Literature DB >> 26134708

Improving fold activation of small transcription activating RNAs (STARs) with rational RNA engineering strategies.

Sarai Meyer1, James Chappell1, Sitara Sankar1, Rebecca Chew1, Julius B Lucks2.   

Abstract

Regulatory RNAs have become integral components of the synthetic biology and bioengineering toolbox for controlling gene expression. We recently expanded this toolbox by creating small transcription activating RNAs (STARs) that act by disrupting the formation of a target transcriptional terminator hairpin placed upstream of a gene. While STARs are a promising addition to the repertoire of RNA regulators, much work remains to be done to optimize the fold activation of these systems. Here we apply rational RNA engineering strategies to improve the fold activation of two STAR regulators. We demonstrate that a combination of promoter strength tuning and multiple RNA engineering strategies can improve fold activation from 5.4-fold to 13.4-fold for a STAR regulator derived from the pbuE riboswitch terminator. We then validate the generality of our approach and show that these same strategies improve fold activation from 2.1-fold to 14.6-fold for an unrelated STAR regulator, opening the door to creating a range of additional STARs to use in a broad array of biotechnologies. We also establish that the optimizations preserve the orthogonality of these STARs between themselves and a set of RNA transcriptional repressors, enabling these optimized STARs to be used in sophisticated circuits.
© 2015 Wiley Periodicals, Inc.

Keywords:  RNA engineering; small transcription activating RNA (STAR); synthetic biology; transcriptional activation; transcriptional regulator

Mesh:

Substances:

Year:  2015        PMID: 26134708     DOI: 10.1002/bit.25693

Source DB:  PubMed          Journal:  Biotechnol Bioeng        ISSN: 0006-3592            Impact factor:   4.530


  8 in total

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3.  Applicability of a computational design approach for synthetic riboswitches.

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4.  Attempted use of PACE for riboswitch discovery generates three new translational theophylline riboswitch side products.

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Journal:  BMC Res Notes       Date:  2018-12-05

5.  Exploring of the feature space of de novo developed post-transcriptional riboregulators.

Authors:  Gert Peters; Jo Maertens; Jeroen Lammertyn; Marjan De Mey
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6.  De novo-designed translation-repressing riboregulators for multi-input cellular logic.

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  8 in total

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