Williams Michael D, Zhang Xing, Park Jeong-Jin, Siems William F, Gang David R, Resar Linda M S, Reeves Raymond, Hill Herbert H
Department of Chemistry, Washington State University, Pullman, WA, 99164, USA.
Anal Bioanal Chem. 2015 Jun;407(16):4581-95. doi: 10.1007/s00216-015-8662-x. Epub 2015 May 6.
Colorectal cancer (CRC) remains a leading cause of cancer death worldwide, despite the fact that it is a curable disease when diagnosed early. The development of new screening methods to aid in early diagnosis or identify precursor lesions at risk for progressing to CRC will be vital to improving the survival rate of individuals predisposed to CRC. Metabolomics is an advancing area that has recently seen numerous applications to the field of cancer research. Altered metabolism has been studied for many years as a means to understand and characterize cancer. However, further work is required to establish standard procedures and improve our ability to identify distinct metabolomic profiles that can be used to diagnose CRC or predict disease progression. The present study demonstrates the use of direct infusion traveling wave ion mobility mass spectrometry to distinguish metabolic profiles from CRC samples and matched non-neoplastic epithelium as well as metastatic and primary tumors at different stages of disease (T1-T4). By directly infusing our samples, the analysis time was reduced significantly, thus increasing the speed and efficiency of this method compared to traditional metabolomics platforms. Partial least squares discriminant analysis was used to visualize differences between the metabolic profiles of sample types and to identify the specific m/z features that led to this differentiation. Identification of the distinct m/z features was made using the human metabolome database. We discovered alterations in fatty acid biosynthesis and oxidative, glycolytic, and polyamine pathways that distinguish tumors from non-malignant colonic epithelium as well as various stages of CRC. Although further studies are needed, our results indicate that colonic epithelial cells undergo metabolic reprogramming during their evolution to CRC, and the distinct metabolites could serve as diagnostic tools or potential targets in therapy or primary prevention. Graphical Abstract Colon tissue biopsy samples were collected from patients after which metabolites were extracted via sonication. Two-dimensional data were collected via IMS in tandem with MS (IMMS). Data were then interpreted statistically via PLS-DA. Scores plots provided a visualization of statistical separation and groupings of sample types. Loading plots allowed identification of influential ion features. Lists of these features were exported and analyzed for specific differences. Direct comparisons of the ion features led to the identification and comparative analyses of candidate biomarkers. These differences were then expressed visually in charts and tables.
尽管结直肠癌(CRC)在早期诊断时是可治愈的疾病,但它仍是全球癌症死亡的主要原因。开发新的筛查方法以辅助早期诊断或识别有进展为CRC风险的前驱病变,对于提高易患CRC个体的生存率至关重要。代谢组学是一个不断发展的领域,最近在癌症研究领域有许多应用。多年来,人们一直在研究代谢改变,以此作为理解和表征癌症的一种手段。然而,还需要进一步的工作来建立标准程序,并提高我们识别可用于诊断CRC或预测疾病进展的独特代谢组学谱的能力。本研究展示了使用直接进样行波离子淌度质谱法来区分CRC样本、匹配的非肿瘤上皮以及疾病不同阶段(T1 - T4)的转移瘤和原发肿瘤的代谢谱。通过直接进样我们的样本,分析时间显著缩短,因此与传统代谢组学平台相比,提高了该方法的速度和效率。使用偏最小二乘判别分析来可视化样本类型代谢谱之间的差异,并识别导致这种差异的特定质荷比(m/z)特征。使用人类代谢组数据库对不同的m/z特征进行鉴定。我们发现脂肪酸生物合成、氧化、糖酵解和多胺途径的改变,这些改变区分了肿瘤与非恶性结肠上皮以及CRC的不同阶段。尽管还需要进一步研究,但我们的结果表明结肠上皮细胞在向CRC演变过程中经历了代谢重编程,并且这些独特的代谢物可作为诊断工具或治疗或一级预防中的潜在靶点。
从患者身上收集结肠组织活检样本,然后通过超声处理提取代谢物。通过离子淌度质谱联用(IMMS)收集二维数据。然后通过偏最小二乘判别分析(PLS - DA)对数据进行统计学解释。得分图提供了样本类型统计分离和分组的可视化。载荷图允许识别有影响的离子特征。导出这些特征列表并分析其特定差异。对离子特征的直接比较导致候选生物标志物的鉴定和比较分析。然后在图表中直观地表达这些差异。
