Literature DB >> 15141959

Two PAK kinase genes, CHM1 and MST20, have distinct functions in Magnaporthe grisea.

Lei Li1, Chaoyang Xue, Kenneth Bruno, Marie Nishimura, Jin-Rong Xu.   

Abstract

In the rice blast fungus Magnaporthe grisea, the Pmk1 mitogen-activated protein (MAP) kinase is essential for appressorium formation and infectious growth. PMK1 is homologous to yeast Fus3 and Kss1 MAP kinases that are known to be regulated by the Ste20 PAK kinase for activating the pheromone response and filamentation pathways. In this study, we isolated and characterized two PAK genes, CHM1 and MST20, in M. grisea. Mutants disrupted in MST20 were reduced in aerial hyphae growth and conidiation, but normal in growth rate, appressorium formation, penetration, and plant infection. In chm1 deletion mutants, growth, conidiation, and appressorium formation were reduced significantly. Even though appressoria formed by chm1 mutants were defective in penetration, chm1 mutants were able to grow invasively on rice leaves and colonize through wounds. The chm1 mutants were altered in conidiogenesis and produced conidia with abnormal morphology. Hyphae of chm1 mutants had normal septation, but the length of hyphal compartments was reduced. On nutritionally poor oatmeal agar, chm1 mutants were unstable and produced sectors that differed from original chm1 mutants in growth rate, conidiation, or colony morphology. However, none of the monoconidial cultures derived from these spontaneous sectors were normal in appressorial penetration and fungal pathogenesis. These data suggest that MST20 is dispensable for plant infection in M. grisea, but CHM1 plays a critical role in appressorium formation and penetration. Both mst20 and chm1 deletion mutants were phenotypically different from the pmk1 mutant that is defective in appressorium formation and infectious hyphae growth. It is likely that MST20 and CHM1 individually play no critical role in activating the PMK1 MAP kinase pathway during appressorium formation and infectious hyphae growth. However, CHM1 appears to be essential for appressorial penetration and CHM1 and MST20 may have redundant functions in M. grisea.

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Year:  2004        PMID: 15141959     DOI: 10.1094/MPMI.2004.17.5.547

Source DB:  PubMed          Journal:  Mol Plant Microbe Interact        ISSN: 0894-0282            Impact factor:   4.171


  32 in total

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4.  A mitogen-activated protein kinase cascade regulating infection-related morphogenesis in Magnaporthe grisea.

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5.  Abiotic stress resistance, a novel moonlighting function of ribosomal protein RPL44 in the halophilic fungus Aspergillus glaucus.

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Review 6.  Under pressure: investigating the biology of plant infection by Magnaporthe oryzae.

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8.  MoCps1 is important for conidiation, conidial morphology and virulence in Magnaporthe oryzae.

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9.  Reverse genetics for functional genomics of phytopathogenic fungi and oomycetes.

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Journal:  Comp Funct Genomics       Date:  2009-10-07

10.  In vivo yeast cell morphogenesis is regulated by a p21-activated kinase in the human pathogen Penicillium marneffei.

Authors:  Kylie J Boyce; Lena Schreider; Alex Andrianopoulos
Journal:  PLoS Pathog       Date:  2009-11-26       Impact factor: 6.823

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