2017
DOI: 10.1016/j.jmb.2017.02.007
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Signaling Consequences of Structural Lesions that Alter the Stability of Chemoreceptor Trimers of Dimers

Abstract: Residues E402 and R404 of the E. coli serine chemoreceptor, Tsr, appear to form a salt bridge that spans the interfaces between neighboring dimers in the Tsr trimer of dimers, a key structural component of receptor core signaling complexes. To assess their functional roles we constructed full sets of single amino acid replacement mutants at E402 and R404 and characterized their signaling behaviors with a suite of in vivo assays. Our results indicate that the E402 and R404 residues of Tsr play their most critic… Show more

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Cited by 17 publications
(17 citation statements)
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“…S6). Interestingly, not only known intradimer contacts, e.g., a conserved phenylalanine corresponding to F396 in Tsr (28), but also some of the contacts critical for the trimer-of-dimer formation, e.g., positions corresponding to E402 and R404 in Tsr (29), are preserved in MCP HKIII (see Fig. S6).…”
Section: Resultsmentioning
confidence: 99%
“…S6). Interestingly, not only known intradimer contacts, e.g., a conserved phenylalanine corresponding to F396 in Tsr (28), but also some of the contacts critical for the trimer-of-dimer formation, e.g., positions corresponding to E402 and R404 in Tsr (29), are preserved in MCP HKIII (see Fig. S6).…”
Section: Resultsmentioning
confidence: 99%
“…Structural changes in the receptor's hairpin tip region (Fig. 1) that produce a wide range of signaling behaviors did not potentiate the CheR effect (53)(54)(55). Perhaps the receptor methylation helices, whose conformation and packing stability are under direct control by the HAMP domain, are central to the CheR effect.…”
Section: A Possible Nonequilibrium Mechanism For Cher Response Enhancmentioning
confidence: 95%
“…We modified the RapidCell (RC) model to simulate chemotactic motility of the ECP with the premise that the ECP mimics E. coli chemotaxis in the presence of two unmixed chemoattractants. The RC model [17] was originally developed to simulate flagellar bacterial chemotaxis in an environment with a spatiotemporally varying concentration gradient of a single chemoattractant, and performs two tasks: chemoattractant signal processing by the methyl-accepting chemotaxis protein (MCP) sensory lattice and adaptive feedback response of the sensory array [16,[23][24][25]. Signal processing by the cell occurs through interactions between chemoattractant-activated chemoreceptors, CheA kinase, and other regulators including CheY, CheR, CheB, and CheZ ( Figure 2).…”
Section: Module 1 Modified Rapidcell (Mrc) Model For Particle Chemosmentioning
confidence: 99%