Dietary limonene promotes gastrointestinal barrier function via upregulating tight/adherens junction proteins through cannabinoid receptor type-1 antagonistic mechanism and alters cellular metabolism in intestinal epithelial cells.

IF 5 3区生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY BioFactors Pub Date : 2024-08-14 DOI:10.1002/biof.2106

K J Senthil Kumar, M Gokila Vani, Gyaltsen Dakpa, Sheng-Yang Wang

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Abstract

Limonene, a dietary monocyclic monoterpene commonly found in citrus fruits and various aromatic plants, has garnered increasing interest as a gastrointestinal protectant. This study aimed to assess the effects of limonene on intestinal epithelial barrier function and investigate the involvement of cannabinoid receptor type-1 (CB1R) in vitro. Additionally, the study focused on examining the metabolomic changes induced by limonene in the intestinal epithelial cells (Caco-2). Initial analysis of transepithelial electrical resistance (TEER) revealed that both l-limonene and d-limonene, isomers of limonene, led to a dose- and time-dependent increase in TEER in normal cells and those inflamed by pro-inflammatory cytokines mixture (CytoMix). Furthermore, both types of limonene reduced CytoMix-induced paracellular permeability, as demonstrated by a decrease in Lucifer yellow flux. Moreover, d-limonene and l-limonene treatment increased the expression of tight junction molecules (TJs) such as occludin, claudin-1, and ZO-1, at both the transcriptional and translational levels. d-Limonene upregulates E-cadherin, a molecule involved in adherens junctions (AJs). Mechanistic investigations demonstrated that d-limonene and l-limonene treatment significantly inhibited CB1R at the protein, while the mRNA level remained unchanged. Notably, the inhibitory effect of d-limonene on CB1R was remarkably similar to that of pharmacological CB1R antagonists, such as rimonabant and ORG27569. d-limonene also alters Caco-2 cell metabolites. A substantial reduction in β-glucose and 2-succinamate was detected, suggesting limonene may impact intestinal epithelial cells' glucose uptake and glutamate metabolism. These findings suggest that d-limonene's CB1R antagonistic property could effectively aid in the recovery of intestinal barrier damage, marking it a promising gastrointestinal protectant.

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膳食中的柠檬烯通过大麻素受体 1 型拮抗机制上调紧密/粘连连接蛋白，促进胃肠道屏障功能，并改变肠上皮细胞的细胞代谢。

柠檬烯是一种常见于柑橘类水果和各种芳香植物中的膳食单环单萜，作为一种胃肠道保护剂已引起越来越多的关注。本研究旨在评估柠檬烯对肠道上皮屏障功能的影响，并调查大麻素受体 1 型（CB1R）在体外的参与情况。此外，该研究还重点考察了柠檬烯在肠上皮细胞（Caco-2）中诱导的代谢组变化。对经上皮细胞电阻（TEER）的初步分析表明，l-柠檬烯和 d-柠檬烯（柠檬烯的异构体）都会导致正常细胞和被促炎细胞因子混合物（CytoMix）感染的细胞中 TEER 的增加，而增加的程度与剂量和时间有关。此外，这两种柠檬烯都能降低 CytoMix 诱导的细胞旁通透性，这体现在荧光黄通量的降低上。此外，d-柠檬烯和 l-柠檬烯处理可在转录和翻译水平上增加紧密连接分子（TJs）的表达，如 occludin、claudin-1 和 ZO-1。机理研究表明，d-柠檬烯和 l-柠檬烯处理可在蛋白水平显著抑制 CB1R，而 mRNA 水平则保持不变。值得注意的是，d-柠檬烯对 CB1R 的抑制作用与药物 CB1R 拮抗剂（如利莫那班和 ORG27569）的抑制作用非常相似。检测发现，β-葡萄糖和 2-琥珀酸盐的含量大幅减少，这表明柠檬烯可能会影响肠上皮细胞的葡萄糖摄取和谷氨酸代谢。这些研究结果表明，d-柠檬烯的 CB1R 拮抗特性可有效帮助肠道屏障损伤的恢复，是一种很有前景的胃肠道保护剂。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

BioFactors 生物-内分泌学与代谢

CiteScore

11.50

自引率

3.30%

发文量

审稿时长

6-12 weeks

期刊介绍： BioFactors, a journal of the International Union of Biochemistry and Molecular Biology, is devoted to the rapid publication of highly significant original research articles and reviews in experimental biology in health and disease. The word “biofactors” refers to the many compounds that regulate biological functions. Biological factors comprise many molecules produced or modified by living organisms, and present in many essential systems like the blood, the nervous or immunological systems. A non-exhaustive list of biological factors includes neurotransmitters, cytokines, chemokines, hormones, coagulation factors, transcription factors, signaling molecules, receptor ligands and many more. In the group of biofactors we can accommodate several classical molecules not synthetized in the body such as vitamins, micronutrients or essential trace elements. In keeping with this unified view of biochemistry, BioFactors publishes research dealing with the identification of new substances and the elucidation of their functions at the biophysical, biochemical, cellular and human level as well as studies revealing novel functions of already known biofactors. The journal encourages the submission of studies that use biochemistry, biophysics, cell and molecular biology and/or cell signaling approaches.