Liu Tao, Qian Wei-Jun, Chen Wan-Nan U, Jacobs Jon M, Moore Ronald J, Anderson David J, Gritsenko Marina A, Monroe Matthew E, Thrall Brian D, Camp David G, Smith Richard D
Biological Sciences Division and Environmental Molecular Sciences Laboratory, Pacific Northwest National Laboratory, Richland, WA 99352, USA.
Proteomics. 2005 Apr;5(5):1263-73. doi: 10.1002/pmic.200401055.
Automated multidimensional capillary liquid chromatography-tandem mass spectrometry (LC-MS/MS) has been increasingly applied in various large scale proteome profiling efforts. However, comprehensive global proteome analysis remains technically challenging due to issues associated with sample complexity and dynamic range of protein abundances, which is particularly apparent in mammalian biological systems. We report here the application of a high efficiency cysteinyl peptide enrichment (CPE) approach to the global proteome analysis of human mammary epithelial cells (HMECs) which significantly improved both sequence coverage of protein identifications and the overall proteome coverage. The cysteinyl peptides were specifically enriched by using a thiol-specific covalent resin, fractionated by strong cation exchange chromatography, and subsequently analyzed by reversed-phase capillary LC-MS/MS. An HMEC tryptic digest without CPE was also fractionated and analyzed under the same conditions for comparison. The combined analyses of HMEC tryptic digests with and without CPE resulted in a total of 14 416 confidently identified peptides covering 4294 different proteins with an estimated 10% gene coverage of the human genome. By using the high efficiency CPE, an additional 1096 relatively low abundance proteins were identified, resulting in 34.3% increase in proteome coverage; 1390 proteins were observed with increased sequence coverage. Comparative protein distribution analyses revealed that the CPE method is not biased with regard to protein M(r) , pI, cellular location, or biological functions. These results demonstrate that the use of the CPE approach provides improved efficiency in comprehensive proteome-wide analyses of highly complex mammalian biological systems.
自动化多维毛细管液相色谱 - 串联质谱法(LC-MS/MS)已越来越多地应用于各种大规模蛋白质组分析工作中。然而,由于与样品复杂性和蛋白质丰度动态范围相关的问题,全面的全球蛋白质组分析在技术上仍然具有挑战性,这在哺乳动物生物系统中尤为明显。我们在此报告一种高效半胱氨酰肽富集(CPE)方法在人乳腺上皮细胞(HMECs)全球蛋白质组分析中的应用,该方法显著提高了蛋白质鉴定的序列覆盖率和整体蛋白质组覆盖率。通过使用硫醇特异性共价树脂特异性富集半胱氨酰肽,经强阳离子交换色谱分离,随后通过反相毛细管LC-MS/MS进行分析。还对未经CPE处理的HMEC胰蛋白酶消化物在相同条件下进行分离和分析以作比较。对经CPE处理和未经CPE处理的HMEC胰蛋白酶消化物进行联合分析,共鉴定出14416个可信度高的肽段,覆盖4294种不同蛋白质,估计人类基因组覆盖率为10%。通过使用高效CPE,又鉴定出1096种相对低丰度蛋白质,蛋白质组覆盖率提高了34.3%;观察到1390种蛋白质的序列覆盖率有所增加。比较蛋白质分布分析表明,CPE方法在蛋白质分子量、pI、细胞定位或生物学功能方面没有偏差。这些结果表明,使用CPE方法在高度复杂的哺乳动物生物系统的全面蛋白质组分析中提高了效率。