AUTHOR=Knöppel Anna , Andersson Dan I. , Näsvall Joakim 

TITLE=Synonymous Mutations in rpsT Lead to Ribosomal Assembly Defects That Can Be Compensated by Mutations in fis and rpoA

JOURNAL=Frontiers in Microbiology

VOLUME=11

YEAR=2020

URL=https://www.frontiersin.org/journals/microbiology/articles/10.3389/fmicb.2020.00340

DOI=10.3389/fmicb.2020.00340

ISSN=1664-302X

ABSTRACT=<p>We previously described how four deleterious synonymous mutations in the <italic>Salmonella enterica rpsT</italic> gene (encoding ribosomal protein S20) result in low S20 levels that can be compensated by mutations that restore [S20]. Here, we have further studied the cause for the deleterious effects of S20 deficiency and found that the S20 mutants were also deficient in four other 30S proteins (S1, S2, S12, and S21), which is likely due to an assembly defect of the S20 deficient 30S subunits. We examined the compensatory effect by six additional mutations affecting the global regulator Fis and the C-terminal domain of the α subunit of RNA polymerase (encoded by <italic>rpoA</italic>). The <italic>fis</italic> and <italic>rpoA</italic> mutations restored the S20 levels, concomitantly restoring the assembly defect and the levels of S1, S2, S12, and S21. These results illustrate the complexity of compensatory evolution and how the negative effects of deleterious mutations can be suppressed by a multitude of mechanisms. Additionally, we found that the mutations in <italic>fis</italic> and <italic>rpoA</italic> caused reduced expression of other ribosomal components. Notably, some of the <italic>fis</italic> mutations and the <italic>rpoA</italic> mutation corrected the fitness of the <italic>rpsT</italic> mutants to wild-type levels, although expression of other ribosomal components was reduced compared to wild-type. This finding raises new questions regarding the relation between translation capacity and growth rate.</p>