PMI R&D, Philip Morris Products S.A., Quai Jeanrenaud 5, CH-2000 Neuchatel, Switzerland.
Lipidomics Consulting Ltd., Irisviksvägen 31D, 02230 Esbo, Finland.
Int J Mol Sci. 2018 Sep 15;19(9):2775. doi: 10.3390/ijms19092775.
Inflammatory bowel disease (IBD) represents a group of progressive disorders characterized by recurrent chronic inflammation of the gut. Ulcerative colitis and Crohn's disease are the major manifestations of IBD. While our understanding of IBD has progressed in recent years, its etiology is far from being fully understood, resulting in suboptimal treatment options. Complementing other biological endpoints, bioanalytical "omics" methods that quantify many biomolecules simultaneously have great potential in the dissection of the complex pathogenesis of IBD. In this review, we focus on the rapidly evolving proteomics and lipidomics technologies and their broad applicability to IBD studies; these range from investigations of immune-regulatory mechanisms and biomarker discovery to studies dissecting host⁻microbiome interactions and the role of intestinal epithelial cells. Future studies can leverage recent advances, including improved analytical methodologies, additional relevant sample types, and integrative multi-omics analyses. Proteomics and lipidomics could effectively accelerate the development of novel targeted treatments and the discovery of complementary biomarkers, enabling continuous monitoring of the treatment response of individual patients; this may allow further refinement of treatment and, ultimately, facilitate a personalized medicine approach to IBD.
炎症性肠病(IBD)代表一组以肠道反复发生慢性炎症为特征的进行性疾病。溃疡性结肠炎和克罗恩病是 IBD 的主要表现形式。尽管近年来我们对 IBD 的认识有所进展,但它的病因远未完全了解,导致治疗选择不佳。除了其他生物学终点外,同时定量许多生物分子的生物分析“组学”方法在剖析 IBD 的复杂发病机制方面具有很大的潜力。在这篇综述中,我们重点介绍了快速发展的蛋白质组学和脂质组学技术及其在 IBD 研究中的广泛适用性;这些研究范围从免疫调节机制的研究和生物标志物的发现到宿主-微生物组相互作用和肠上皮细胞作用的研究。未来的研究可以利用包括改进的分析方法、更多相关的样本类型和综合多组学分析在内的最新进展。蛋白质组学和脂质组学可以有效地加速新型靶向治疗方法的开发和互补生物标志物的发现,从而能够持续监测个体患者的治疗反应;这可能会进一步细化治疗方法,并最终促进 IBD 的个性化医疗方法。
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