Binding of the C-terminal Domain of the Alpha Subunit of RNA Polymerase to the Phage Mu Middle Promoter

Overview

Journal J Bacteriol

Publisher American Society for Microbiology

Specialty Microbiology

Date 2004 Nov 18

PMID 15547256

Citations 2

Authors

Ji Ma

Martha M Howe

Affiliations

Soon will be listed here.

Abstract

The C-terminal domain of the alpha subunit (alpha CTD) of Escherichia coli RNA polymerase is often involved in transcriptional regulation. The alpha CTD typically stimulates transcription via interactions with promoter UP element DNA and transcriptional activators. DNase I footprinting and gel mobility shift assays were used to look for potential interaction of the alpha CTD with the phage Mu middle promoter P(m) and its activator protein Mor. Binding of RNA polymerase to P(m) in the presence of Mor resulted in production of a DNase I footprint downstream of Mor due to open complex formation and generation of a second footprint just upstream of the Mor binding site. Generation of the upstream footprint did not require open complex formation and also occurred in reactions in which the alpha CTD or His-alpha proteins were substituted for RNA polymerase. In gel mobility shift assays, the formation of a supershifted ternary complex demonstrated that Mor and His-alpha bind synergistically to P(m) DNA. Gel shift assays with short DNA fragments demonstrated that only the Mor binding site and a single upstream alpha CTD binding site were required for ternary complex formation. These results suggest that the alpha CTD plays a role in P(m) transcription by binding to P(m) DNA just upstream from Mor and making protein-protein interactions with Mor that stabilize the binding of both proteins.

Citing Articles

The phage Mu middle promoter Pm contains a partial UP element.

Ma J, Howe M G3 (Bethesda). 2015; 5(4):507-16.

PMID: 25645531 PMC: 4390567. DOI: 10.1534/g3.114.013607.

Genetic analysis of phage Mu Mor protein amino acids involved in DNA minor groove binding and conformational changes.

Kumaraswami M, Avanigadda L, Rai R, Park H, Howe M J Biol Chem. 2011; 286(41):35852-35862.

PMID: 21859715 PMC: 3195604. DOI: 10.1074/jbc.M111.269860.

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