Oral VA-SNEDDS delivers morin to hepatic stellate cells, significantly attenuating liver fibrosis in rats.
Background
Chronic hepatic fibrosis is a progressive liver disease marked by excessive extracellular matrix (ECM) accumulation, primarily driven by activated hepatic stellate cells (aHSCs). Current treatments often fall short, and long-term management requires non-invasive strategies. Oral medication is ideal for prolonged therapy, yet achieving targeted drug delivery to aHSCs via oral routes remains a significant challenge due to the vulnerability of nanoparticles to degradation during intestinal transit. This study addresses this critical gap by developing a robust oral delivery system.
Study Design
Researchers fabricated an oral vitamin A (VA)-functionalized self-nanoemulsifying drug delivery system, termed VA-SNEDDS, designed for precise delivery of morin (MOR) to aHSCs. The system's integrity and translocation were assessed after oral administration. Its therapeutic efficacy was then evaluated in a carbon tetrachloride (CCl4)-induced fibrotic rat model. Primary endpoints included measuring ECM deposition, hydroxyproline content, and transforming growth factor-β1 (TGF-β1) expression, alongside assessing overall liver function. The study aimed to demonstrate successful intestinal translocation, systemic circulation via the lymphatic pathway, and targeted accumulation in aHSCs.
Results
The designed VA-SNEDDS successfully translocated across the intestinal epithelium, maintaining its structural integrity, and entered systemic circulation via the lymphatic pathway. Crucially, it ultimately accumulated in aHSCs within fibrotic livers through VA- and retinol-binding protein receptor-mediated binding. This targeted delivery mechanism proved effective in vivo. In the CCl4-induced fibrotic rat model, treatment with MOR-loaded VA-SNEDDS significantly attenuated liver fibrosis. This attenuation was evidenced by a reduction in ECM deposition, hydroxyproline content, and transforming growth factor-β1 (TGF-β1) expression. Concurrently, the treatment restored liver function, indicating a broad therapeutic benefit. While specific quantitative data (e.g., percentages, p-values) were not detailed in the abstract, the findings consistently pointed to a robust anti-fibrotic effect.
The oral MOR-loaded VA-SNEDDS significantly attenuated liver fibrosis by reducing
ECMdeposition, hydroxyproline content, andTGF-β1expression, while restoring liver function.
Key Findings
- Oral VA-SNEDDS maintained structural integrity during intestinal transit and entered systemic circulation via the lymphatic pathway.
- VA-SNEDDS accumulated specifically in aHSCs within fibrotic livers via
VA- andretinol-binding protein receptor-mediated binding. - MOR-loaded VA-SNEDDS significantly attenuated liver fibrosis in
CCl4-induced rats. - Treatment reduced
ECMdeposition, hydroxyproline content, andTGF-β1expression. - MOR-loaded VA-SNEDDS concurrently restored liver function in fibrotic rats.
Why It Matters
This study presents a groundbreaking advance for liver fibrosis treatment by demonstrating a viable oral, targeted drug delivery platform. The ability of VA-SNEDDS to maintain structural integrity through the gut and specifically target aHSCs via VA- and retinol-binding protein receptor-mediated binding overcomes a major hurdle in oral nanomedicine. This orally administrable, aHSCs-targeted platform could revolutionize long-term therapy for liver fibrosis, offering a non-invasive alternative to current limited options. It opens the door for developing new oral anti-fibrotic agents, potentially improving patient compliance and reducing treatment burden. Further research is needed to translate this preclinical success into human clinical protocols, including dose optimization and safety profiling.
liver-fibrosis
hepatic-stellate-cells
oral-delivery
nanoemulsion
morin
drug-delivery