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The Need for Review and Understanding of SELDI/MALDI Mass Spectroscopy Data Prior to Analysis

Multiple studies have reported that surface enhanced laser desorption/ionization time of flight mass spectroscopy (SELDI-TOF-MS) is useful in the early detection of disease based on the analysis of bodily fluids. Use of any multiplex mass spectroscopy based approach as in the analysis of bodily flui...

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Autores principales: Grizzle, William E., Semmes, O. John, Bigbee, William, Zhu, Liu, Malik, Gunjan, Oelschlager, Denise K, Manne, Barkha, Manne, Upender
Formato: Texto
Lenguaje:English
Publicado: Libertas Academica 2007
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2657646/
https://www.ncbi.nlm.nih.gov/pubmed/19305634
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author Grizzle, William E.
Semmes, O. John
Bigbee, William
Zhu, Liu
Malik, Gunjan
Oelschlager, Denise K
Manne, Barkha
Manne, Upender
author_facet Grizzle, William E.
Semmes, O. John
Bigbee, William
Zhu, Liu
Malik, Gunjan
Oelschlager, Denise K
Manne, Barkha
Manne, Upender
author_sort Grizzle, William E.
collection PubMed
description Multiple studies have reported that surface enhanced laser desorption/ionization time of flight mass spectroscopy (SELDI-TOF-MS) is useful in the early detection of disease based on the analysis of bodily fluids. Use of any multiplex mass spectroscopy based approach as in the analysis of bodily fluids to detect disease must be analyzed with great care due to the susceptibility of multiplex and mass spectroscopy methods to biases introduced via experimental design, patient samples, and/or methodology. Specific biases include those related to experimental design, patients, samples, protein chips, chip reader and spectral analysis. Contributions to biases based on patients include demographics (e.g., age, race, ethnicity, sex), homeostasis (e.g., fasting, medications, stress, time of sampling), and site of analysis (hospital, clinic, other). Biases in samples include conditions of sampling (type of sample container, time of processing, time to storage), conditions of storage, (time and temperature of storage), and prior sample manipulation (freeze thaw cycles). Also, there are many potential biases in methodology which can be avoided by careful experimental design including ensuring that cases and controls are analyzed randomly. All the above forms of biases affect any system based on analyzing multiple analytes and especially all mass spectroscopy based methods, not just SELDI-TOF-MS. Also, all current mass spectroscopy systems have relatively low sensitivity compared with immunoassays (e.g., ELISA). There are several problems which may be unique to the SELDI-TOF-MS system marketed by Ciphergen(®). Of these, the most important is a relatively low resolution (±0.2%) of the bundled mass spectrometer which may cause problems with analysis of data. Foremost, this low resolution results in difficulties in determining what constitutes a “peak” if a peak matching approach is used in analysis. Also, once peaks are selected, the peaks may represent multiple proteins. In addition, because peaks may vary slightly in location due to instrumental drift, long term identification of the same peaks may prove to be a challenge. Finally, the Ciphergen(®) system has some “noise” of the baseline which results from the accumulation of charge in the detector system. Thus, we must be very aware of the factors that may affect the use of proteomics in the early detection of disease, in determining aggressive subsets of cancers, in risk assessment and in monitoring the effectiveness of novel therapies.
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spelling pubmed-26576462009-03-20 The Need for Review and Understanding of SELDI/MALDI Mass Spectroscopy Data Prior to Analysis Grizzle, William E. Semmes, O. John Bigbee, William Zhu, Liu Malik, Gunjan Oelschlager, Denise K Manne, Barkha Manne, Upender Cancer Inform Review Multiple studies have reported that surface enhanced laser desorption/ionization time of flight mass spectroscopy (SELDI-TOF-MS) is useful in the early detection of disease based on the analysis of bodily fluids. Use of any multiplex mass spectroscopy based approach as in the analysis of bodily fluids to detect disease must be analyzed with great care due to the susceptibility of multiplex and mass spectroscopy methods to biases introduced via experimental design, patient samples, and/or methodology. Specific biases include those related to experimental design, patients, samples, protein chips, chip reader and spectral analysis. Contributions to biases based on patients include demographics (e.g., age, race, ethnicity, sex), homeostasis (e.g., fasting, medications, stress, time of sampling), and site of analysis (hospital, clinic, other). Biases in samples include conditions of sampling (type of sample container, time of processing, time to storage), conditions of storage, (time and temperature of storage), and prior sample manipulation (freeze thaw cycles). Also, there are many potential biases in methodology which can be avoided by careful experimental design including ensuring that cases and controls are analyzed randomly. All the above forms of biases affect any system based on analyzing multiple analytes and especially all mass spectroscopy based methods, not just SELDI-TOF-MS. Also, all current mass spectroscopy systems have relatively low sensitivity compared with immunoassays (e.g., ELISA). There are several problems which may be unique to the SELDI-TOF-MS system marketed by Ciphergen(®). Of these, the most important is a relatively low resolution (±0.2%) of the bundled mass spectrometer which may cause problems with analysis of data. Foremost, this low resolution results in difficulties in determining what constitutes a “peak” if a peak matching approach is used in analysis. Also, once peaks are selected, the peaks may represent multiple proteins. In addition, because peaks may vary slightly in location due to instrumental drift, long term identification of the same peaks may prove to be a challenge. Finally, the Ciphergen(®) system has some “noise” of the baseline which results from the accumulation of charge in the detector system. Thus, we must be very aware of the factors that may affect the use of proteomics in the early detection of disease, in determining aggressive subsets of cancers, in risk assessment and in monitoring the effectiveness of novel therapies. Libertas Academica 2007-02-19 /pmc/articles/PMC2657646/ /pubmed/19305634 Text en © 2005 The authors. http://creativecommons.org/licenses/by/3.0 This article is an open-access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/3.0/).
spellingShingle Review
Grizzle, William E.
Semmes, O. John
Bigbee, William
Zhu, Liu
Malik, Gunjan
Oelschlager, Denise K
Manne, Barkha
Manne, Upender
The Need for Review and Understanding of SELDI/MALDI Mass Spectroscopy Data Prior to Analysis
title The Need for Review and Understanding of SELDI/MALDI Mass Spectroscopy Data Prior to Analysis
title_full The Need for Review and Understanding of SELDI/MALDI Mass Spectroscopy Data Prior to Analysis
title_fullStr The Need for Review and Understanding of SELDI/MALDI Mass Spectroscopy Data Prior to Analysis
title_full_unstemmed The Need for Review and Understanding of SELDI/MALDI Mass Spectroscopy Data Prior to Analysis
title_short The Need for Review and Understanding of SELDI/MALDI Mass Spectroscopy Data Prior to Analysis
title_sort need for review and understanding of seldi/maldi mass spectroscopy data prior to analysis
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2657646/
https://www.ncbi.nlm.nih.gov/pubmed/19305634
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