Constitutively signaling fragments of Tsr, the Escherichia coli serine chemoreceptor.

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J Bacteriol. 1994 October; 176(20): 6340-6348

research-article

Constitutively signaling fragments of Tsr, the Escherichia coli serine chemoreceptor.

P Ames and J S Parkinson

Biology Department, University of Utah, Salt Lake City 84112.

ABSTRACT

Tsr, the serine chemoreceptor of Escherichia coli, has two signalingmodes. One augments clockwise (CW) flagellar rotation, and theother augments counterclockwise (CCW) rotation. To identifythe portion of the Tsr molecule responsible for these activities,we isolated soluble fragments of the Tsr cytoplasmic domainthat could alter the flagellar rotation patterns of unstimulatedwild-type cells. Residues 290 to 470 from wild-type Tsr generateda CW signal, whereas the same fragment with a single amino acidreplacement (alanine 413 to valine) produced a CCW signal. Thesoluble components of the chemotaxis phosphorelay system neededfor expression of these Tsr fragment signals were identifiedby epistasis analysis. Like full-length receptors, the fragmentsappeared to generate signals through interactions with the CheAautokinase and the CheW coupling factor. CheA was required forboth signaling activities, whereas CheW was needed only forCW signaling. Purified Tsr fragments were also examined foreffects on CheA autophosphorylation activity in vitro. Consistentwith the in vivo findings, the CW fragment stimulated CheA,whereas the CCW fragment inhibited CheA. CheW was required forstimulation but not for inhibition. These findings demonstratethat a 180-residue segment of the Tsr cytoplasmic domain canproduce two active signals. The CCW signal involves a directcontact between the receptor and the CheA kinase, whereas theCW signal requires participation of CheW as well. The correlationbetween the in vitro effects of Tsr signaling fragments on CheAactivity and their in vivo behavioral effects lends convincingsupport to the phosphorelay model of chemotactic signaling.

J Bacteriol. 1994 October; 176(20): 6340-6348

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