Balanced cell division is secured by two different regulatory sites in OxyS RNA

Author:

Elgrably-Weiss Maya,Hussain Fayyaz,Georg Jens,Shraiteh Bushra,Altuvia Shoshy

Abstract

The hydrogen peroxide-induced small RNA OxyS has been proposed to originate from the 3′ UTR of a peroxide mRNA. Unexpectedly, phylogenetic OxyS targetome predictions indicate that most OxyS targets belong to the category of “cell cycle,” including cell division and cell elongation. Previously, we reported thatEscherichia coliOxyS inhibits cell division by repressing expression of the essential transcription termination factornusG, thereby leading to the expression of the KilR protein, which interferes with the function of the major cell division protein, FtsZ. By interfering with cell division, OxyS brings about cell-cycle arrest, thus allowing DNA damage repair. Cell division and cell elongation are opposing functions to the extent that inhibition of cell division requires a parallel inhibition of cell elongation for the cells to survive. In this study, we report that in addition to cell division, OxyS inhibitsmepS, which encodes an essential peptidoglycan endopeptidase that is responsible for cell elongation. Our study indicates that cell-cycle arrest and balancing between cell division and cell elongation are important and conserved functions of the oxidative stress-induced sRNA OxyS.

Funder

Israel Science Foundation

the Israel Academy of Sciences and Humanities

Deutsche Forschungsgemeinschaft

Publisher

Cold Spring Harbor Laboratory

Subject

Molecular Biology

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