Albumin Modifications as Early Biomarkers of Chronic Liver Diseases

NCT ID: NCT06318949

Last Updated: 2025-02-12

Basic Information

• Recruitment Status: RECRUITING
• Clinical Phase: NA
• Total Enrollment: 756 participants
• Study Classification: INTERVENTIONAL
• Study Start Date: 2024-12-09
• Study Completion Date: 2029-12-01

Brief Summary

Chronic liver diseases, affecting over 800 million people worldwide, lead to approximately 2 million annual deaths. The need for early, sensitive diagnostic strategies to prevent disease progression and reduce mortality is still unmet. The traditional serum markers lack sensitivity and specificity, leading to the integration of these biomarkers into panel tests with algorithms or imaging measures. Despite their widespread use, these tests have limitations at an individual level, including an inability to predict disease progression or response to treatment. To address these shortcomings, our project proposes utilizing albumin post-translational modifications (PTM) as a predictive biomarker for liver disease progression. The hypothesis is that albumin modifications occur in the early stages of hepatocellular damage and are indicative of future liver diseases. These modifications can be detected through serum albumin isoform determination, albumin isoforms profiles or the albumin's ligand-binding capacities. Innovatively, the study will use the Serum Enhanced Binding (SEB) test, which identifies reduced ligand-binding capacities, and discusses a second patent for determining a typical isoform profile based on the hepatic injury type.

Our preliminary results from animal models and a proof-of-concept studies with patients support this hypotheses. Our previous studies demonstrated also significant differences in albumin isoform profiles in response to different types of hepatic injury and high sensitivity and specificity in the SEB test among cirrhotic patients.

The primary objective of the MALAHBAR project is to evaluate the capacity of albumin PTM to predict liver disease progression over three years in chronic liver disease patients. Secondary objectives include assessing the predictive ability of different albumin isoforms and the SEB test for liver disease progression, evaluating diagnostic performances and confirming characteristic albumin isoform profiles related to specific hepatic injuries. The study could represent a significant advancement in liver disease diagnostics and management, offering new insights into the role of albumin in liver pathology.

Detailed Description

More than 800 million people suffer from chronic liver disease (CLD) with approximately 2 million deaths per year. The progression of CLD, could be asymptomatic until the appearance of fibrosis, cirrhosis and sometimes hepatocellular carcinoma. The prevention and early diagnosis of liver disease is therefore a major public health issue.

Due to their lack of sensitivity and specificity, direct serum markers are now combined in " panel tests ", sometimes gathered and used in algorithms (FibroMeter, FibroTest, FIBROSpect, Hepascore…) to help diagnose fibrosis or cirrhosis and to assess the stage of liver damage. Other biomarkers, in particular molecules involved in the fibrosis process, (protein-based biomarkers, microRNA or collagen-based biomarkers) have been the subject of numerous studies, but have not yet led to clinically exploitable biomarkers for the medium- or long-term monitoring of CLD. Non-invasive, sensitive and specific biomarkers for the early detection of liver dysfunction leading to advanced liver disease are therefore still awaited.

It has been shown that chemical and structural modifications of human serum albumin (HAS) leading to different isoforms could be used as biomarkers for advanced liver disease. Our work supports the hypothesis that the main changes in HSA occur in the early stages of cellular liver damage and could be predictive of future liver disease. These modifications can be revealed by the profile of isoforms in the patient's serum, or even more efficiently by the binding capacities of HAS for different ligands with specific binding sites. On this basis, a patent application has been filed for the SEB (Serum enhanced binding) test.

The study plans to recruit 756 patients in 6 university hospital centers (CHU of Limoges, Angers, Poitiers, Tours, Rennes, and Pointe à Pitre). The recruitment period is of 1.5 year.

Each patient will be followed during 3 years maximumThe study requires no supplementary visit as compared to the standard care. Study visits will take place during usual visits of the standard care as follows:.

• Inclusion visit : study information by the investigator and if the patient is not opposed to participate to the study, either blood sampling (a supplementary tube can be add to a routine blood sampling realised for standard cares) or re-use of a residual blood sample after routine tests have been done, and data collection from the medical file.
• Follow-up visits: visits at 1, 2 and 3 years depending to the diagnostic of the investigator. During these visits: collection of a blood sampling the same conditions described for the inclusion visit and data collection from the medical file.

The samples will be sent to the central laboratory in the CHU of Limoges (Pharmacology, Toxicology and Pharmacovigilance) where HSA isoforms will be analysed by LC-QTOF and SEB tests realised.

The main goal is to validate HAS modifications as biomarker able to predict the evolution of liver damage and thus prevent worsening of the liver disease and finally improve the quality of care.

Conditions

Chronic Liver Disease

Study Design

• Allocation Method: NA
• Intervention Model: SINGLE_GROUP
• Primary Study Purpose: DIAGNOSTIC
• Blinding Strategy: NONE

Study Groups

experimental arm

Group Type: EXPERIMENTAL

blood sampling

Intervention Type: PROCEDURE

If the patient does not object to participating in the study, a blood sample is taken at each visit (an additional tube may be added to a routine blood sample taken for standard care), or a residual blood sample is reused after routine tests have been performed, and data is collected from the medical record.

Interventions

blood sampling

If the patient does not object to participating in the study, a blood sample is taken at each visit (an additional tube may be added to a routine blood sample taken for standard care), or a residual blood sample is reused after routine tests have been performed, and data is collected from the medical record.

Intervention Type: PROCEDURE

Eligibility Criteria

Inclusion Criteria

• At least 18 years old
• With a compensated fibrosis defined by an hepatic elasticity ≥10 kPa measured by FibroScan®
• Having had blood test at the hospital as part of a consultation or an hospitalisation at the inclusion including usual parameters for the liver disease follow-up
• Affiliated with or beneficiaries of a social security system
• Not opposed to participate to the study after being informed

Exclusion Criteria

• Patients suffering from decompensated cirrhosis or with an history of decompensated cirrhosis
• Patients who received an albumin infusion in the month before the inclusion visit
• Patients suffering from stage 4 or 5 renal failure (GFR < 29 ml/min/1,73m²)
• Patients suffering from cancer
• Pregnant or breastfeeding women or women of childbearing age without effective contraception (based on declaration)
• Patients suffering from impairment of mental faculties or a psychiatric disorder which could interfere with the understanding of the study

• Minimum Eligible Age: 18 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: No

Sponsors

University Hospital, Limoges

OTHER

Sponsor Role: lead

Responsible Party

Responsibility Role: SPONSOR

Locations

Angers Univeristy Hospital

Angers, , France

Site Status: RECRUITING

Limoges University Hospital

Limoges, , France

Site Status: RECRUITING

Poitiers University Hospital

Poitiers, , France

Site Status: RECRUITING

Rennes University Hospital

Rennes, , France

Site Status: RECRUITING

Toulouse University Hospital

Toulouse, , France

Site Status: RECRUITING

Tours University Hospital

Tours, , France

Site Status: NOT_YET_RECRUITING

Pointe à Pitre University Hospital

Pointe-à-Pitre, , Guadeloupe

Site Status: NOT_YET_RECRUITING

Countries

France; Guadeloupe

Central Contacts

Souleiman EL BALKHI, MD

Role: CONTACT

Souleiman.ElBalkhi@chu-limoges.fr

0555058035

Facility Contacts

Jerome BOURSIER, MD

Role: primary

JeBoursier@chu-angers.fr

Souleiman EL BALKHI, MD

Role: primary

Souleiman.ElBalkhi@chu-limoges.fr

Paul CARRIER, MD

Role: backup

Paul.Carrier@chu-limoges.fr

Valentin ROLLE, MD

Role: primary

v.rolle@chu-poitiers.fr

Florent ARTRU, MD

Role: primary

florent.artru@chu-rennes.fr

Christophe BUREAU, MD

Role: primary

bureau.c@chu-toulouse.fr

Laure ELKRIEF, MD

Role: primary

l.elkrief@chu-tours.fr

Moana GELU-SIMEON

Role: primary

moana.simeon@chu-guadeloupe.fr

Other Identifiers

87RI22_0007 (MALAHBAR)

Identifier Type: -

Identifier Source: org_study_id