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      Plasma QconCATs reveal a gender-specific proteomic signature in apheresis platelet plasma supernatants

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          Abstract

          Clinical translation of proteomic technologies is often hampered by technical limitations, including inter-laboratory inconsistencies of label-free derived relative quantification, time-consuming analytical approaches and the subsequent challenge of performing proteomic analyses on large cohorts of subjects. Here we introduce plasma QconCAT-based targeted proteomics, an approach that allows the simultaneous absolute quantitation down to the picogram level of hundreds of proteins in a single liquid chromatography-selected reaction monitoring mass spectrometry run. We demonstrate the robustness of the approach by analyzing apheresis platelet concentrate supernatants at storage day 1 and the end of the shelf life for this blood-derived therapeutic, day 5. The targeted approach was repeatable and robust revealing potential gender-specific signatures across a set of three male and female donors. This technical note represents a proof-of-principle of the application of QconCAT-based MRM strategies to transfusion-medicine relevant issues, such as storage and gender-dependent proteomic signatures in blood-derived therapeutics.

          Biological significance

          Gender differences in the proteome composition of apheresis platelet supernatants have always been postulated, and might underlie a higher risk of adverse reactions when transfusing apheresis products from female donors. Preliminary proteomic studies provided an overview of gender-dependent relative compositional differences in the proteome of apheresis platelet supernatants during routine storage in the blood bank. Here we apply a proteomics approach for absolute quantitation of approximately 100 proteins in apheresis platelet supernatants from male and female donors at storage days 1 and 5. Absolute quantitative proteomic analyses allowed us to confirm and expand on previous observations about gender and storage-dependency of platelet supernatant protein profiles.

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          Author and article information

          Journal
          101475056
          34573
          J Proteomics
          J Proteomics
          Journal of proteomics
          1874-3919
          1876-7737
          25 January 2018
          02 March 2015
          29 April 2015
          01 February 2018
          : 120
          : 1-6
          Affiliations
          University of Colorado Denver School of Medicine, Biochemistry and Molecular Genetics, School of Medicine University of Colorado Denver, Anschutz Medical Campus, Aurora, CO, USA
          Author notes
          [* ] Corresponding author at: Department of Biochemistry and Molecular Genetics, University of Colorado Health Sciences Center, 12801 East 17th Ave., Aurora, CO, USA. Tel.: +1 303 724 5544. kirk.hansen@ 123456UCDenver.edu (K.C. Hansen)
          Article
          PMC5794015 PMC5794015 5794015 nihpa936266
          10.1016/j.jprot.2015.02.010
          5794015
          25743772
          fe7c1275-9cfd-4f35-a531-0b20001313e6
          History
          Categories
          Article

          Transfusion medicine,Donor variability,Storage,Targeted proteomics

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