脂质组学与靶向、单细胞和空间转录组学的整合揭示了结肠癌中一种尚未解决的促炎状态。

Integration of lipidomics with targeted, single cell, and spatial transcriptomics defines an unresolved pro-inflammatory state in colon cancer.

作者信息

Soundararajan Ramani, Maurin Michelle M, Rodriguez-Silva Jetsen, Upadhyay Gunjan, Alden Ashley J, Gowda Siddabasave Gowda B, Schell Michael J, Yang Mingli, Levine Noah Jhad, Gowda Divyavani, Sundaraswamy Punith M, Hui Shu-Ping, Pflieger Lance, Wang Heiman, Marcet Jorge, Martinez Carolina, Bennett Robert David, Chudzinski Allen, Karachristos Andreas, Nywening Timothy M, Cavallaro Paul M, Anderson Matthew Linley, Coffey Robert J, Nebozhyn Michael V, Loboda Andrey, Coppola Domenico, Pledger Warren Jackson, Halade Ganesh V, Yeatman Timothy J

机构信息

Department of Surgery, University of South Florida Health, Tampa, Florida, USA.

Department of Internal Medicine, University of South Florida Health, Tampa, Florida, USA.

出版信息

Gut. 2025 Mar 6;74(4):586-602. doi: 10.1136/gutjnl-2024-332535.

DOI:10.1136/gutjnl-2024-332535

PMID:39658263

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11885055/

Abstract

BACKGROUND

Over a century ago, Virchow proposed that cancer represents a chronically inflamed, poorly healing wound. Normal wound healing is represented by a transitory phase of inflammation, followed by a pro-resolution phase, with prostaglandin (PGE2/PGD2)-induced 'lipid class switching' producing inflammation-quenching lipoxins (LXA4, LXB4).

OBJECTIVE

We explored if lipid dysregulation in colorectal cancers (CRCs) is driven by a failure to resolve inflammation.

DESIGN

We performed liquid chromatography and tandem mass spectrometry (LC-MS/MS) untargeted analysis of 40 human CRC and normal paired samples and targeted, quantitative analysis of 81 human CRC and normal paired samples. We integrated analysis of lipidomics, quantitative reverse transcription-PCR, large scale gene expression, and spatial transcriptomics with public scRNASEQ data to characterize pattern, expression and cellular localisation of genes that produce and modify lipid mediators.

RESULTS

Targeted, quantitative LC-MS/MS demonstrated a marked imbalance of pro-inflammatory mediators, with a dearth of resolving lipid mediators. In tumours, we observed prominent over-expression of arachidonic acid derivatives, the genes encoding their synthetic enzymes and receptors, but poor expression of genes producing pro-resolving synthetic enzymes and resultant lipoxins (LXA4, LXB4) and associated receptors. These results indicate that CRC is the product of defective lipid class switching likely related to inadequate or ineffective levels of PGE2/PGD2.

CONCLUSION

We show that the lipidomic profile of CRC tumours exhibits a distinct pro-inflammatory bias with a deficiency of endogenous resolving mediators secondary to defective lipid class switching. These observations pave the way for 'resolution medicine', a novel therapeutic approach for inducing or providing resolvins to mitigate the chronic inflammation driving cancer growth and progression.

摘要

背景

一个多世纪前，魏尔啸提出癌症代表一种慢性炎症、愈合不良的伤口。正常伤口愈合以炎症的短暂阶段为特征，随后是促消退阶段，前列腺素（PGE2/PGD2）诱导的“脂质类别转换”产生消退炎症的脂氧素（LXA4、LXB4）。

目的

我们探讨了结直肠癌（CRC）中的脂质失调是否由炎症消退失败所致。

设计

我们对40对人CRC和正常配对样本进行了液相色谱和串联质谱（LC-MS/MS）非靶向分析，并对81对人CRC和正常配对样本进行了靶向定量分析。我们将脂质组学、定量逆转录PCR、大规模基因表达和空间转录组学分析与公开的scRNASEQ数据相结合，以表征产生和修饰脂质介质的基因的模式、表达和细胞定位。

结果

靶向定量LC-MS/MS显示促炎介质明显失衡，消退脂质介质缺乏。在肿瘤中，我们观察到花生四烯酸衍生物、编码其合成酶和受体的基因显著过度表达，但产生促消退合成酶以及由此产生的脂氧素（LXA4、LXB4）和相关受体的基因表达不佳。这些结果表明，CRC是脂质类别转换缺陷的产物，可能与PGE2/PGD2水平不足或无效有关。