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Dive into the research topics where Robin E. Osterhout is active.

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Featured researches published by Robin E. Osterhout.


Nature Chemical Biology | 2009

Absolute Metabolite Concentrations and Implied Enzyme Active Site Occupancy in Escherichia coli

Bryson D. Bennett; Elizabeth Kimball; Melissa Gao; Robin E. Osterhout; Stephen J. Van Dien; Joshua D. Rabinowitz

Absolute metabolite concentrations are critical to a quantitative understanding of cellular metabolism, as concentrations impact both the free energies and rates of metabolic reactions. Here we use liquid chromatography-tandem mass spectrometry to quantify more than 100 metabolite concentrations in aerobic, exponentially growing E. coli with glucose, glycerol, or acetate as the carbon source. The total observed intracellular metabolite pool is approximately 300 mM. A small number of metabolites dominate the metabolome on a molar basis, with glutamate most abundant. Metabolite concentration exceeds Km for most substrate-enzyme pairs. An exception is lower glycolysis, where concentrations of intermediates are near the Km of their consuming enzymes and all reactions are near equilibrium. This may facilitate efficient flux reversibility given thermodynamic and osmotic constraints. The data and analyses presented here highlight the ability to identify organizing metabolic principles from systems-level absolute metabolite concentration data.


Nature Chemical Biology | 2011

Metabolic engineering of Escherichia coli for direct production of 1,4-butanediol

Harry Yim; Robert Haselbeck; Wei Niu; Catherine J. Pujol-Baxley; Anthony P. Burgard; Jeff Boldt; Julia Khandurina; John D. Trawick; Robin E. Osterhout; Rosary Stephen; Jazell Estadilla; Sy Teisan; H Brett Schreyer; Stefan Andrae; Tae Hoon Yang; Sang Yup Lee; Stephen J. Van Dien

1,4-Butanediol (BDO) is an important commodity chemical used to manufacture over 2.5 million tons annually of valuable polymers, and it is currently produced exclusively through feedstocks derived from oil and natural gas. Herein we report what are to our knowledge the first direct biocatalytic routes to BDO from renewable carbohydrate feedstocks, leading to a strain of Escherichia coli capable of producing 18 g l(-1) of this highly reduced, non-natural chemical. A pathway-identification algorithm elucidated multiple pathways for the biosynthesis of BDO from common metabolic intermediates. Guided by a genome-scale metabolic model, we engineered the E. coli host to enhance anaerobic operation of the oxidative tricarboxylic acid cycle, thereby generating reducing power to drive the BDO pathway. The organism produced BDO from glucose, xylose, sucrose and biomass-derived mixed sugar streams. This work demonstrates a systems-based metabolic engineering approach to strain design and development that can enable new bioprocesses for commodity chemicals that are not naturally produced by living cells.


Current Opinion in Biotechnology | 2016

Development of a commercial scale process for production of 1,4-butanediol from sugar.

Anthony P. Burgard; Robin E. Osterhout; Stephen J. Van Dien; Harry Yim

A sustainable bioprocess for the production of 1,4-butanediol (BDO) from carbohydrate feedstocks was developed. BDO is a chemical intermediate that goes into a variety of products including automotive parts, electronics, and apparel, and is currently manufactured commercially through energy-intensive petrochemical processes using fossil raw materials. This review highlights the development of an Escherichia coli strain and an overall process that successfully performed at commercial scale for direct production of bio-BDO from dextrose. Achieving such high level performance required an integrated technology platform enabling detailed engineering of enzyme, pathway, metabolic network, and organism, as well as development of effective fermentation and downstream recovery processes.


Journal of Industrial Microbiology & Biotechnology | 2015

An integrated biotechnology platform for developing sustainable chemical processes.

Nelson Barton; Anthony P. Burgard; Jason S. Crater; Robin E. Osterhout; Priti Pharkya; Brian Steer; Jun Sun; John D. Trawick; Stephen J. Van Dien; Tae Hoon Yang; Harry Yim

Genomatica has established an integrated computational/experimental metabolic engineering platform to design, create, and optimize novel high performance organisms and bioprocesses. Here we present our platform and its use to develop E. coli strains for production of the industrial chemical 1,4-butanediol (BDO) from sugars. A series of examples are given to demonstrate how a rational approach to strain engineering, including carefully designed diagnostic experiments, provided critical insights about pathway bottlenecks, byproducts, expression balancing, and commercial robustness, leading to a superior BDO production strain and process.


Archive | 2009

Microorganisms for the production of adipic acid and other compounds

Anthony P. Burgard; Priti Pharkya; Robin E. Osterhout


Archive | 2010

Microorganisms for the production of 1,4-butanediol and related methods

Stephen J. Van Dien; Anthony P. Burgard; Robert Haselbeck; Catherine J. Pujol-Baxley; Wei Niu; John D. Trawick; Harry Yim; Robin E. Osterhout; Jun Sun


Archive | 2010

Microorganisms and methods for the biosynthesis of adipate, hexamethylenediamine and 6-aminocaproic acid

Anthony P. Burgard; Robin E. Osterhout; Priti Pharkya


Archive | 2009

Microorganisms for the production of 1,4-butanediol

Anthony P. Burgard; Robin E. Osterhout; Jun Sun


Archive | 2010

Microorganisms and methods for the co-production of isopropanol with primary alcohols, diols and acids

Priti Pharkya; Anthony P. Burgard; Robin E. Osterhout; Jun Sun


Archive | 2009

Microorganisms for the production of methacrylic acid

Anthony P. Burgard; Robin E. Osterhout; Priti Pharkya

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Priti Pharkya

Pennsylvania State University

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