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Download fileMultiplexed MRM with Internal Standards for Cerebrospinal Fluid Candidate Protein Biomarker Quantitation
journal contribution
posted on 2014-08-01, 00:00 authored by Andrew
J. Percy, Juncong Yang, Andrew G. Chambers, Romain Simon, Darryl B. Hardie, Christoph H. BorchersMultiplexed quantitation is essential
for discovering, verifying,
and validating biomarkers for risk stratification, disease prognostication,
and therapeutic monitoring. The most promising strategy for quantifying
unverified protein biomarkers in biofluids relies on selected/multiple
reaction monitoring (SRM or MRM) technology with isotopically labeled
standards employed within a bottom-up proteomic workflow. Since cerebrospinal
fluid (CSF) is an important fluid for studying central nervous system
(CNS) related diseases, we sought to develop a rapid, antibody- and
fractionation-free MRM-based approach with a complex mixture of peptide
standards to quantify a highly multiplexed panel of candidate protein
biomarkers in human CSF. Development involved peptide transition optimization,
denaturation/digestion protocol evaluation, transition interference
screening, and protein quantitation via peptide standard curves. The
final method exhibited excellent reproducibility (average coefficient
of variation of <1% for retention time and <6% for signal) and
breadth of quantitation (130 proteins from 311 interference-free peptides)
in a single 43-min run. These proteins are of high-to-low abundance
with determined concentrations from 118 μg/mL (serum albumin)
to 550 pg/mL (apolipoprotein C-I). Overall, the method consists of
the most highly multiplexed and broadest panel of candidate protein
biomarkers in human CSF reported thus far and is well suited for subsequent
verification studies on patient samples.
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Keywords
peptide standardsquantifying unverified protein biomarkersverification studiestransition interference screeningrisk stratificationretention timecandidate protein biomarkersmultiplexed panelprotein quantitationInternal StandardsCSFpeptide transition optimizationpatient samplescerebrospinal fluidSRMCerebrospinal Fluid Candidate Protein Biomarker QuantitationMultiplexed quantitationdisease prognosticationMultiplexed MRMCNSserum albumin