Dimerization and protease resistance: New insight into the function of PR-1 |
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Authors: | Shunwen Lu Justin D. Faris Robert Sherwood Michael C. Edwards |
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Affiliation: | 1. USDA-ARS, Cereal Crops Research Unit, Fargo, ND 58102, USA;2. Cornell University Life Sciences Core Laboratories Center, Ithaca, NY 14853, USA |
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Abstract: | The group 1 pathogenesis-related (PR-1) proteins have long been considered hallmarks of hypersensitive response/defense pathways in plants, but their biochemical functions are still obscure despite resolution of the NMR/X-ray structures of several PR-1-like proteins, including P14a (the prototype PR-1). We report here the characterization of two basic PR-1 proteins (PR-1-1 and PR-1-5) recently identified from hexaploid wheat (Triticum aestivum). Both proteins were expressed in Pichia pastoris as a single major species of ∼15 kDa. Sequence identity of the expressed PR-1 proteins was verified by MALDI-TOF/TOF analysis. Accumulation of the native PR-1-5 protein in pathogen-challenged wheat was confirmed by protein gel blot analysis. Low-temperature SDS-PAGE and yeast two-hybrid assays revealed that PR-1-1 exists primarily as a monomer whereas PR-1-5 forms homodimers. Both PR-1 proteins are resistant to proteases compared to bovine serum albumin, but PR-1-1 shows resistance mainly to subtilisin and protease K (serine proteases) whereas PR-1-5 shows resistance to subtilisin, protease K and papain (a cysteine protease). Site-specific mutations at the five putative active sites in the PR-1 domain all affected dimerization, with the mutations at Glu-72 and Glu-102 (in the PR-1-5 numeration) also diminishing protease resistance. Sequence analysis revealed that the Glu-72 and Glu-102 residues are located in motif-like sequences that are conserved in both PR-1 and the human apoptosis-related caspase proteins. These findings prompt us to examine the function of PR-1 for a role in protease-mediated programmed cell death pathways in plants. |
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Keywords: | BSA, bovine serum albumin HR, hypersensitive response HRP, horseradish peroxidase Lt-SDS-PAGE, low temperature-SDS-PAGE PCD, programmed cell death PCK1, phosphoenolpyruvate carboxykinase SP, signal peptide Y2H, yeast two-hybrid WT, wild type |
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