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    Towards in vivo estimation of reaction kinetics using high-throughput metabolomics data: a maximum likelihood approach

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    Type
    Article
    Authors
    Zhang, Weiruo
    Kolte, Ritesh cc
    Dill, David L.
    Date
    2015
    Permanent link to this record
    http://hdl.handle.net/10754/673079
    
    Metadata
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    Abstract
    Background: High-throughput assays such as mass spectrometry have opened up the possibility for large-scale in vivo measurements of the metabolome. This data could potentially be used to estimate kinetic parameters for many metabolic reactions. However, high-throughput in vivo measurements have special properties that are not taken into account in existing methods for estimating kinetic parameters, including significant relative errors in measurements of metabolite concentrations and reaction rates, and reactions with multiple substrates and products, which are sometimes reversible. A new method is needed to estimate kinetic parameters taking into account these factors. Results: A new method, InVEst (In Vivo Estimation), is described for estimating reaction kinetic parameters, which addresses the specific challenges of in vivo data. InVEst uses maximum likelihood estimation based on a model where all measurements have relative errors. Simulations show that InVEst produces accurate estimates for a reversible enzymatic reaction with multiple reactants and products, that estimated parameters can be used to predict the effects of genetic variants, and that InVEst is more accurate than general least squares and graphic methods on data with relative errors. InVEst uses the bootstrap method to evaluate the accuracy of its estimates. Conclusions: InVEst addresses several challenges of in vivo data, which are not taken into account by existing methods. When data have relative errors, InVEst produces more accurate and robust estimates. InVEst also provides useful information about estimation accuracy using bootstrapping. It has potential applications of quantifying the effects of genetic variants, inference of the target of a mutation or drug treatment and improving flux estimation.
    Citation
    Zhang, W., Kolte, R., & Dill, D. L. (2015). Towards in vivo estimation of reaction kinetics using high-throughput metabolomics data: a maximum likelihood approach. BMC Systems Biology, 9(1). doi:10.1186/s12918-015-0214-7
    Sponsors
    D.L.D. and W.Z. were supported by a King Abdullah University of Science and Technology (KAUST) research grant under the KAUST Stanford Academic Excellence Alliance program. R.K. was supported by Stanford Graduate Fellowship.
    Publisher
    BMC
    Journal
    BMC SYSTEMS BIOLOGY
    DOI
    10.1186/s12918-015-0214-7
    PubMed ID
    26437964
    PubMed Central ID
    PMC4595320
    Additional Links
    https://bmcsystbiol.biomedcentral.com/articles/10.1186/s12918-015-0214-7
    ae974a485f413a2113503eed53cd6c53
    10.1186/s12918-015-0214-7
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