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利用结肠上皮细胞代谢重建来理解人类结肠上皮细胞中与疾病相关的代谢变化。

Understanding disease-associated metabolic changes in human colon epithelial cells using ColonEpithelium metabolic reconstruction.

作者信息

Jiang Boyu, Quinn-Bohmann Nick, Diener Christian, Nathan Vignesh Bose, Han-Hallett Yu, Reddivari Lavanya, Gibbons Sean M, Baloni Priyanka

出版信息

bioRxiv. 2024 Oct 25:2024.10.22.619644. doi: 10.1101/2024.10.22.619644.

DOI:10.1101/2024.10.22.619644
PMID:39484551
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11526933/
Abstract

The colon epithelium plays a key role in the host-microbiome interactions, allowing uptake of various nutrients and driving important metabolic processes. To unravel detailed metabolic activities in the human colon epithelium, our present study focuses on the generation of the first cell-type specific genome-scale metabolic model (GEM) of human colonic epithelial cells, named iColonEpithelium. GEMs are powerful tools for exploring reactions and metabolites at systems level and predicting the flux distributions at steady state. Our cell-type-specific iColonEpithelium metabolic reconstruction captures genes specifically expressed in the human colonic epithelial cells. The iColonEpithelium is also capable of performing metabolic tasks specific to the cell type. A unique transport reaction compartment has been included to allow simulation of metabolic interactions with the gut microbiome. We used iColonEpithelium to identify metabolic signatures associated with inflammatory bowel disease. We integrated single-cell RNA sequencing data from Crohn's Diseases (CD) and ulcerative colitis (UC) samples with the iColonEpithelium metabolic network to predict metabolic signatures of colonocytes between CD and UC compared to healthy samples. We identified reactions in nucleotide interconversion, fatty acid synthesis and tryptophan metabolism were differentially regulated in CD and UC conditions, which were in accordance with experimental results. The iColonEpithelium metabolic network can be used to identify mechanisms at the cellular level, and our network has the potential to be integrated with gut microbiome models to explore the metabolic interactions between host and gut microbiota under various conditions.

摘要

结肠上皮在宿主-微生物组相互作用中起关键作用,可摄取各种营养物质并驱动重要的代谢过程。为了阐明人类结肠上皮中的详细代谢活动,我们目前的研究聚焦于生成人类结肠上皮细胞的首个细胞类型特异性基因组规模代谢模型(GEM),命名为iColonEpithelium。GEM是在系统水平探索反应和代谢物以及预测稳态通量分布的强大工具。我们的细胞类型特异性iColonEpithelium代谢重建捕获了在人类结肠上皮细胞中特异性表达的基因。iColonEpithelium还能够执行特定于该细胞类型的代谢任务。已纳入一个独特的转运反应区室,以模拟与肠道微生物组的代谢相互作用。我们使用iColonEpithelium来识别与炎症性肠病相关的代谢特征。我们将来自克罗恩病(CD)和溃疡性结肠炎(UC)样本的单细胞RNA测序数据与iColonEpithelium代谢网络整合,以预测与健康样本相比,CD和UC中结肠细胞的代谢特征。我们确定了在CD和UC条件下核苷酸相互转化、脂肪酸合成和色氨酸代谢中的反应受到差异调节,这与实验结果一致。iColonEpithelium代谢网络可用于在细胞水平识别机制,并且我们的网络有潜力与肠道微生物组模型整合,以探索在各种条件下宿主与肠道微生物群之间的代谢相互作用。

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