Title : Screening and identification of a novel PGAM5-specific inhibitor for attenuating multi-organ injury

Introduction: The necroptosis regulator PGAM5 drives a pathological cycle of mitochondrial dysfunction and necroptotic signaling, contributing to multi-organ injury and representing a potential therapeutic target. Despite its clinical relevance, few PGAM5-specific small-molecule inhibitors have been developed.

Objectives: We aimed to identify a safe and effective natural small-molecule inhibitor targeting PGAM5 as a novel therapeutic strategy.

Methods: Global PGAM5 knockout mice and pancreas-specific PGAM5 knocdown mice were used to clarify the regulatory role of PGAM5 in pancreatic injury in acute pancreatitis (AP). Subsequently, high-throughput screening of candidate compounds targeting PGAM5 was conducted based on the Traditional Chinese Medicine Systems Pharmacology Database and Analysis Platform (TCMSP). Combined with molecular docking, in vitro binding experiments, and functional verification experiments, Plantainoside D (PD) was finally identified as a natural small-molecule inhibitor targeting PGAM5. Finally, the protective effect of PD was evaluated using preclinical models of various organ injuries.

Results: We identify PGAM5 as a critical mediator of pancreatic acinar cell (PAC) necrosis in AP. Genetic suppression of PGAM5 significantly mitigates PACs necrosis in both in vitro and in vivo AP models. Through high-throughput virtual screening of the TCMSP natural-product database, we identified PD, a phenylethanoid glycoside, as the first reported PGAM5-specific small-molecule inhibitor. By binding PGAM5, PD inhibits its phosphatase activity and prevents oligomerization, thereby restoring mitochondrial homeostasis and blocking necroptosis. Importantly, systemic PD administration demonstrated broad protective efficacy in multiple organ-injury models—including autoimmune hepatitis, acute kidney injury, myocardial ischemia—reperfusion, and lung fibrosis—as well as local efficacy in a pathological high intraocular pressure(ph-IOP)—induced retinal ganglion cell (RGC) injury model.

Conclusion: These findings establish PGAM5 as a druggable target in organ injury and identify PD as a natural compound with favorable safety and strong translational potential, providing a foundation for necroptosis-targeted therapeutic development.

Chen Lin is a postdoctoral researcher at Yangzhou University. Her research centers on pancreatic necrosis-associated molecular targets and precision therapeutic strategies for acute pancreatitis. She has published work in the field of acute pancreatitis, with a particular focus on the identification of key necrosis-related targets and the development of novel pharmacological interventions.