Surface analysis of peptide mass spectra to improve time and mass localization

Author

Carrillo, B. ; Kearney, R.E. ; Yanofsky, C. ; Lekpor, K. ; Bell, A. ; Boismenu, D.

Author_Institution

Dept. of Biomedical Eng., McGill Univ., Que., Canada

Volume

1

fYear

2004

fDate

1-5 Sept. 2004

Firstpage

220

Lastpage

223

Abstract

Current peak detections algorithms for processing mass spectrometry (MS) spectra generally rely on two dimensional techniques for identifying the location and intensity of peaks from a single spectrum. However, when high performance liquid chromatography (HPLC) is coupled with mass spectrometry, a third dimension, retention time, is introduced. The ensemble of MS spectra may then be regarded as a 3D surface where spectral intensity is a function of m/z (mass-to-charge) and time. This suggests that peak localization can be improved by incorporating the time domain data and average data across both dimensions. This work describes a surface intensity analysis algorithm and the results of its use.

Keywords

biological techniques; chromatography; mass spectra; mass spectroscopic chemical analysis; molecular biophysics; proteins; high performance liquid chromatography; mass localization; mass spectrometry; peak detection algorithm; peptide mass spectra; retention time; surface analysis; time localization; Biological information theory; Cells (biology); Genomics; Humans; Isolation technology; Mass spectroscopy; Peptides; Proteins; Proteomics; Signal to noise ratio; HPLC; Proteomics; mass spectrometry; peptides;

fLanguage

English

Publisher

ieee

Conference_Titel

Engineering in Medicine and Biology Society, 2004. IEMBS '04. 26th Annual International Conference of the IEEE

Conference_Location

San Francisco, CA

Print_ISBN

0-7803-8439-3

Type

conf

DOI

10.1109/IEMBS.2004.1403131

Filename

1403131