The mitogen-activated protein kinase module CcSte11-CcSte7-CcPmk1 regulates pathogenicity via the transcription factor CcSte12 in Cytospora chrysosperma

Lu Yu; Yuchen Yang; Xiaolin Qiu; Dianguang Xiong; Chengming Tian

doi:10.1007/s44154-023-00142-w

Stress Biology (Jan 2024)

The mitogen-activated protein kinase module CcSte11-CcSte7-CcPmk1 regulates pathogenicity via the transcription factor CcSte12 in Cytospora chrysosperma

Lu Yu,
Yuchen Yang,
Xiaolin Qiu,
Dianguang Xiong,
Chengming Tian

Affiliations

Lu Yu: State Key Laboratory of Efficient Production of Forest Resources
Yuchen Yang: State Key Laboratory of Efficient Production of Forest Resources
Xiaolin Qiu: State Key Laboratory of Efficient Production of Forest Resources
Dianguang Xiong: State Key Laboratory of Efficient Production of Forest Resources
Chengming Tian: State Key Laboratory of Efficient Production of Forest Resources

DOI: https://doi.org/10.1007/s44154-023-00142-w
Journal volume & issue: Vol. 4, no. 1
pp. 1 – 19

Abstract

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Abstract The pathogen Cytospora chrysosperma is the causal agent of poplar canker disease and causes considerable economic losses in China. Mitogen-activated protein kinase (MAPK) cascades play a crucial role in mediating cellular responses and Pmk1-MAPKs are indispensable for pathogenic related processes in plant pathogenic fungi. In previous studies, we demonstrated that the CcPmk1 acts as a core regulator of fungal pathogenicity by modulating a small number of master downstream targets, such as CcSte12. In this study, we identified and characterized two upstream components of CcPmk1: MAPKKK CcSte11 and MAPKK CcSte7. Deletion of CcSte11 and CcSte7, resulted in slowed growth, loss of sporulation and virulence, similar to the defects observed in the CcPmk1 deletion mutant. In addition, CcSte11, CcSte7 and CcPmk1 interact with each other, and the upstream adaptor protein CcSte50 interact with CcSte11 and CcSte7. Moreover, we explored the global regulation network of CcSte12 by transcriptional analysis between CcSte12 deletion mutants and wild-type during the simulated infection process. Two hydrolase activity GO terms (GO:0004553 and GO:0016798) and starch and sucrose metabolism (mgr00500) KEGG pathway were significantly enriched in the down-regulated genes of CcSte12 deletion mutants. In addition, a subset of glycosyl hydrolase genes and putative effector genes were significantly down-regulated in the CcSte12 deletion mutant, which might be important for fungal pathogenicity. Especially, CcSte12 bound to the CcSp84 promoter region containing the TGAAACA motif. Moreover, comparison of CcSte12-regulated genes with CcPmk1-regulated genes revealed 116 overlapping regulated genes in both CcSte12 and CcPmk1, including some virulence-associated genes. Taken together, the protein complexes CcSte11-CcSte7-CcPmk1 receive signals transmitted by upstream CcSte50 and transmit signals to downstream CcSte12, which regulates hydrolase, effectors and other genes to promote virulence. Overall, these results indicate that the CcPmk1-MAPK signaling pathway of C. chrysosperma plays a key role in the pathogenicity.

Published in Stress Biology

ISSN: 2731-0450 (Online)
Publisher: Springer
Country of publisher: Singapore
LCC subjects: Science: Biology (General)
Website: https://www.springer.com/journal/44154

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