基于拟靶向液相色谱-质谱联用的胃癌患者血清代谢组分析

doi:10.3724/SP.J.1123.2013.11050

色谱 ›› 2014, Vol. 32 ›› Issue (2): 126-132.DOI: 10.3724/SP.J.1123.2013.11050

基于拟靶向液相色谱-质谱联用的胃癌患者血清代谢组分析

杨太忠^1,2, 罗萍², 李艳丽², 华瑞¹, 尹沛源², 许国旺²

1. 吉林大学第一医院, 吉林长春 130021;
2. 中国科学院大连化学物理研究所, 辽宁大连 116023

收稿日期:2013-11-27 修回日期:2013-12-20 出版日期:2014-02-08 发布日期:2014-01-25
通讯作者: 华瑞，尹沛源
基金资助:
国家科技重大专项(2012ZX10002011)；国家自然科学基金项目(81200289).

A serum metabolomics study of gastric cancer based on pseudotargeted liquid chromatography-mass spectrometry approach

YANG Taizhong^1,2, LUO Ping², LI Yanli², HUA Rui¹, YIN Peiyuan², XU Guowang²

1. The First Hospital of Jilin University, Changchun 130021, China;
2. Dalian Institute of Chemical Physics, Chinese Academy of Sciences, Dalian 116023, China

Received:2013-11-27 Revised:2013-12-20 Online:2014-02-08 Published:2014-01-25

摘要/Abstract

摘要：

胃癌是一种高发的恶性肿瘤，是癌症相关死亡的第二大病因。早期筛查是提高患者生存率的有效手段，但目前临床上尚缺乏实现胃癌无创筛检的可靠标志物。本研究采用了基于液相色谱-质谱联用的拟靶向代谢组学方法分析了20例胃癌患者及40例正常人血清代谢组，以期发现新的潜在代谢标志物。代谢组数据的主成分分析和偏最小二乘法数据分析结果显示，胃癌患者与健康人群的血清代谢组存在明显的差异，结合非参数检验进一步筛选并定性出57个差异代谢物。其中二氢胆固醇经验证组样本验证，具有成为胃癌代谢标志物的潜力。本研究在发现胃癌的潜在代谢标志物的同时，也为胃癌患者代谢分型提供了重要的科学依据。

关键词: 代谢组学, 拟靶向, 胃癌, 液相色谱-质谱, 肿瘤标志物

Abstract:

Gastric cancer is one of the most common malignant and the second most frequent cause of cancer-related mortality in the world. Noninvasive screen methods including tumor markers are intensively needed in the clinic. To discover metabolic markers for gastric cancers, the sera metabolic profiles of 20 gastric cancer (GC) patients and 40 healthy controls were analyzed by liquid chromatography coupled with mass spectrometry (LC-MS) using a pseudotargeted approach. The results of principal component analysis (PCA) and partial least squares-discriminant analysis (PLS-DA) indicated that obvious classification could be observed between GC and the healthy controls. According to the results of non-parametric statistical test, 57 ions were identified among all the differential metabolic features. Of all the identified differential metabolites, dihydrocholesterol provide good diagnostic performance of GC, which was also validated by another cohort including the 20 gastric cancer patients and the 39 healthy controls. With this robust pseudotargeted approach, our study provides both potential tumor markers and the basis for the metabolic phenotype of gastric cancers.

Key words: gastric cancer, liquid chromatography-mass spectrometry (LC-MS), metabolomics, pseudotargeted, tumor biomarker

中图分类号:

O658

杨太忠, 罗萍, 李艳丽, 华瑞, 尹沛源, 许国旺. 基于拟靶向液相色谱-质谱联用的胃癌患者血清代谢组分析[J]. 色谱, 2014, 32(2): 126-132.

YANG Taizhong, LUO Ping, LI Yanli, HUA Rui, YIN Peiyuan, XU Guowang. A serum metabolomics study of gastric cancer based on pseudotargeted liquid chromatography-mass spectrometry approach[J]. Chinese Journal of Chromatography, 2014, 32(2): 126-132.

参考文献

[1] Parkin D M, Bray F, Ferlay J, et al. CA Cancer J Clin, 2005, 55(2): 74
[2] Genta R M. Aliment Pharmacol Ther, 2004, 20(2): 42
[3] Marrelli D, Roviello F, De Stefano A, et al. Oncology, 1999, 57(1): 55
[4] Karl-Heinz O, Nelly A, Singh B, et al. Phytochemistry, 2003, 62(6): 971
[5] Nicholson J K, Connelly J, Lindon J C, et al. Nat Rev Drug Discov, 2002, 1(2): 153
[6] Holmes E, Wilson I D, Nicholson J K. Cell, 2008, 135(5): 714
[7] Zhu Y Z, Feng Y N, Jin Z H. Chinese Journal of Chromatography (朱永哲, 冯雅男, 金正汉, 等. 色谱), 2013, 31(9): 850
[8] Dai W D, Zhang F X, Jia Z H, et al. Chinese Journal of Chromatography (戴伟东, 张凤霞, 贾振华, 等. 色谱), 2011, 29(11): 1049
[9] Yin P, Xu G. Expert Rev Mol Diagn, 2013, 13(4): 339
[10] Rainer L, Zhao X, Cora W, et al. Plos One, 2010, 5(7): e11519
[11] Anderson L, Hunter C L. Mol Cell Proteomics, 2006, 5(4): 573
[12] Li Y, Ruan Q, Li Y L, et al. J Chromatogr A, 2012, 1255: 228
[13] Chen S L, Kong H W, Lu X, et al. Anal Chem, 2013, 85(17): 8326
[14] Zhao Y, Zhao C, Lu X, et al. J Proteome Res, 2013, 12(11): 5072
[15] Zhou L N, Ding L L, Yin P Y, et al. J Proteome Res, 2012, 11(11): 5433
[16] Yin P Y, Wan D F, Zhao C X, et al. Mol Biosyst, 2009, 5(8): 868
[17] Zhao X, Fritsche J, Wang J, et al. Metabolomics, 2010, 6(3): 362
[18] Chen J, Zhao X, Fritsche J, et al. Anal Chem, 2008, 80(4): 1280
[19] Zhao S M, Wang Y S, Dou A B, et al. Chinese Journal of Chromatography (赵素敏, 王宜生, 窦阿波, 等. 色谱), 2011, 29(9): 843
[20] Dong J, Cai X M, Zhao L L, et al. Metabolomics, 2010, 6(4): 478
[21] Zhao Z, Xiao Y, Elson P, et al. J Clin Oncol, 2007, 25(19): 2696
[22] Mills G B, Moolenaar W H. Nat Rev Cancer, 2003, 3(8): 582
[23] Zhou L, Wang Q, Yin P, et al. Anal Bioanal Chem, 2012, 403(1): 203

基于拟靶向液相色谱-质谱联用的胃癌患者血清代谢组分析

A serum metabolomics study of gastric cancer based on pseudotargeted liquid chromatography-mass spectrometry approach

PDF

可视化

被引次数

摘要/Abstract

引用本文

使用本文

扫码分享

参考文献

相关文章 15

编辑推荐

Metrics

[1]	王亚婷, 杨阳, 孙秀兰, 纪剑. 基于气相色谱-质谱法的广泛靶向代谢组学方法开发[J]. 色谱, 2023, 41(6): 520-526.
[2]	曲涛, 陈阳, 杨长军, 刘其耸, 陈惠, 何志勇, 王召君, 陈洁, 曾茂茂. 松花粉干预卵巢早衰大鼠肝脏的广泛靶向代谢组学分析[J]. 色谱, 2023, 41(1): 47-57.
[3]	谷艳, 臧鹏, 李进霞, 闫燕艳, 王佳. 基于超高效液相色谱-静电场轨道阱高分辨质谱的深静脉血栓模型大鼠血浆代谢组学分析[J]. 色谱, 2022, 40(8): 736-745.
[4]	张莹, 杨静, 马跃新, 曹玲, 黄青. 基于超高效液相色谱-质谱法的肽段分析中非特异性吸附评估及通用型最小化策略[J]. 色谱, 2022, 40(7): 616-624.
[5]	马占君, 李振国, 王欢, 王仁军, 韩晓菲. 基于液相色谱-串联质谱的结肠癌血清氧固醇标志物筛选[J]. 色谱, 2022, 40(6): 541-546.
[6]	郭民康, 张健. 基于超高效液相色谱-串联质谱的股骨头坏死组织外泌体脂质代谢组学分析[J]. 色谱, 2022, 40(2): 123-129.
[7]	何祉安, 林厚维, 桂娟, 朱伟超, 何建华, 汪航, 冯蕾. 基于超高效液相色谱-高分辨质谱和渗透压校正样本浓度变异性的尿液代谢组学分析[J]. 色谱, 2021, 39(4): 391-398.
[8]	欧阳瑒, 迟磊, 徐超, 赵欣捷, 崔振泽. 基于液相色谱-质谱代谢组学方法研究中药定喘汤对呼吸道合胞病毒感染的疗效[J]. 色谱, 2021, 39(3): 281-290.
[9]	沈葹, 杨奕, 王晶波, 陈曦, 刘婷婷, 卓勤. 基于超高效液相色谱-四极杆飞行时间质谱的非靶向代谢组学用于不同来源单花蜜的差异分析[J]. 色谱, 2021, 39(3): 291-300.
[10]	杨凯歌, 王薇薇, 王彦, 阎超. 血清和血清外泌体的蛋白质组分析及其在肝内胆管癌中的应用[J]. 色谱, 2021, 39(11): 1191-1202.
[11]	牟红梅, 慈志娟, 艾沙江·买买提, 梁艳萍, 刘笑宏, 杜晓云, 于强, 李庆余, 李元军. 基于非靶向代谢组学的茄梨和红茄梨成熟期果皮代谢产物的差异分析[J]. 色谱, 2021, 39(11): 1203-1212.
[12]	王稳, 陈迪, 朴海龙. 基于超高效液相色谱-飞行时间质谱法测定LAMTOR1在肝脏炎症恶性转化中调控的代谢物[J]. 色谱, 2021, 39(10): 1118-1127.
[13]	王芳, 王松, 丛海林, 于冰. 基于毛细管电泳-质谱联用技术的代谢/蛋白质组学分析[J]. 色谱, 2020, 38(9): 1013-1021.
[14]	徐坤, 金钰龙, 黄嫣嫣, 赵睿. 超高效液相色谱-质谱联用法监测人心房钠尿肽的化学合成[J]. 色谱, 2020, 38(3): 324-331.
[15]	金一宝, 李上富, 王珏, 高丹, 刘红霞, 蒋宇扬, 殷果, 王铁杰. 基于液相色谱-质谱联用的代谢组学技术研究Pokemon诱导的胞内脂代谢变化[J]. 色谱, 2020, 38(2): 162-168.