Rapid Generation of Sequence-diverse Terminator Libraries and Their Parameterization Using Quantitative Term-Seq

Overview

Journal Synth Biol (Oxf)

Publisher Oxford University Press

Date 2020 Sep 30

PMID 32995547

Citations 10

Authors

Andrew J Hudson

Hans-Joachim Wieden

Affiliations

Soon will be listed here.

Abstract

Synthetic biology and the rational design and construction of biological devices require vast numbers of characterized biological parts, as well as reliable design tools to build increasingly complex, multigene architectures. Design principles for intrinsic terminators have been established; however, additional sequence-structure studies are needed to refine parameters for termination-based genetic devices. We report a rapid single-pot method to generate libraries of thousands of randomized bidirectional intrinsic terminators and a modified quantitative Term-Seq (qTerm-Seq) method to simultaneously identify terminator sequences and measure their termination efficiencies (TEs). Using qTerm-Seq, we characterize hundreds of additional strong terminators (TE > 90%) with some terminators reducing transcription read-through by up to 1000-fold in . Our terminator library and qTerm-Seq pipeline constitute a flexible platform enabling identification of terminator parts that can achieve transcription termination not only over a desired range but also to investigate their sequence-structure features, including for specific genetic and application contexts beyond the common systems such as .

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