Blood peptidome-degradome profile of breast cancer.

Cancer invasion and metastasis are closely associated with activities within the degradome; however, little is known about whether these activities can be detected in the blood of cancer patients.The peptidome-degradome profiles of pooled blood plasma sampled from 15 breast cancer patients (BCP) and...

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Main Authors: Yufeng Shen, Nikola Tolić, Tao Liu, Rui Zhao, Brianne O Petritis, Marina A Gritsenko, David G Camp, Ronald J Moore, Samuel O Purvine, Francisco J Esteva, Richard D Smith
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2010-10-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2956627?pdf=render
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spelling doaj-a35c75e8bc704d8e98faab98b84dc01b2020-11-25T01:35:16ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-10-01510e1313310.1371/journal.pone.0013133Blood peptidome-degradome profile of breast cancer.Yufeng ShenNikola TolićTao LiuRui ZhaoBrianne O PetritisMarina A GritsenkoDavid G CampRonald J MooreSamuel O PurvineFrancisco J EstevaRichard D SmithCancer invasion and metastasis are closely associated with activities within the degradome; however, little is known about whether these activities can be detected in the blood of cancer patients.The peptidome-degradome profiles of pooled blood plasma sampled from 15 breast cancer patients (BCP) and age, race, and menopausal status matched control healthy persons (HP) were globally characterized using advanced comprehensive separations combined with tandem Fourier transform mass spectrometry and new data analysis approaches that facilitated top-down peptidomic analysis. The BCP pool displayed 71 degradome protein substrates that encompassed 839 distinct peptidome peptides. In contrast, the HP 50 degradome substrates found encompassed 425 peptides. We find that the ratios of the peptidome peptide relative abundances can vary as much as >4000 fold between BCP and HP. The experimental results also show differential degradation of substrates in the BCP sample in their functional domains, including the proteolytic and inhibitory sites of the plasmin-antiplasmin and thrombin-antithrombin systems, the main chains of the extracellular matrix protection proteins, the excessive degradation of innate immune system key convertases and membrane attack complex components, as well as several other cancer suppressor proteins.Degradomics-peptidomics profiling of blood plasma is highly sensitive to changes not evidenced by conventional bottom-up proteomics and potentially provides unique signatures of possible diagnostic utility.http://europepmc.org/articles/PMC2956627?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Yufeng Shen
Nikola Tolić
Tao Liu
Rui Zhao
Brianne O Petritis
Marina A Gritsenko
David G Camp
Ronald J Moore
Samuel O Purvine
Francisco J Esteva
Richard D Smith
spellingShingle Yufeng Shen
Nikola Tolić
Tao Liu
Rui Zhao
Brianne O Petritis
Marina A Gritsenko
David G Camp
Ronald J Moore
Samuel O Purvine
Francisco J Esteva
Richard D Smith
Blood peptidome-degradome profile of breast cancer.
PLoS ONE
author_facet Yufeng Shen
Nikola Tolić
Tao Liu
Rui Zhao
Brianne O Petritis
Marina A Gritsenko
David G Camp
Ronald J Moore
Samuel O Purvine
Francisco J Esteva
Richard D Smith
author_sort Yufeng Shen
title Blood peptidome-degradome profile of breast cancer.
title_short Blood peptidome-degradome profile of breast cancer.
title_full Blood peptidome-degradome profile of breast cancer.
title_fullStr Blood peptidome-degradome profile of breast cancer.
title_full_unstemmed Blood peptidome-degradome profile of breast cancer.
title_sort blood peptidome-degradome profile of breast cancer.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2010-10-01
description Cancer invasion and metastasis are closely associated with activities within the degradome; however, little is known about whether these activities can be detected in the blood of cancer patients.The peptidome-degradome profiles of pooled blood plasma sampled from 15 breast cancer patients (BCP) and age, race, and menopausal status matched control healthy persons (HP) were globally characterized using advanced comprehensive separations combined with tandem Fourier transform mass spectrometry and new data analysis approaches that facilitated top-down peptidomic analysis. The BCP pool displayed 71 degradome protein substrates that encompassed 839 distinct peptidome peptides. In contrast, the HP 50 degradome substrates found encompassed 425 peptides. We find that the ratios of the peptidome peptide relative abundances can vary as much as >4000 fold between BCP and HP. The experimental results also show differential degradation of substrates in the BCP sample in their functional domains, including the proteolytic and inhibitory sites of the plasmin-antiplasmin and thrombin-antithrombin systems, the main chains of the extracellular matrix protection proteins, the excessive degradation of innate immune system key convertases and membrane attack complex components, as well as several other cancer suppressor proteins.Degradomics-peptidomics profiling of blood plasma is highly sensitive to changes not evidenced by conventional bottom-up proteomics and potentially provides unique signatures of possible diagnostic utility.
url http://europepmc.org/articles/PMC2956627?pdf=render
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