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Engineering allostery

Journal

TRENDS IN GENETICS
Volume 30, Issue 12, Pages 521-528

Publisher

ELSEVIER SCIENCE LONDON
DOI: 10.1016/j.tig.2014.09.004

Keywords

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Funding

  1. Wyss Technology Development Fellowship
  2. US Department of Energy [DE-FG02-02ER63445]
  3. US National Institutes of Health [P41 GM103533]

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Allosteric proteins have great potential in synthetic biology, but our limited understanding of the molecular underpinnings of allostery has hindered the development of designer molecules, including transcription factors with new DNA-binding or ligand-binding specificities that respond appropriately to inducers. Such allosteric proteins could function as novel switches in complex circuits, metabolite sensors, or as orthogonal regulators for independent, inducible control of multiple genes. Advances in DNA synthesis and next-generation sequencing technologies have enabled the assessment of millions of mutants in a single experiment, providing new opportunities to study allostery. Using the classic Lad protein as an example, we describe a genetic selection system using a bidirectional reporter to capture mutants in both allosteric states, allowing the positions most crucial for allostery to be identified. This approach is not limited to bacterial transcription factors, and could reveal new mechanistic insights and facilitate engineering of other major classes of allosteric proteins such as nuclear receptors, two-component systems, G protein-coupled receptors, and protein kinases.

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