4.4 Article

Mechanisms of induced resistance in lettuce against Bremia lactucae by DL-β-amino-butyric acid (BABA)

期刊

EUROPEAN JOURNAL OF PLANT PATHOLOGY
卷 126, 期 4, 页码 553-573

出版社

SPRINGER
DOI: 10.1007/s10658-009-9564-6

关键词

Downy mildew; Induced resistance; Butanoic acids

资金

  1. European Community under the Sixth Framework Program for Research
  2. Technological Development and Demonstration Activities
  3. Integrated Project QUALITYLOWINPUTFOOD [FP6-FOOD-CT-2003-506358]

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BABA induced local and systemic resistance in lettuce (Lactuca sativa) against the Oomycete Bremia lactucae. Structure-activity analysis showed no induced resistance by related amino-butanoic acids or beta-alanine. The R-enantiomer of BABA induced resistance whereas the S-enantiomer did not, suggesting binding to a specific receptor. Other compounds known to be involved in SAR signaling, including abscisic acid, methyl-jasmonate, ethylene, sodium-salicylate and BionA (R) (BTH) did not induce resistance. Systemic translocation of C-14-BABA and systemic protection against downy mildew were tightly correlated. BABA did not affect spore germination, appressorium formation, or penetration of B. lactucae into the host. Epifluorescence and confocal microscopy revealed that BABA induced rapid encasement with callose of the primary infection structures of the pathogen, thus preventing it from further developing intercellular hyphae and haustoria. Invaded host cells treated with BABA did not accumulate phenolics, callose or lignin, or express HR. In contrast, cells of genetically-resistant cultivars accumulated phenolics, callose and lignin and exhibited HR within one day after inoculation. The callose synthesis inhibitor DDG did not inhibit callose encasement nor compromised the resistance induced by BABA. PR-proteins accumulated too late to be responsible for the induced resistance. DAB staining indicated that BABA induced a rapid accumulation of H2O2 in the penetrated epidermal host cells. Whether H2O2 stops the pathogen directly or via another metabolic route is not known.

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