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- W2135965013 abstract "Disease and drugs can modulate the concentrations of hundreds of proteins in the blood which can be accurately measured using contemporary proteomic methods. Nevertheless, it is common practice to reduce the plurality of disease and drug effects by a few proteins for the pragmatic purposes of immunoassay development. The vast majority of putative biomarkers discovered by this reductionist approach never reach the clinic for two reasons: the prohibitive time and cost of assay development and the acute risk of a reduced protein panel failing when validated on a broader cross-section of the population. Global Proteomics is an alternate methodology where all blood proteins modulated by disease or drug are used to r esolve pharmacodynamic questions without the time, cost, and risk of developing an immunoassay . The Global Proteomic approach was applied to an Alzheimer study where it was demonstrated that a large panel of plasma proteins is pr edictive of disease severity (as measured by the Mini Mental State Examination). Furthermore, a subset of this panel was shown to be modulated by disease treatment (donepezil), thereby providing a means to quantify response to tr eatment. Finally, to establish that the Global Proteomics methodology has broad utility, it was also applied to a Hypertension study, illustrating that a panel of plasma proteins can also be derived that are corr elated with disease severity (as measured by blood pressure). In par ticular, the Global Proteomics methodology can readily distinguish patients responsive and non-responsive to hypertension therapies. The Global Proteomics approach is based upon a bioinformatics analysis approach which clusters samples by proteomic similarity and then uses a geometric representation of sample similarity to answer common pharmacodynamic questions." @default.
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- W2135965013 date "2008-10-02" @default.
- W2135965013 modified "2023-09-27" @default.
- W2135965013 title "Global Proteomics: Pharmacodynamic Decision Making via Geometric Interpretations of Proteomic Analyses" @default.
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- W2135965013 doi "https://doi.org/10.4172/jpb.1000040" @default.
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