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• W2034003178 abstract "Mutations in peroxisome biogenesis proteins (peroxins) can lead to developmental deficiencies in various eukaryotes. PEX14 and PEX13 are peroxins involved in docking cargo-receptor complexes at the peroxisomal membrane, thus aiding in the transport of the cargo into the peroxisomal matrix. Genetic screens have revealed numerous Arabidopsis thaliana peroxins acting in peroxisomal matrix protein import; the viable alleles isolated through these screens are generally partial loss-of-function alleles, whereas null mutations that disrupt delivery of matrix proteins to peroxisomes can confer embryonic lethality. In this study, we used forward and reverse genetics in Arabidopsis to isolate four pex14 alleles. We found that all four alleles conferred reduced PEX14 mRNA levels and displayed physiological and molecular defects suggesting reduced but not abolished peroxisomal matrix protein import. The least severe pex14 allele, pex14-3, accumulated low levels of a C-terminally truncated PEX14 product that retained partial function. Surprisingly, even the severe pex14-2 allele, which lacked detectable PEX14 mRNA and PEX14 protein, was viable, fertile, and displayed residual peroxisome matrix protein import. As pex14 plants matured, import improved. Together, our data indicate that PEX14 facilitates, but is not essential for peroxisomal matrix protein import in plants." @default.
• W2034003178 created "2016-06-24" @default.
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• W2034003178 date "2011-05-08" @default.
• W2034003178 modified "2023-10-03" @default.
• W2034003178 title "Matrix proteins are inefficiently imported into Arabidopsis peroxisomes lacking the receptor-docking peroxin PEX14" @default.
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• W2034003178 cites W1967424027 @default.
• W2034003178 cites W1967503648 @default.
• W2034003178 cites W1968509140 @default.
• W2034003178 cites W1969624770 @default.
• W2034003178 cites W1969836693 @default.
• W2034003178 cites W1969867336 @default.
• W2034003178 cites W1976257663 @default.
• W2034003178 cites W1978661900 @default.
• W2034003178 cites W1978751527 @default.
• W2034003178 cites W1980381018 @default.
• W2034003178 cites W1980954702 @default.
• W2034003178 cites W1982912301 @default.
• W2034003178 cites W1983112089 @default.
• W2034003178 cites W1983281364 @default.
• W2034003178 cites W1990991454 @default.
• W2034003178 cites W1993691427 @default.
• W2034003178 cites W1996385741 @default.
• W2034003178 cites W2007209781 @default.
• W2034003178 cites W2011682300 @default.
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• W2034003178 doi "https://doi.org/10.1007/s11103-011-9782-0" @default.
• W2034003178 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/3529590" @default.
• W2034003178 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/21553312" @default.
• W2034003178 hasPublicationYear "2011" @default.
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