Nucleocytoplasmic Distribution Is Required for Activation of Resistance by the Potato NB-LRR Receptor Rx1 and Is Balanced by Its Functional Domains

被引:131
作者
Slootweg, Erik [1 ]
Roosien, Jan [1 ]
Spiridon, Laurentiu N. [2 ]
Petrescu, Andrei-Jose [2 ]
Tameling, Wladimir [3 ]
Joosten, Matthieu [3 ]
Pomp, Rikus [1 ]
van Schaik, Casper [1 ]
Dees, Robert [4 ]
Borst, Jan Willem [5 ]
Smant, Geert [1 ]
Schots, Arjen [4 ]
Bakker, Jaap [1 ,6 ]
Goverse, Aska [1 ,6 ]
机构
[1] Wageningen Univ, Dept Plant Sci, Nematol Lab, NL-6708 PB Wageningen, Netherlands
[2] Romanian Acad, Inst Biochem, Bucharest 060031, Romania
[3] Wageningen Univ, Dept Plant Sci, Phytopathol Lab, NL-6708 PB Wageningen, Netherlands
[4] Wageningen Univ, Dept Plant Sci, Lab Mol Recognit & Antibody Technol, NL-6708 PB Wageningen, Netherlands
[5] Wageningen Univ, Dept Agrotechnol & Food Sci, Biochem Lab, NL-6703 HA Wageningen, Netherlands
[6] Ctr BioSyst Genom, NL-6700 AB Wageningen, Netherlands
关键词
SECONDARY STRUCTURE PREDICTION; NUCLEAR-LOCALIZATION SIGNALS; INNATE IMMUNE-RESPONSE; LEUCINE-RICH REPEAT; TO-CELL MOVEMENT; DISEASE-RESISTANCE; VIRUS-X; ARABIDOPSIS-THALIANA; COAT PROTEIN; IN-VIVO;
D O I
10.1105/tpc.110.077537
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The Rx1 protein, as many resistance proteins of the nucleotide binding-leucine-rich repeat (NB-LRR) class, is predicted to be cytoplasmic because it lacks discernable nuclear targeting signals. Here, we demonstrate that Rx1, which confers extreme resistance to Potato virus X, is located both in the nucleus and cytoplasm. Manipulating the nucleocytoplasmic distribution of Rx1 or its elicitor revealed that Rx1 is activated in the cytoplasm and cannot be activated in the nucleus. The coiled coil (CC) domain was found to be required for accumulation of Rx1 in the nucleus, whereas the LRR domain promoted the localization in the cytoplasm. Analyses of structural subdomains of the CC domain revealed no autonomous signals responsible for active nuclear import. Fluorescence recovery after photobleaching and nuclear fractionation indicated that the CC domain binds transiently to large complexes in the nucleus. Disruption of the Rx1 resistance function and protein conformation by mutating the ATP binding phosphate binding loop in the NB domain, or by silencing the cochaperone SGT1, impaired the accumulation of Rx1 protein in the nucleus, while Rx1 versions lacking the LRR domain were not affected in this respect. Our results support a model in which interdomain interactions and folding states determine the nucleocytoplasmic distribution of Rx1.
引用
收藏
页码:4195 / 4215
页数:21
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