Multiplex Targeted Proteomic
Assay for Biomarker Detection
in Plasma: A Pancreatic Cancer Biomarker Case Study
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Abstract
Biomarkers are most frequently proteins that are measured
in the
blood. Their development largely relies on antibody creation to test
the protein candidate performance in blood samples of diseased versus
nondiseased patients. The creation of such antibody assays has been
a bottleneck in biomarker progress due to the cost, extensive time,
and effort required to complete the task. Targeted proteomics is an
emerging technology that is playing an increasingly important role
to facilitate disease biomarker development. In this study, we applied
a SRM-based targeted proteomics platform to directly detect candidate
biomarker proteins in plasma to evaluate their clinical utility for
pancreatic cancer detection. The characterization of these protein
candidates used a clinically well-characterized cohort that included
plasma samples from patients with pancreatic cancer, chronic pancreatitis,
and healthy age-matched controls. Three of the five candidate proteins,
including gelsolin, lumican, and tissue inhibitor of metalloproteinase
1, demonstrated an AUC value greater than 0.75 in distinguishing pancreatic
cancer from the controls. In addition, we provide an analysis of the
reproducibility, accuracy, and robustness of the SRM-based proteomics
platform. This information addresses important technical issues that
could aid in the adoption of the targeted proteomics platform for
practical clinical utility