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Sample complexity reduction for two-dimensional electrophoresis using solution isoelectric focusing prefractionation

โœ Scribed by Matthew R. Richardson; Sean Liu; Heather N. Ringham; Victor Chan; Frank A. Witzmann


Publisher
John Wiley and Sons
Year
2008
Tongue
English
Weight
398 KB
Volume
29
Category
Article
ISSN
0173-0835

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โœฆ Synopsis


Abstract

Despite its excellent resolving power, 2โ€DE is of limited use when analyzing cellular proteomes, especially in differential expression studies. Frequently, fewer than 2000 protein spots are detected on a single 2โ€D gel (a fraction of the total proteome) regardless of the gel platform, sample, or detection method used. This is due to the vast number of proteins expressed and their equally vast dynamic range. To exploit 2โ€DE unique ability as both an analytical and a preparative tool, the significant sample prefractionation is necessary. We have used solution isoelectric focusing (sIEF) via the ZOOMยฎ IEF Fractionator (Invitrogen) to generate sample fractions from complex bacterial lysates, followed by parallel 2โ€DE, using narrowโ€range IPG strips that bracket the sIEF fractions. The net result of this process is a significant enrichment of the bacterial proteome resolved on multiple 2โ€D gels. After prefractionation, we detected 5525 spots, an approximate 3.5โ€fold increase over the 1577 spots detected in an unfractionated gel. We concluded that sIEF is an effective means of prefractionation to increase depth of field and improve the analysis of lowโ€abundance proteins.


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