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Gut Microbiota Metabolite 3-Indolepropionic Acid Directly Activates Hepatic Stellate Cells by ROS/JNK/p38 Signaling Pathways

Xiaoyan Yuan, Junting Yang, Yuling Huang, Jia Li, Yuanyuan Li

2023Biomolecules16 citationsDOIOpen Access PDF

Abstract

There has been a growing interest in studying the communication of gut microbial metabolites between the gut and the liver as liver fibrosis progresses. Although 3-Indolepropionic acid (IPA) is regarded as a clinically valuable gut metabolite for the treatment of certain chronic diseases, the effects of oral administration of IPA on hepatic fibrosis in different animal models have been conflicting. While some mechanisms have been proposed to explain these contradictory effects, the direct impact of IPA on hepatic fibrosis remains unclear. In this study, we found that IPA could directly activate LX-2 human hepatic stellate cells in vitro. IPA upregulated the expression of fibrogenic marker genes and promoted the features associated with HSCs activation, including proliferation and contractility. IPA also increased reactive oxygen species (ROS) in mitochondria and the expression of inflammation-related genes in LX-2 cells. However, when a ROS-blocking agent was used, these effects were reduced. p38 and JNK, the downstream signaling cascades of ROS, were found to be required for the activation of LX-2 induced by IPA. These findings suggest that IPA can directly activate hepatic stellate cells through ROS-induced JNK and p38 signaling pathways.

Topics & Concepts

Hepatic stellate cellReactive oxygen speciesDownregulation and upregulationHepatic fibrosisCell biologySignal transductionMetaboliteInflammationp38 mitogen-activated protein kinasesBiologyFibrosisGut floraChemistryCancer researchEndocrinologyMAPK/ERK pathwayBiochemistryInternal medicineImmunologyMedicineGeneLiver Disease Diagnosis and TreatmentLiver physiology and pathologyLiver Diseases and Immunity