Establishment and optimization of peptide biomarker screening model in diabetes in vitro by HPLC/ESI-TOF mass spectrometry

Mei Zhang; Dong Hua Lü; Rong Ji Dai; Yu Lin Deng

Establishment and optimization of peptide biomarker screening model in diabetes in vitro by HPLC/ESI-TOF mass spectrometry

Mei Zhang, Dong Hua Lü, Rong Ji Dai, Yu Lin Deng^*

^*此作品的通讯作者

Beijing Institute of Technology

科研成果: 期刊稿件 › 文章 › 同行评审

2 引用（Scopus）

摘要

Diabetes mellitus is an incurable disease, so it is necessary to establish a model to screen biomarkers for early warning in order to minimize the likelihood of long-term complications. Currently, advanced glycation end products (AGEs) are considered to be biomarkers of many diseases, such as diabetes and its complications. In this study, a model for further proteomics study was established to analyze the glycation of HSA with ¹⁸O-labeling strategy. 30 peptides were randomly selected to optimize tryptic digestion and ¹⁸O-labeling condition by HPLC-ESI/TOF. The best tryptic digestion condition was: HSA:Trypsin=50:1, w/w for 20 h. The best ¹⁸O-labeling condition was to dilute urea to 1 M and adjust KH₂PO₄-K₂HPO₄ buffer pH to 6.0 to give a final labeling efficiency of 98.5±0.7%. The inter- and intra-day precisions and stability were satisfactory. This model was established and optimized for further quantitative proteomics study.

源语言	英语
页（从-至）	563-568
页数	6
期刊	Journal of Beijing Institute of Technology (English Edition)
卷	22
期	4
出版状态	已出版 - 12月 2013

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title = "Establishment and optimization of peptide biomarker screening model in diabetes in vitro by HPLC/ESI-TOF mass spectrometry",

abstract = "Diabetes mellitus is an incurable disease, so it is necessary to establish a model to screen biomarkers for early warning in order to minimize the likelihood of long-term complications. Currently, advanced glycation end products (AGEs) are considered to be biomarkers of many diseases, such as diabetes and its complications. In this study, a model for further proteomics study was established to analyze the glycation of HSA with 18O-labeling strategy. 30 peptides were randomly selected to optimize tryptic digestion and 18O-labeling condition by HPLC-ESI/TOF. The best tryptic digestion condition was: HSA:Trypsin=50:1, w/w for 20 h. The best 18O-labeling condition was to dilute urea to 1 M and adjust KH2PO4-K2HPO4 buffer pH to 6.0 to give a final labeling efficiency of 98.5±0.7%. The inter- and intra-day precisions and stability were satisfactory. This model was established and optimized for further quantitative proteomics study.",

keywords = "Diabetes biomarker, HPLC/ESI-TOF MS, Human serum albumin, O-labeling, Tryptic digestion",

author = "Mei Zhang and L{\"u}, {Dong Hua} and Dai, {Rong Ji} and Deng, {Yu Lin}",

year = "2013",

month = dec,

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TY - JOUR

T1 - Establishment and optimization of peptide biomarker screening model in diabetes in vitro by HPLC/ESI-TOF mass spectrometry

AU - Zhang, Mei

AU - Lü, Dong Hua

AU - Dai, Rong Ji

AU - Deng, Yu Lin

PY - 2013/12

Y1 - 2013/12

N2 - Diabetes mellitus is an incurable disease, so it is necessary to establish a model to screen biomarkers for early warning in order to minimize the likelihood of long-term complications. Currently, advanced glycation end products (AGEs) are considered to be biomarkers of many diseases, such as diabetes and its complications. In this study, a model for further proteomics study was established to analyze the glycation of HSA with 18O-labeling strategy. 30 peptides were randomly selected to optimize tryptic digestion and 18O-labeling condition by HPLC-ESI/TOF. The best tryptic digestion condition was: HSA:Trypsin=50:1, w/w for 20 h. The best 18O-labeling condition was to dilute urea to 1 M and adjust KH2PO4-K2HPO4 buffer pH to 6.0 to give a final labeling efficiency of 98.5±0.7%. The inter- and intra-day precisions and stability were satisfactory. This model was established and optimized for further quantitative proteomics study.

AB - Diabetes mellitus is an incurable disease, so it is necessary to establish a model to screen biomarkers for early warning in order to minimize the likelihood of long-term complications. Currently, advanced glycation end products (AGEs) are considered to be biomarkers of many diseases, such as diabetes and its complications. In this study, a model for further proteomics study was established to analyze the glycation of HSA with 18O-labeling strategy. 30 peptides were randomly selected to optimize tryptic digestion and 18O-labeling condition by HPLC-ESI/TOF. The best tryptic digestion condition was: HSA:Trypsin=50:1, w/w for 20 h. The best 18O-labeling condition was to dilute urea to 1 M and adjust KH2PO4-K2HPO4 buffer pH to 6.0 to give a final labeling efficiency of 98.5±0.7%. The inter- and intra-day precisions and stability were satisfactory. This model was established and optimized for further quantitative proteomics study.

KW - Diabetes biomarker

KW - HPLC/ESI-TOF MS

KW - Human serum albumin

KW - O-labeling

KW - Tryptic digestion

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M3 - Article

AN - SCOPUS:84892461023

SN - 1004-0579

VL - 22

SP - 563

EP - 568

JO - Journal of Beijing Institute of Technology (English Edition)

JF - Journal of Beijing Institute of Technology (English Edition)

IS - 4

ER -

Establishment and optimization of peptide biomarker screening model in diabetes in vitro by HPLC/ESI-TOF mass spectrometry

摘要

联合国可持续发展目标

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引用此