Cyclic AMP Receptor Protein-Dependent Activation of the Escherichia coli acs P2 Promoter by a Synergistic Class III Mechanism

Author:

Beatty Christine M.1,Browning Douglas F.12,Busby Stephen J. W.2,Wolfe Alan J.1

Affiliation:

1. Department of Microbiology and Immunology, Stritch School of Medicine, Loyola University Chicago, Maywood, Illinois 60153

2. School of Biosciences, University of Birmingham, Birmingham B15 2TT, United Kingdom

Abstract

ABSTRACT The cyclic AMP receptor protein (CRP) activates transcription of the Escherichia coli acs gene, which encodes an acetate-scavenging enzyme required for fitness during periods of carbon starvation. Two promoters direct transcription of acs , the distal acs P1 and the proximal acs P2. In this study, we demonstrated that acs P2 can function as the major promoter and showed by in vitro studies that CRP facilitates transcription by “focusing” RNA polymerase to acs P2. We proposed that CRP activates transcription from acs P2 by a synergistic class III mechanism. Consistent with this proposal, we showed that CRP binds two sites, CRP I and CRP II. Induction of acs expression absolutely required CRP I, while optimal expression required both CRP I and CRP II. The locations of these DNA sites for CRP (centered at positions −69.5 and −122.5, respectively) suggest that CRP interacts with RNA polymerase through class I interactions. In support of this hypothesis, we demonstrated that acs transcription requires the surfaces of CRP and the C-terminal domain of the α subunit of RNA polymerase holoenzyme (α-CTD), which is known to participate in class I interactions: activating region 1 of CRP and the 287, 265, and 261 determinants of the α-CTD. Other surface-exposed residues in the α-CTD contributed to acs transcription, suggesting that the α-CTD may interact with at least one protein other than CRP.

Publisher

American Society for Microbiology

Subject

Molecular Biology,Microbiology

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