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A Screen for rfaH Suppressors Reveals a Key Role for a Connector Region of Termination Factor Rho
- Source :
- mBio, Vol 8, Iss 3, p e00753-17 (2017), mBio, mBio, Vol 8, Iss 3 (2017)
- Publication Year :
- 2017
- Publisher :
- American Society for Microbiology, 2017.
-
Abstract
- RfaH activates horizontally acquired operons that encode lipopolysaccharide core components, pili, toxins, and capsules. Unlike its paralog NusG, which potentiates Rho-mediated silencing, RfaH strongly inhibits Rho. RfaH is recruited to its target operons via a network of contacts with an elongating RNA polymerase (RNAP) and a specific DNA element called ops to modify RNAP into a pause- and NusG-resistant state. rfaH null mutations confer hypersensitivity to antibiotics and detergents, altered susceptibility to bacteriophages, and defects in virulence. Here, we carried out a selection for suppressors that restore the ability of a ΔrfaH mutant Escherichia coli strain to grow in the presence of sodium dodecyl sulfate. We isolated rho, rpoC, and hns suppressor mutants with changes in regions previously shown to be important for their function. In addition, we identified mutants with changes in an unstructured region that connects the primary RNA-binding and helicase domains of Rho. The connector mutants display strong defects in vivo, consistent with their ability to compensate for the loss of RfaH, and act synergistically with bicyclomycin (BCM), which has been recently shown to inhibit Rho transformation into a translocation-competent state. We hypothesize that the flexible connector permits the reorientation of Rho domains and serves as a target for factors that control the motor function of Rho allosterically. Our results, together with the existing data, support a model in which the connector segment plays a hitherto overlooked role in the regulation of Rho-dependent termination.<br />IMPORTANCE The transcription termination factor Rho silences foreign DNA, reduces antisense transcription, mediates surveillance of mRNA quality, and maintains genome integrity by resolving transcription-replication collisions and deleterious R loops. Upon binding to RNA, Rho undergoes a rate-limiting transition from an open “lock washer” state to a closed ring capable of processive translocation on, and eventually the release of, the nascent transcript. Recent studies revealed that Rho ligands, including its cofactor NusG and inhibitor bicyclomycin, control the ring dynamics allosterically. In this work, we used a genetic selection for suppressors of RfaH, a potent inhibitor of Rho, to isolate a new class of mutations in a flexible region that connects the primary RNA-binding and ATPase/translocase domains of Rho. We propose that the connector is essential for the modulation of Rho activity by different RNA sequences and accessory proteins.
- Subjects :
- termination
DNA Replication
Models, Molecular
0301 basic medicine
Transcription, Genetic
Termination factor
030106 microbiology
Mutant
Microbiology
Bicyclomycin
03 medical and health sciences
chemistry.chemical_compound
Suppression, Genetic
Rho
Transcription (biology)
Virology
RNA polymerase
Operon
Escherichia coli
Translocase
polarity
RfaH
Genetics
biology
Chemistry
Escherichia coli Proteins
Sodium Dodecyl Sulfate
Helicase
RNA
DNA-Directed RNA Polymerases
Bridged Bicyclo Compounds, Heterocyclic
Peptide Elongation Factors
Rho Factor
QR1-502
Cell biology
030104 developmental biology
Transcription Termination, Genetic
Trans-Activators
biology.protein
Research Article
Subjects
Details
- Language :
- English
- ISSN :
- 21507511
- Volume :
- 8
- Issue :
- 3
- Database :
- OpenAIRE
- Journal :
- mBio
- Accession number :
- edsair.doi.dedup.....c3cc8472f8c5311657fc1a1ad84e9c7e