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UK funding (98 534 £) : Co-localisation et agrégation d’enzymes pour une activité métabolique accrue pour les produits chimiques de base Ukri01/09/2016 UK Research and Innovation, Royaume Uni
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Co-localisation et agrégation d’enzymes pour une activité métabolique accrue pour les produits chimiques de base
| Abstract | Bio-based alternatives to petrochemical commodities, which are required as inputs into a variety of industrial applications such as polymers, coatings and surfactants, are predicted to rise from 2% to 25% of global production over the next ten years. The international chemical market is currently worth around $4 trillion with bio-production offering advantages such as environmental sustainability, cheaper production costs and protection from oil-price volatility. Approaches such as metabolic engineering and synthetic biology can be used to make bio-products and processes more efficient and cost competitive, and are fueling innovation in the chemical industry. In this application we outline a method that offers the potential for a significant step-change in bio-commodity production of a chemical called 1,3-butanediol through the development of intracellular enzyme-aggregates. We will apply this technology to specific bacteria called acetogens that can live on gaseous exhaust fumes. The project brings together 2 existing and protected technologies (background IP from the University of Kent and ZuvaSyntha) to exemplify the use of enzyme-aggregates in a commercially important strain capable of synthesising commodity chemicals and generate possible novel foreground IP under a joint venture. The use of bacterial microcompartment-derived tags (such as P18 and D18) will be used to provide an intracellular scaffold for the co-localisation of multi-enzyme pathways in microrgansms offering the opportunity to increase flux and catalytic efficiency and protect sensitive intracellular features from the potentially toxic oxyfunctionalised intermediates that arise within the cell. ZuvaSyntha's novel metabolic pathway for the transformation of acetic acid into 1,3-butanediol has been developed for use in anaerobic microorganisms and has been shown by computational metabolic modelling (Prof. David Fell, Oxford Brookes University) to be capable of efficiently converting syngas to BD. By producing the metabolic enzymes with P18 or D18 incorporated into their N-terminii the protein will assemble into an enzyme-aggregate that will represent an internal cellular bioreactor. Such an approach will generate microbial cell factories with significantly enhanced metabolic function. The results of this project will determine to what extent protein scaffolds and aggregates can be used in acetogens to enhance their metabolic capability for the production of metabolites that are generated via toxic intermediates. The research will reveal the scope to which these various aggregates can be redesigned and re-engineered for the synthesis of important commodities. In so doing the research will provide primary data on the potential that scaffolds have for application in syngas fermentation, through the enhancement of specific metabolic process that are associated with the production of important platform chemicals. The research will also help define an important area of synthetic biology, permitting the exploitation of scaffolds and addressing the basic advantages of internal bioreactors in biology. In this respect, the research will be of general interest to those in applied areas of the biotechnology industry, especially those interested in metabolic engineering. More specifically it will also provide a highly advanced system for the generation of an important commodity chemical in the form of 1,3-butanediol. |
| Category | Research Grant |
| Reference | BB/N023722/1 |
| Status | Closed |
| Funded period start | 01/09/2016 |
| Funded period end | 31/10/2017 |
| Funded value | £98 534,00 |
| Source | https://gtr.ukri.org/projects?ref=BB%2FN023722%2F1 |
Participating Organisations
| University of Kent |
Cette annonce se réfère à une date antérieure et ne reflète pas nécessairement l’état actuel. L’état actuel est présenté à la page suivante : University of Kent, Canterbury, Royaume Uni.