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A truncated NLR protein, TIR-NBS2, is required for activated defense responses in the exo70B1 mutant.


ABSTRACT: During exocytosis, the evolutionarily conserved exocyst complex tethers Golgi-derived vesicles to the target plasma membrane, a critical function for secretory pathways. Here we show that exo70B1 loss-of-function mutants express activated defense responses upon infection and express enhanced resistance to fungal, oomycete and bacterial pathogens. In a screen for mutants that suppress exo70B1 resistance, we identified nine alleles of TIR-NBS2 (TN2), suggesting that loss-of-function of EXO70B1 leads to activation of this nucleotide binding domain and leucine-rich repeat-containing (NLR)-like disease resistance protein. This NLR-like protein is atypical because it lacks the LRR domain common in typical NLR receptors. In addition, we show that TN2 interacts with EXO70B1 in yeast and in planta. Our study thus provides a link between the exocyst complex and the function of a 'TIR-NBS only' immune receptor like protein. Our data are consistent with a speculative model wherein pathogen effectors could evolve to target EXO70B1 to manipulate plant secretion machinery. TN2 could monitor EXO70B1 integrity as part of an immune receptor complex.

SUBMITTER: Zhao T 

PROVIDER: S-EPMC4305288 | biostudies-literature | 2015 Jan

REPOSITORIES: biostudies-literature

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A truncated NLR protein, TIR-NBS2, is required for activated defense responses in the exo70B1 mutant.

Zhao Ting T   Rui Lu L   Li Juan J   Nishimura Marc T MT   Vogel John P JP   Liu Na N   Liu Simu S   Zhao Yaofei Y   Dangl Jeffery L JL   Tang Dingzhong D  

PLoS genetics 20150124 1


During exocytosis, the evolutionarily conserved exocyst complex tethers Golgi-derived vesicles to the target plasma membrane, a critical function for secretory pathways. Here we show that exo70B1 loss-of-function mutants express activated defense responses upon infection and express enhanced resistance to fungal, oomycete and bacterial pathogens. In a screen for mutants that suppress exo70B1 resistance, we identified nine alleles of TIR-NBS2 (TN2), suggesting that loss-of-function of EXO70B1 lea  ...[more]

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