Sinorhizobium meliloti CtrA Stability Is Regulated in a CbrA-Dependent Manner That Is Influenced by CpdR1

Abstract

ABSTRACTCbrA is a DivJ/PleC-like histidine kinase of DivK that is required for cell cycle progression and symbiosis in the alphaproteobacteriumSinorhizobium meliloti. Loss ofcbrAresults in increased levels of CtrA as well as its phosphorylation. While many of the knownCaulobacter crescentusregulators of CtrA phosphorylation and proteolysis are phylogenetically conserved withinS. meliloti, the latter lacks the PopA regulator that is required for CtrA degradation inC. crescentus. In order to investigate whether CtrA proteolysis occurs inS. meliloti, CtrA stability was assessed. During exponential growth, CtrA is unstable and therefore likely to be degraded in a cell cycle-regulated manner. Loss ofcbrAsignificantly increases CtrA stability, but this phenotype is restored to that of the wild type by constitutive ectopic expression of a CpdR1 variant that cannot be phosphorylated (CpdR1D53A). Addition of CpdR1D53Afully suppressescbrAmutant cell cycle defects, consistent with regulation of CtrA stability playing a key role in mediating proper cell cycle progression inS. meliloti. Importantly, thecbrAmutant symbiosis defect is also suppressed in the presence of CpdR1D53A. Thus, regulation of CtrA stability by CbrA and CpdR1 is associated with free-living cell cycle outcomes and symbiosis.IMPORTANCEThe cell cycle is a fundamental process required for bacterial growth, reproduction, and developmental differentiation. Our objective is to understand how a two-component signal transduction network directs cell cycle events during free-living growth and host colonization. TheSinorhizobium melilotinitrogen-fixing symbiosis with plants is associated with novel cell cycle events. This study identifies a link between the regulated stability of an essential response regulator, free-living cell cycle progression, and symbiosis.