A single point mutation in the Listeria monocytogenes ribosomal gene rpsU enables SigB activation independently of the stressosome and the anti-sigma factor antagonist RsbV

Ma, Xuchuan; Tempelaars, Marcel H.; Zwietering, Marcel H.; Boeren, Sjef; O’Byrne, Conor P.; den Besten, Heidy M. W.; Abee, Tjakko

doi:10.3389/fmicb.2024.1304325

Cited by 2 publications

(1 citation statement)

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“…The signal of energy/nutritional stress enters the SigB activation pathway probably downstream from RsbU (Shin et al, 2010). Our recent study also showed that the SigB activation in RpsU 17Arg-Pro mutants is independent from the stressosome and the anti-sigma factor antagonist RsbV (Ma et al, 2024). It is conceivable that altered ribosomal function in the RpsU mutant results in poor growth performance, with the mechanisms underlying SigB activation and possible link to nutritional stress requiring further study.…”

Section: Discussionmentioning

confidence: 88%

Ribosomal mutations enable a switch between high fitness and high stress resistance in Listeria monocytogenes

Koomen,

Ma,

Bombelli

et al. 2024

Front. Microbiol.

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Multiple stress resistant variants of Listeria monocytogenes with mutations in rpsU encoding ribosomal protein RpsU have previously been isolated after a single exposure to acid stress. These variants, including L. monocytogenes LO28 variant V14 with a complete deletion of the rpsU gene, showed upregulation of the general stress sigma factor Sigma B-mediated stress resistance genes and had a lower maximum specific growth rate than the LO28 WT, signifying a trade-off between stress resistance and fitness. In the current work V14 has been subjected to an experimental evolution regime, selecting for higher fitness in two parallel evolving cultures. This resulted in two evolved variants with WT-like fitness: 14EV1 and 14EV2. Comparative analysis of growth performance, acid and heat stress resistance, in combination with proteomics and RNA-sequencing, indicated that in both lines reversion to WT-like fitness also resulted in WT-like stress sensitivity, due to lack of Sigma B-activated stress defense. Notably, genotyping of 14EV1 and 14EV2 provided evidence for unique point-mutations in the ribosomal rpsB gene causing amino acid substitutions at the same position in RpsB, resulting in RpsB22Arg-His and RpsB22Arg-Ser, respectively. Combined with data obtained with constructed RpsB22Arg-His and RpsB22Arg-Ser mutants in the V14 background, we provide evidence that loss of function of RpsU resulting in the multiple stress resistant and reduced fitness phenotype, can be reversed by single point mutations in rpsB leading to arginine substitutions in RpsB at position 22 into histidine or serine, resulting in a WT-like high fitness and low stress resistance phenotype. This demonstrates the impact of genetic changes in L. monocytogenes’ ribosomes on fitness and stress resistance.

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Section: Discussionmentioning

confidence: 88%