4.7 Article

RNA Sequence and Structure Determinants of Pol III Transcriptional Termination in Human Cells

JOURNAL OF MOLECULAR BIOLOGY (2021)

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Journal

JOURNAL OF MOLECULAR BIOLOGY
Volume 433, Issue 13, Pages -

Publisher

ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD
DOI: 10.1016/j.jmb.2021.166978

Keywords

transcription; termination; RNA polymerase III; aptamer; synthetic biology

Categories

Biochemistry & Molecular Biology

Funding

  1. Northwestern University's Graduate School Cluster in Biotechnology, System, and Synthetic Biology
  2. National Institutes of Health Training Grant through Northwestern University's Biotechnology Training Program [T32GM008449]
  3. National Institutes of Health Training Grant through Northwestern University's Molecular Biophysics Training Program [T32GM008382]
  4. Northwestern University - Flow Cytometry Core Facility - Cancer Center Support Grant [NCI CA060553]
  5. National Institute of Biomedical Imaging and Bioengineering [1R01EB026510]
  6. NSF CAREER [1452441]
  7. National Institute for General Medicine Sciences [R01GM130901]

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Through the newly developed in cellulo Pol III transcription termination assay, it was found that efficient Pol III termination requires the cooperation of poly-U tracts, RNA sequence, and structural elements in nascent RNA. Different promoter types have different requirements for transcription termination.
The precise mechanism of transcription termination of the eukaryotic RNA polymerase III (Pol III) has been a subject of considerable debate. Although previous studies have clearly shown that multiple uracils at the end of RNA transcripts are required for Pol III termination, the effects of upstream RNA secondary structure in the nascent transcript on transcriptional termination is still unclear. To address this, we developed an in cellulo Pol III transcription termination assay using the recently developed Tornado-Corn RNA aptamer system to create a Pol III-transcribed RNA that produces a detectable fluorescent signal when transcribed in human cells. To study the effects of RNA sequence and structure on Pol III termination, we systematically varied the sequence context upstream of the aptamer and identified sequence characteristics that enhance or diminish termination. For transcription from Pol III type 3 promoters, we found that only poly-U tracts longer than the average length found in the human genome efficiently terminate Pol III transcription without RNA secondary structure elements. We observed that RNA secondary structure elements placed in proximity to shorter poly-U tracts induced termination, and RNA secondary structure by itself was not sufficient to induce termination. For Pol III type 2 promoters, we found that the shorter poly-U tract lengths of 4 uracils were sufficient to induce termination. These findings demonstrate a key role for sequence and structural elements within Pol III-transcribed nascent RNA for efficient transcription termination, and demonstrate a generalizable assay for characterizing Pol III transcription in human cells. (C) 2021 Elsevier Ltd. All rights reserved.

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