Literature DB >> 26819888

Establishment of a Strategy for the Discovery and Verification of Low-Abundance Biomarker Peptides in Plasma Using Two Types of Stable-Isotope Tags.

Yoshio Kodera1, Yuya Hido2, Rika Kato2, Tatsuya Saito2, Yusuke Kawashima1, Satoru Minamida3, Kazumasa Matsumoto4, Masatsugu Iwamura3.   

Abstract

Serum and plasma contain thousands of different proteins and peptides, which can provide valuable information about the numerous processes that take place within the body. However, detailed analysis of proteins and peptides in serum and plasma remains challenging due to the presence of many high-abundance proteins, the large dynamic range of protein and peptide concentrations, the extensive complexity caused by posttranslational modifications, and considerable individual variability. In particular, detailed analysis and identification of native peptides is extremely difficult due to the tremendous variety of cleavage possibilities and posttranslational modifications, which results in extremely high complexity. Therefore, widely ranging searches based on peptide identification are difficult. Herein, we describe the highly accurate and sensitive quantitative analysis of over 2,500 peptides with the concentration limit of about 10 pM. The strategy combined isobaric tag labeling, amine-reactive 6-plex tandem mass tag labeling, and a modified differential solubilization method for high-yield peptide extraction [Saito, T. et al. J. Electrophoresis 2013 57: 1-9]. Using this strategy, we quantitatively analyzed six pooled plasma samples (three pre-surgery and three post-surgery) to discover potential candidate biomarker peptides of renal cell carcinoma. The concentrations of 27 peptides were found to be altered following surgery. A preliminary validation study was conducted using about 80 plasma samples to demonstrate the possibility that even unidentified potential candidate biomarker peptides can be verified using the isotope tag/dimethyl labeling method. We also discuss technical consideration and potential of this strategy for facilitating native peptide research.

Entities:  

Keywords:  biomarker peptide; isobaric tag; isotope tag; plasma; renal cell carcinoma

Year:  2015        PMID: 26819888      PMCID: PMC4337364          DOI: 10.5702/massspectrometry.S0044

Source DB:  PubMed          Journal:  Mass Spectrom (Tokyo)        ISSN: 2186-5116


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Journal:  Proteomics       Date:  2004-04       Impact factor: 3.984

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Journal:  Proteomics       Date:  2007-02       Impact factor: 3.984

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Journal:  Proteomics Clin Appl       Date:  2009-07       Impact factor: 3.494

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8.  [Plasma bradykinin concentration in patients with cardiovascular diseases].

Authors:  M Minami; H Togashi; M Sano; T Endoh; H Saito; F Hashimoto; K Fujita; H Yasuda; Y Kuriyamoto; T Nishino
Journal:  Nihon Yakurigaku Zasshi       Date:  1983-08

9.  Plasma peptidome profiling of acute hepatitis E patients by MALDI-TOF/TOF.

Authors:  Shikha Taneja; Imran Ahmad; Somdutta Sen; Saravanan Kumar; Reena Arora; Vijay K Gupta; Rakesh Aggarwal; Krishnamoorthy Narayanasamy; Vanga S Reddy; Shahid Jameel
Journal:  Proteome Sci       Date:  2011-02-04       Impact factor: 2.480

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  2 in total

1.  Identification of the salusin-β receptor using proteoliposomes embedded with endogenous membrane proteins.

Authors:  Masayoshi Shichiri; Daisuke Nonaka; Lyang-Ja Lee; Kenji Tanaka
Journal:  Sci Rep       Date:  2018-12-14       Impact factor: 4.379

Review 2.  Proteomic approaches for characterizing renal cell carcinoma.

Authors:  David J Clark; Hui Zhang
Journal:  Clin Proteomics       Date:  2020-07-29       Impact factor: 3.988

  2 in total

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