Structural insights into the unique mechanism of transcription activation by Caulobacter crescentus GcrA

Canonical bacterial transcription activators bind to non-transcribed promoter elements to increase transcription of their target genes. Here we report crystal structures of binary complexes comprising domains of Caulobacter crescentus GcrA, a noncanonical bacterial transcription factor, that support...

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Bibliographic Details
Main Authors: Wu, Xiaoxian, Shen, Liqiang, Zhuang, Ningning, Zhang, Yu, Haakonsen, Diane Laure, Sanderlin, Allen G, Liu, Yue, Laub, Michael T
Other Authors: Massachusetts Institute of Technology. Department of Biology
Format: Article
Published: Oxford University Press 2018
Online Access:http://hdl.handle.net/1721.1/115371
https://orcid.org/0000-0002-4668-1695
https://orcid.org/0000-0002-8288-7607
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Summary:Canonical bacterial transcription activators bind to non-transcribed promoter elements to increase transcription of their target genes. Here we report crystal structures of binary complexes comprising domains of Caulobacter crescentus GcrA, a noncanonical bacterial transcription factor, that support a novel mechanism for transcription activation through the preferential binding of methylated cis-regulatory elements and the promotion of open complex formation through an interaction with region 2 of the principal σ factor, σ70. We present crystal structures of the C-terminal, σ factor-interacting domain (GcrA-SID) in complex with domain 2 of σ70 (σ702), and the N-terminal, DNA-binding domain (GcrA-DBD) in complex with methylated double-stranded DNA (dsDNA). The structures reveal interactions essential for transcription activation and DNA recognition by GcrA. These structures, along with mutational analyses, support a mechanism of transcription activation in which GcrA associates with RNA polymerase (RNAP) prior to promoter binding through GcrA-SID, arming RNAP with a flexible GcrA-DBD. The RNAP-GcrA complex then binds and activates target promoters harboring a methylated GcrA binding site either upstream or downstream of the transcription start site.