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Regulatory Mechanisms Underlying Biological Control Activity of Pseudomonas chlororaphis PA23.

机译:绿假单胞菌PA23生物防治活性的调控机制。

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摘要

Biological control is an intriguing alternative to the use of chemical pesticides as it represents a safer, more environmentally friendly approach to managing plant pathogens. Pseudomonas chlororaphis strain PA23 was isolated from soybean root tips and it was found to be an excellent antagonist of sclerotinia stem rot. Our studies have shown that pyrrolnitrin (PRN) is the key metabolite required for S. sclerotiorum inhibition, while phenazine (PHZ) is important for biofilm establishment. For this reason, research efforts were directed towards elucidating the mechanisms governing PA23-mediated antibiotic production. To determine how these compounds were regulated, QS-deficient strains and an rpoS mutant were generated. The QS-deficient strains no longer inhibited the fungal pathogen S. sclerotiorum in vitro and exhibited reduced PRN, PHZ and protease production. Analysis of transcriptional fusions revealed that RpoS has a positive and negative effect on phzI and phzR, respectively. In a reciprocal manner, RpoS is positively regulated by QS. Characterization of a phzRrpoS double mutant showed reduced antifungal activity as well as PRN and PHZ production, similar to the QS-deficient strains. Furthermore, phzR but not rpoS was able to complement the phzRrpoS double mutant for the aforementioned traits, indicating that the Phz QS system is a central regulator of PA23-mediated antagonism.;GacS/GacA, PsrA, RpoS and the PhzI/PhzR QS are members of a complex regulatory hierarchy that influence secondary metabolite production in PA23. An additional system, termed Rsm, was identified, adding yet another layer of complexity to the regulatory network. The Rsm system in PA23 appears to be comprised of a single small non-coding regulatory RNA termed RsmZ, and two RNA binding proteins RsmA and RsmE. We discovered that the expression of rsmZ, rsmA and rsmE all require GacA. In addition, both PsrA and QS were shown to positively regulate rsmZ transcription. For rsmE, GacA may indirectly regulate expression through PsrA, RpoS and QS, as all three regulators control rsmE transcription. Furthermore, we believe that the positive effects of PsrA and QS on rsmE transcription are likely mediated through RpoS as only RpoS show direct activation of rsmE in an E. coli background.
机译:生物控制是化学农药使用的一种有趣替代方法,因为它代表了一种更安全,更环保的植物病原体管理方法。从大豆根尖分离出绿假单胞菌菌株PA23,发现其是菌核病茎腐的优良拮抗剂。我们的研究表明,吡咯菌素(PRN)是抑制葡萄球菌的关键代谢产物,而吩嗪(PHZ)对于生物膜的建立很重要。因此,研究工作致力于阐明控制PA23介导的抗生素生产的机制。为了确定如何调节这些化合物,生成了QS缺陷菌株和rpoS突变体。缺乏QS的菌株不再在体外抑制真菌病原菌S.sclerotiorum,并表现出降低的PRN,PHZ和蛋白酶产生。转录融合的分析表明,RpoS分别对phzI和phzR具有正面和负面影响。以相互的方式,RpoS由QS积极调控。 phzRrpoS双突变体的表征显示出降低的抗真菌活性以及PRN和PHZ产生,类似于QS缺陷型菌株。此外,phzR而非rpoS能够补充phzRrpoS双突变体的上述特征,这表明Phz QS系统是PA23介导的拮抗作用的中央调节剂; GacS / GacA,PsrA,RpoS和PhzI / PhzR QS是影响PA23中次级代谢产物产生的复杂监管体系的成员。确定了另一个称为Rsm的系统,这给监管网络增加了另一层复杂性。 PA23中的Rsm系统似乎由称为RsmZ的单个小非编码调控RNA和两个RNA结合蛋白RsmA和RsmE组成。我们发现rsmZ,rsmA和rsmE的表达均需要GacA。此外,PsrA和QS都显示出正调控rsmZ转录。对于rsmE,GacA可能通过PsrA,RpoS和QS间接调节表达,因为这三个调节因子都控制rsmE转录。此外,我们认为PsrA和QS对rsmE转录的积极影响可能是通过RpoS介导的,因为只有RpoS在大肠杆菌背景中显示rsmE的直接激活。

著录项

  • 作者

    Selin, Carrie Lynn.;

  • 作者单位

    University of Manitoba (Canada).;

  • 授予单位 University of Manitoba (Canada).;
  • 学科 Biology Microbiology.
  • 学位 Ph.D.
  • 年度 2012
  • 页码 169 p.
  • 总页数 169
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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