The application of multiple reaction monitoring to assess ApoA-I methionine oxidations in diabetes and cardiovascular disease

Hussein N. Yassine; Angela M. Jackson; Peter D. Reaven; Dobrin Nedelkov; Randall W. Nelson; Serrine S. Lau; Christoph H. Borchers

doi:10.1016/j.trprot.2014.10.001

The application of multiple reaction monitoring to assess ApoA-I methionine oxidations in diabetes and cardiovascular disease

Hussein N. Yassine, Angela M. Jackson, Peter D. Reaven, Dobrin Nedelkov, Randall W. Nelson, Serrine S. Lau, Christoph H. Borchers

Research output: Contribution to journal › Article › peer-review

23 Scopus citations

Abstract

The oxidative modification of apolipoprotein A-I's methionine148 (M148) is associated with defective HDL function in vitro. Multiple reaction monitoring (MRM) is a mass spectrometric technique that can be used to quantitate post-translational modifications. In this study, we developed an MRM assay to monitor the abundance ratio of the peptide containing oxidized M148 to the native peptide in ApoA-I. Measurement of the oxidized-to-unoxidized-M148 ratio was reproducible (CV < 5%). The extent of methionine M148 oxidation in the HDL of healthy controls, and type 2 diabetic participants with and without prior cardiovascular events (CVD) were then examined. The results suggest a significant increase in the relative ratio of the peptide containing oxidized M148 to the unmodified peptide in the HDL of participants with diabetes and CVD (p < 0.001), compared to participants without CVD. Monitoring the abundance ratio of the peptides containing oxidized and unoxidized M148 by MRM provides a means of examining the relationship between M148 oxidation and vascular complications in CVD.

Original language	English (US)
Pages (from-to)	18-24
Number of pages	7
Journal	Translational Proteomics
Volume	4-5
DOIs	https://doi.org/10.1016/j.trprot.2014.10.001
State	Published - 2014

Keywords

Cardiovascular disease
Diabetes
HDL
Multiple reaction monitoring
Proteomics

ASJC Scopus subject areas

Biochemistry

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10.1016/j.trprot.2014.10.001

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title = "The application of multiple reaction monitoring to assess ApoA-I methionine oxidations in diabetes and cardiovascular disease",

abstract = "The oxidative modification of apolipoprotein A-I's methionine148 (M148) is associated with defective HDL function in vitro. Multiple reaction monitoring (MRM) is a mass spectrometric technique that can be used to quantitate post-translational modifications. In this study, we developed an MRM assay to monitor the abundance ratio of the peptide containing oxidized M148 to the native peptide in ApoA-I. Measurement of the oxidized-to-unoxidized-M148 ratio was reproducible (CV < 5%). The extent of methionine M148 oxidation in the HDL of healthy controls, and type 2 diabetic participants with and without prior cardiovascular events (CVD) were then examined. The results suggest a significant increase in the relative ratio of the peptide containing oxidized M148 to the unmodified peptide in the HDL of participants with diabetes and CVD (p < 0.001), compared to participants without CVD. Monitoring the abundance ratio of the peptides containing oxidized and unoxidized M148 by MRM provides a means of examining the relationship between M148 oxidation and vascular complications in CVD.",

keywords = "Cardiovascular disease, Diabetes, HDL, Multiple reaction monitoring, Proteomics",

author = "Yassine, {Hussein N.} and Jackson, {Angela M.} and Reaven, {Peter D.} and Dobrin Nedelkov and Nelson, {Randall W.} and Lau, {Serrine S.} and Borchers, {Christoph H.}",

note = "Funding Information: Dr. Yassine was supported by K23HL107389, AHA12CRP11750017. Drs. Nelson, Reaven, Lau and Yassine were supported by R24DK090958. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. MRM method development was done by the Arizona Proteomics Consortium, which is supported by NIEHS grant P30ES06694 to the Southwest Environmental Health Sciences Center (SWEHSC to Dr. Lau), NIH/NCI grant P30CA023074 to the Arizona Cancer Center (AZCC), and by the BIO5 Institute of the University of Arizona. CHB and AMJ would also like to thank Genome Canada and Genome British Columbia for their support of the University of Victoria – Genome BC Proteomics Centre through Science and Technology Innovation Centre funding. Publisher Copyright: {\textcopyright} 2014 The Authors",

year = "2014",

doi = "10.1016/j.trprot.2014.10.001",

language = "English (US)",

volume = "4-5",

pages = "18--24",

journal = "Translational Proteomics",

issn = "2212-9626",

publisher = "Elsevier BV",

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TY - JOUR

T1 - The application of multiple reaction monitoring to assess ApoA-I methionine oxidations in diabetes and cardiovascular disease

AU - Yassine, Hussein N.

AU - Jackson, Angela M.

AU - Reaven, Peter D.

AU - Nedelkov, Dobrin

AU - Nelson, Randall W.

AU - Lau, Serrine S.

AU - Borchers, Christoph H.

N1 - Funding Information: Dr. Yassine was supported by K23HL107389, AHA12CRP11750017. Drs. Nelson, Reaven, Lau and Yassine were supported by R24DK090958. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. MRM method development was done by the Arizona Proteomics Consortium, which is supported by NIEHS grant P30ES06694 to the Southwest Environmental Health Sciences Center (SWEHSC to Dr. Lau), NIH/NCI grant P30CA023074 to the Arizona Cancer Center (AZCC), and by the BIO5 Institute of the University of Arizona. CHB and AMJ would also like to thank Genome Canada and Genome British Columbia for their support of the University of Victoria – Genome BC Proteomics Centre through Science and Technology Innovation Centre funding. Publisher Copyright: © 2014 The Authors

PY - 2014

Y1 - 2014

N2 - The oxidative modification of apolipoprotein A-I's methionine148 (M148) is associated with defective HDL function in vitro. Multiple reaction monitoring (MRM) is a mass spectrometric technique that can be used to quantitate post-translational modifications. In this study, we developed an MRM assay to monitor the abundance ratio of the peptide containing oxidized M148 to the native peptide in ApoA-I. Measurement of the oxidized-to-unoxidized-M148 ratio was reproducible (CV < 5%). The extent of methionine M148 oxidation in the HDL of healthy controls, and type 2 diabetic participants with and without prior cardiovascular events (CVD) were then examined. The results suggest a significant increase in the relative ratio of the peptide containing oxidized M148 to the unmodified peptide in the HDL of participants with diabetes and CVD (p < 0.001), compared to participants without CVD. Monitoring the abundance ratio of the peptides containing oxidized and unoxidized M148 by MRM provides a means of examining the relationship between M148 oxidation and vascular complications in CVD.

AB - The oxidative modification of apolipoprotein A-I's methionine148 (M148) is associated with defective HDL function in vitro. Multiple reaction monitoring (MRM) is a mass spectrometric technique that can be used to quantitate post-translational modifications. In this study, we developed an MRM assay to monitor the abundance ratio of the peptide containing oxidized M148 to the native peptide in ApoA-I. Measurement of the oxidized-to-unoxidized-M148 ratio was reproducible (CV < 5%). The extent of methionine M148 oxidation in the HDL of healthy controls, and type 2 diabetic participants with and without prior cardiovascular events (CVD) were then examined. The results suggest a significant increase in the relative ratio of the peptide containing oxidized M148 to the unmodified peptide in the HDL of participants with diabetes and CVD (p < 0.001), compared to participants without CVD. Monitoring the abundance ratio of the peptides containing oxidized and unoxidized M148 by MRM provides a means of examining the relationship between M148 oxidation and vascular complications in CVD.

KW - Cardiovascular disease

KW - Diabetes

KW - HDL

KW - Multiple reaction monitoring

KW - Proteomics

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DO - 10.1016/j.trprot.2014.10.001

M3 - Article

AN - SCOPUS:84982061491

SN - 2212-9626

VL - 4-5

SP - 18

EP - 24

JO - Translational Proteomics

JF - Translational Proteomics

ER -

The application of multiple reaction monitoring to assess ApoA-I methionine oxidations in diabetes and cardiovascular disease

Abstract

Keywords

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