D ;

vanderKlei, I ;

vanVeldhoven, PP ;

Veenhuis, M .

JOURNAL OF CELL BIOLOGY, 1996, 135 (01) :1-3

[5] MUTATIONS IN THE PTS1 RECEPTOR GENE, PXR1, DEFINE COMPLEMENTATION GROUP-2 OF THE PEROXISOME BIOGENESIS DISORDERS [J].

DODT, G ;

BRAVERMAN, N ;

WONG, C ;

MOSER, A ;

MOSER, HW ;

WATKINS, P ;

VALLE, D ;

GOULD, SJ .

NATURE GENETICS, 1995, 9 (02) :115-125

[6] PAS1, A YEAST GENE REQUIRED FOR PEROXISOME BIOGENESIS, ENCODES A MEMBER OF A NOVEL FAMILY OF PUTATIVE ATPASES [J].

ERDMANN, R ;

WIEBEL, FF ;

FLESSAU, A ;

RYTKA, J ;

BEYER, A ;

FROHLICH, KU ;

KUNAU, WH .

CELL, 1991, 64 (03) :499-510

[7] IDENTIFICATION AND CHARACTERIZATION OF THE PUTATIVE HUMAN PEROXISOMAL C-TERMINAL TARGETING SIGNAL IMPORT RECEPTOR [J].

FRANSEN, M ;

BREES, C ;

BAUMGART, E ;

VANHOOREN, JCT ;

BAES, M ;

MANNAERTS, GP ;

VANVELDHOVEN, PP .

JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (13) :7731-7736

[8]

Fukuda S, 1996, AM J HUM GENET, V59, P1210

[9] 2 COMPLEMENTARY APPROACHES TO STUDY PEROXISOME BIOGENESIS IN SACCHAROMYCES-CEREVISIAE - FORWARD AND REVERSED GENETICS [J].

KUNAU, WH ;

BEYER, A ;

FRANKEN, T ;

GOTTE, K ;

MARZIOCH, M ;

SAIDOWSKY, J ;

SKALETZROROWSKI, A ;

WIEBEL, FF .

BIOCHIMIE, 1993, 75 (3-4) :209-224

[10]

LAZAROW PB, 1994, METABOLIC BASIS INHE, P2287

← 1 2 3 4 →