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Proteomics of prostate cancer serum and plasma using low and high throughput approaches.


ABSTRACT: Despite progress, MS-based proteomics in biofluids, especially blood, faces challenges such as dynamic range and throughput limitations in biomarker and disease studies. In this work, we used cutting-edge proteomics technologies to construct label-based and label-free workflows, capable of quantifying approximately 2,000 proteins in biofluids. With 70µL of blood and a single depletion strategy, we conducted an analysis of a homogenous cohort (n = 32), comparing medium-grade prostate cancer patients (Gleason score: 7(3 + 4); TNM stage: T2cN0M0, stage IIB) to healthy donors. The results revealed dozens of differentially expressed proteins in both plasma and serum. We identified the upregulation of Prostate Specific Antigen (PSA), a well-known biomarker for prostate cancer, in the serum of cancer cohort. Further bioinformatics analysis highlighted noteworthy proteins which appear to be differentially secreted into the bloodstream, making them good candidates for further exploration.

SUBMITTER: Hamza GM 

PROVIDER: S-EPMC10929178 | biostudies-literature | 2024 Mar

REPOSITORIES: biostudies-literature

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Proteomics of prostate cancer serum and plasma using low and high throughput approaches.

Hamza Ghaith M GM   Raghunathan Rekha R   Ashenden Stephanie S   Zhang Bairu B   Miele Eric E   Jarnuczak Andrew F AF  

Clinical proteomics 20240312 1


Despite progress, MS-based proteomics in biofluids, especially blood, faces challenges such as dynamic range and throughput limitations in biomarker and disease studies. In this work, we used cutting-edge proteomics technologies to construct label-based and label-free workflows, capable of quantifying approximately 2,000 proteins in biofluids. With 70µL of blood and a single depletion strategy, we conducted an analysis of a homogenous cohort (n = 32), comparing medium-grade prostate cancer patie  ...[more]

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