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Hope for Liver Disease Patients: New Study Reveals Drug’s Ability to Reverse Damage

Pharm'Up 2 min read

A groundbreaking study has provided crucial insights into how a drug can reverse the damage caused by alcohol-related liver disease by actively reshaping the tissue’s architecture. This discovery could pave the way for the first approved therapies for this condition, offering a new lifeline to thousands of patients.

The Challenge: Understanding Fibrosis and a New Solution

In the UK, liver disease is a major cause of mortality, with over 11,000 deaths annually. A key characteristic of the disease is fibrosis, where repeated damage replaces healthy liver tissue with stiff, non-functional scar tissue. This process impairs the liver’s ability to function and, if left unchecked, can lead to permanent damage. While a group of drugs called cyclophilin inhibitors had shown promise in early trials for some types of liver disease, it was unclear how they worked and if they were effective against alcohol-related liver disease, which currently has no approved therapies.

Innovative 3D Models Provide the Answer
To close this knowledge gap, a team of researchers from the Roger Williams Institute of Liver Studies at King’s College London, led by Dr. Elena Palma, Dr. Luca Urbani, and Professor Shilpa Chokshi, developed two sophisticated 3D models using actual human liver tissue. The tissue was sourced from patients at King’s College Hospital undergoing surgery, ensuring the models were clinically relevant and more likely to be translatable to human patients.

  • Model 1: Human Liver Slices: The researchers first took thin, healthy slices of human liver tissue and exposed them to alcohol to mimic the damage seen in patients. They then treated these slices with a cyclophilin inhibitor. Analysis showed that the drug effectively reduced fibrosis by stopping the buildup of the structural proteins responsible for making the tissue stiff.
  • Model 2: Isolated Stellate Cells: The second model focused on a specific type of liver cell, stellate cells, which are the primary drivers of fibrosis. By isolating these cells and ‘activating’ them in the lab to replicate the fibrotic process, the team was able to confirm that the drug works by changing the three-dimensional organization and the type of proteins produced by these cells. This action ultimately restructures the damaged tissue, allowing it to return to a healthier state.

The findings from both models confirmed that cyclophilin inhibitors reduce fibrosis by reshaping the architecture of the damaged tissue. As the study’s principal investigator, Dr. Elena Palma, noted, “There are currently no approved therapies for the treatment of alcohol-induced liver disease,” making this discovery particularly significant. This research offers a new and promising therapeutic approach, underscoring the value of collaboration between researchers and clinicians to create meaningful, patient-focused solutions.

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