Abstract

Most pathways for bacterial chemotaxis involve methylation of the sensory transducer. Studies in this laboratory are concerned with methylation-independent pathways in Salmonella typhimurium and Escherichia coli for chemotaxis to oxygen (aerotaxis) and to sugars transported by the phosphotransferase system (PTS). The methylation-independent and the methylation-dependent pathways converge before the switch that controls the direction of rotation of the flagellar motors. The interaction between these pathways and also the point of convergence will be investigated. The mechanism by which transducer methylation is depressed by substrates of the PTS, and the role of cGMP in this phenomenon will be studied using behavior, in vitro assays of transducer methylation and demethylation, and protein chemistry. It is proposed to determine the mechanism by which deletion of protein methylesterase (CheB) inverts the aerotactic response. Chemotaxis to PTS sugars is unique in requiring an intact transport system for the attractant. It is proposed to identify the components necessary for sensory transduction, their function, and particularly the mechanism of adaption. Initial investigations will be concerned with the phosphorylatio of PTS components at sites other than the active site. Aerotaxis is mediated by a """"""""protometer"""""""" that detects changes in the proton motive force and transmits a signal that results in appropriate behavioral change. As a first step toward the long range goal of identifying and characterizing the components of the aerotactic system, E. coli mutants in aerotaxis wilal be selected, mapped and characterized. The mechanism of the repellent response to high concentrations of oxygen will be investigated. ATP is required for either signal transmission or the flagella switch. 8-Azidoadenosine added to the cells can substitute for adenine in activating chemotaxis. After confirming the formation of azidoadenosine triphosphate, the cells will be irradiated and fractionated to identify ATP-binding components of the chemotactic pathway. Subsequently, the mode of action of ATP in chemotaxis will be determined.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM029481-04A1
Application #
3277098
Study Section
Microbial Physiology and Genetics Subcommittee 2 (MBC)
Project Start
1981-09-28
Project End
1990-08-31
Budget Start
1985-09-18
Budget End
1986-08-31
Support Year
4
Fiscal Year
1985
Total Cost
Indirect Cost

  Institution

Name
Loma Linda University
Department
Type
School of Medicine & Dentistry
DUNS #
City
Loma Linda
State
CA
Country
United States
Zip Code
92350

  Publications

Watts, Kylie J; Johnson, Mark S (2018) Analyzing Protein Domain Interactions in Chemoreceptors by In Vivo PEGylation. Methods Mol Biol 1729:137-145
Garcia, Darysbel; Watts, Kylie J; Johnson, Mark S et al. (2016) Delineating PAS-HAMP interaction surfaces and signalling-associated changes in the aerotaxis receptor Aer. Mol Microbiol 100:156-72
Watts, Kylie J; Johnson, Mark S; Taylor, Barry L (2011) Different conformations of the kinase-on and kinase-off signaling states in the Aer HAMP domain. J Bacteriol 193:4095-103
Watts, Kylie J; Taylor, Barry L; Johnson, Mark S (2011) PAS/poly-HAMP signalling in Aer-2, a soluble haem-based sensor. Mol Microbiol 79:686-99
Campbell, Asharie J; Watts, Kylie J; Johnson, Mark S et al. (2011) Role of the F1 region in the Escherichia coli aerotaxis receptor Aer. J Bacteriol 193:358-66
Campbell, Asharie J; Watts, Kylie J; Johnson, Mark S et al. (2010) Gain-of-function mutations cluster in distinct regions associated with the signalling pathway in the PAS domain of the aerotaxis receptor, Aer. Mol Microbiol 77:575-86
Airola, Michael V; Watts, Kylie J; Bilwes, Alexandrine M et al. (2010) Structure of concatenated HAMP domains provides a mechanism for signal transduction. Structure 18:436-48
Watts, Kylie J; Johnson, Mark S; Taylor, Barry L (2008) Structure-function relationships in the HAMP and proximal signaling domains of the aerotaxis receptor Aer. J Bacteriol 190:2118-27
Taylor, Barry L; Watts, Kylie J; Johnson, Mark S (2007) Oxygen and redox sensing by two-component systems that regulate behavioral responses: behavioral assays and structural studies of aer using in vivo disulfide cross-linking. Methods Enzymol 422:190-232
Taylor, Barry L (2007) Aer on the inside looking out: paradigm for a PAS-HAMP role in sensing oxygen, redox and energy. Mol Microbiol 65:1415-24

Showing the most recent 10 out of 44 publications