Author:
Andres Tennus

Doctoral defence: Sirli Rosendahl “Fitness effects of chromosomal toxin-antitoxin systems in Pseudomonas putida”

On 22 August at 10:15 Sirli Rosendahl will defend her doctoral thesis “Fitness effects of chromosomal toxin-antitoxin systems in Pseudomonas putida for obtaining the degree of Doctor of Philosophy (in Molecular Biology).

Supervisor:
Associate Professor Rita Hõrak, University of Tartu

Oponent:
Professor Pierre Genevaux, Paul Sabatier University (Toulouse, France)

Summary:

Image
Sirli Rosendahl

Most bacteria encode small genetic modules called toxin-antitoxin (TA) systems in their chromosome, which consist of a poisonous toxin and its antidote. It is puzzling why such potentially lethal genetic elements are so widely distributed among bacteria and this could indicate that TA systems benefit their host in some way. The functions of chromosomal TA systems have been intensely studied, but no consensus regarding their importance to bacteria has been reached. Some TA systems have been shown to stabilize mobile genomic DNA, while others can protect bacteria against phages, and some have been proposed to participate in bacterial stress response regulation. However, there are also studies that cannot detect any beneficial effect of TA systems and propose that they are generally selfish DNA elements. This thesis focuses on the chromosomal TA systems of the soil bacterium Pseudomonas putida. The most thoroughly studied P. putida TA system is GraTA. While the toxin GraT is a ribosome-dependent mRNAse, it is conditionally toxic and causes cold-sensitive ribosome biogenesis defect. Interestingly, the major cellular chaperone DnaK was implicated in GraT-caused ribosome biogenesis defect, yet the exact role of DnaK in GraT toxicity has remained unclear. Even though the toxin GraT is functional and can affect the stress tolerance of P. putida in the absence of the antitoxin GraA, the whole TA system deletion has no fitness effects. This raises the question about the importance of GraTA along with other TA systems encoded in P. putida genome. This thesis describes the cellular changes that take place in P. putida cells lacking the antitoxin GraA and shows that DnaK enhances GraT toxicity, probably by helping GraT attain its proper fold. This work shows that TA systems are not beneficial to P. putida. Instead, they can be costly to P. putida in competition assays and during phage invasion. The results of this thesis shed light onto the biological importance of TA systems and clearly point to the selfish nature of TA systems.

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