Structural basis of transcriptional activation by the OmpR/PhoB-family response regulator PmrA

Author:

Lou Yuan-Chao1,Huang Hsuan-Yu2,Yeh Hsin-Hong3,Chiang Wei-Hung2,Chen Chinpan3,Wu Kuen-Phon24ORCID

Affiliation:

1. Biomedical Translation Research Center, Academia Sinica , Taipei  11529 , Taiwan

2. Institute of Biological Chemistry, Academia Sinica , Taipei  11529 , Taiwan

3. Institute of Biomedical Sciences, Academia Sinica , Taipei  11529 , Taiwan

4. Institute of Biochemical Sciences, College of Life Science, National Taiwan University , Taipei  10617 , Taiwan

Abstract

Abstract PmrA, an OmpR/PhoB-family response regulator, triggers gene transcription responsible for polymyxin resistance in bacteria by recognizing promoters where the canonical-35 element is replaced by the pmra-box, representing the PmrA recognition sequence. Here, we report a cryo-electron microscopy (cryo-EM) structure of a bacterial PmrA-dependent transcription activation complex (TAC) containing a PmrA dimer, an RNA polymerase σ70 holoenzyme (RNAPH) and the pbgP promoter DNA. Our structure reveals that the RNAPH mainly contacts the PmrA C-terminal DNA-binding domain (DBD) via electrostatic interactions and reorients the DBD three base pairs upstream of the pmra-box, resulting in a dynamic TAC conformation. In vivo assays show that the substitution of the DNA-recognition residue eliminated its transcriptional activity, while variants with altered RNAPH-interacting residues resulted in enhanced transcriptional activity. Our findings suggest that both PmrA recognition-induced DNA distortion and PmrA promoter escape play crucial roles in its transcriptional activation.

Funder

Ministry of Science and Technology of Taiwan

Academia Sinica

Publisher

Oxford University Press (OUP)

Subject

Genetics

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