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This review aims to elucidate the mechanisms by which GPBAR1 impacts critical processes in hepatitis B-associated liver failure.

March 26, 2026Open Access

Research Progress on the Mechanism and Targeted Intervention of G Protein-Coupled Bile Acid Receptor 1 (GPBAR1)-Mediated “Inflammation-Apoptosis-Metabolism-Microcirculation” Regulatory Network in Hepatitis B-Associated Liver Failure

Puntos clave

This review aims to elucidate the mechanisms by which GPBAR1 impacts critical processes in hepatitis B-associated liver failure.
Systematic review of molecular pathways involved in GPBAR1 signaling.
Analysis of GPBAR1's effects on inflammation, hepatocyte apoptosis, and bile acid metabolism.
Comparison of GPBAR1-targeted therapies to existing GPCR approaches.
GPBAR1 regulates inflammation and apoptosis through NF-κB and PI3K/Akt pathways.
It maintains bile acid balance via CYP7A1 and CYP8A1.
Abnormal GPBAR1 expression correlates with severity and prognosis of HBV-LF.

Resumen

Abstract: Hepatitis B-associated liver failure (HBV-LF) is a severe hepatic disease induced by hepatitis B virus infection, characterized by massive hepatocyte necrosis, rapid liver dysfunction, uncontrolled inflammation, bile acid metabolism disorders and immune microenvironment imbalance. It has a high short-term mortality of 40%– 70% worldwide. Current mainstream treatments, including antiviral and organ support therapies, only control viral replication and maintain organ function, but cannot effectively reverse the excessive inflammatory cascade and metabolic disorders that drive HBV-LF progression. This review systematically summarizes the molecular mechanisms by which GPBAR1 regulates the four core pathological processes of HBV-LF: uncontrolled inflammation, massive hepatocyte apoptosis, bile acid metabolism disorders and hepatic microcirculation disturbance, and clarifies its value as a potential therapeutic target. G protein-coupled bile acid receptor 1 (GPBAR1/TGR5) is a key membrane receptor for bile acids and critically regulates hepatic physiology and pathology. Given the limited direct evidence in HBV-LF, we cautiously extrapolate relevant mechanisms from chronic hepatitis B, acute liver injury and metabolic liver diseases based on shared pathological features, while noting that these mechanisms require further validation in HBV-LF models and clinical samples. We review the structure, distribution, activation and signaling pathways of GPBAR1, focusing on its protective role in HBV-LF: inhibiting excessive inflammation via NF-κB and Keap1-Nrf2 pathways, reducing hepatocyte apoptosis through mitochondrial and PI3K/Akt pathways, maintaining bile acid balance by regulating CYP7A1/CYP8A1, and improving hepatic immunity and microcirculation via NKT, CCL2/CCR2 and ET-1 axes. Abnormal GPBAR1 expression correlates with HBV-LF severity and poor prognosis. We also summarize preclinical progress of GPBAR1 agonists (e.g. INT-767, BAR501) and compare GPBAR1-targeted strategies with other GPCR therapies. This review provides a theoretical basis for mechanistic research and target identification of HBV-LF. Keywords: hepatitis b-associated liver failure, g protein-coupled bile acid receptor 1, uncontrolled inflammation, bile acid metabolism disorder, immune microenvironment imbalance

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