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Multi-region proteome analysis quantifies spatial heterogeneity of prostate tissue biomarkers

Authors :
Guo, Tiannan
Li, Li
Zhong, Qing
Rupp, Niels J.
Charmpi, Konstantina
Wong, Christine E.
Wagner, Ulrich
Rueschoff, Jan H.
Jochum, Wolfram
Fankhauser, Christian Daniel
Saba, Karim
Poyet, Cedric
Wild, Peter J.
Aebersold, Ruedi
Beyer, Andreas
Guo, Tiannan
Li, Li
Zhong, Qing
Rupp, Niels J.
Charmpi, Konstantina
Wong, Christine E.
Wagner, Ulrich
Rueschoff, Jan H.
Jochum, Wolfram
Fankhauser, Christian Daniel
Saba, Karim
Poyet, Cedric
Wild, Peter J.
Aebersold, Ruedi
Beyer, Andreas
Publication Year :
2018

Abstract

It remains unclear to what extent tumor heterogeneity impacts on protein biomarker discovery. Here, we quantified proteome intra-tissue heterogeneity (ITH) based on a multi-region analysis of prostate tissues using pressure cycling technology and Sequential Windowed Acquisition of all THeoretical fragment ion mass spectrometry. We quantified 6,873 proteins and analyzed the ITH of 3,700 proteins. The level of ITH varied depending on proteins and tissue types. Benign tissues exhibited more complex ITH patterns than malignant tissues. Spatial variability of 10 prostate biomarkers was validated by immunohistochemistry in an independent cohort (n = 83) using tissue microarrays. Prostate-specific antigen was preferentially variable in benign prostatic hyperplasia, whereas growth/differentiation factor 15 substantially varied in prostate adenocarcinomas. Furthermore, we found that DNA repair pathways exhibited a high degree of variability in tumorous tissues, which may contribute to the genetic heterogeneity of tumors. This study conceptually adds a new perspective to protein biomarker discovery: it suggests that recent technological progress should be exploited to quantify and account for spatial proteome variation to complement biomarker identification and utilization.

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1201319500
Document Type :
Electronic Resource