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A novel pex2 mutant:: catalase-deficient but temperature-sensitive PTS1 and PTS2 import

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ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/S0006-291X(02)00419-9

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CHO cell mutants; peroxisome biogenesis; complementation groups; peroxin; PEX2; peroxisome biogenesis disorders; temperature-sensitive protein import; green fluorescent protein

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We searched for Chinese hamster ovary (CHO) cell mutants defective in peroxisome biogenesis by using peroxisome targeting sequence (PTS) of Pex3p (amino acid residues 1-40)-fused enhanced green fluorescent protein (EGFP). From mutagenized wild-type CHO-K1 cells stably expressing rat Pex2p and Pex3p(1-40)-EGFP, cell colonies resistant to the 9-(1'-pyrene)nonanol/ultraviolet treatment were examined for intracellular location of peroxisomal proteins, including EGFP chimera, catalase, and matrix proteins with PTS types 1 and 2. One clone, ZPEG309, showed a distinct phenotype: import defect of catalase, but normal transport of PTS I and PTS2 proteins at 37degreesC. PTS1 and PTS2 import was abrogated when ZPEG309 Was Cultured at 39degreesC. Genetic defect of ZPEG309 was a nonsense point mutation in a codon for Arg(50) in CHO PEX2 and a mutation resulting in a C-terminal truncation of the introduced rat Pex2p. Therefore, ZPEG309 is a novel pex2, catalase-deficient mutant with temperature-sensitive PTS I and PTS2 import. (C) 2002 Elsevier Science (USA). All rights reserved.

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